Neuronal Responses to Physiological Stress

Abstract

Physiological stress can be defined as any external or internal condition that challenges the homeostasis of a cell or an organism. It can be divided into three different aspects: environmental stress, intrinsic developmental stress, and aging. Throughout life all living organisms are challenged by changes in the environment. Fluctuations in oxygen levels, temperature, and redox state for example, trigger molecular events that enable an organism to adapt, survive, and reproduce. In addition to external stressors, organisms experience stress associated with morphogenesis and changes in inner chemistry during normal development. For example, conditions such as intrinsic hypoxia and oxidative stress, due to an increase in tissue mass, have to be confronted by developing embryos in order to complete their development. Finally, organisms face the challenge of stochastic accumulation of molecular damage during aging that results in decline and eventual death. Studies have shown that the nervous system plays a pivotal role in responding to stress. Neurons not only receive and process information from the environment but also actively respond to various stresses to promote survival. These responses include changes in the expression of molecules such as transcription factors and microRNAs that regulate stress resistance and adaptation. Moreover, both intrinsic and extrinsic stresses have a tremendous impact on neuronal development and maintenance with implications in many diseases. Here, we review the responses of neurons to various physiological stressors at the molecular and cellular level.

Introduction

Stress is an inherent component of the natural world that applies to virtually all the biological systems. Biological stress signifies any condition that forces living systems away from a physiological steady state, and its impact is closely connected to the nature of elements that shape living organisms. As stress can be applied to many different levels of biological organization, the term has been used in many different contexts to date. “Physiological stress” is referred to as the primary biological stress and can be defined as any external or internal condition that challenges the homeostasis of a cell or an organism. Taking into account the different possible sources of biological stress, we can conceive three different aspects of physiological stress: environmental stress, intrinsic developmental stress, and aging (Figure 1).

Figure 1

Environmental stress

Biological systems are designed to develop and live in a variety of changing environments. During evolution many different adaptations have been developed to provide organisms with the ability not only to survive but also to reproduce under different, often hostile conditions. Such adaptations are associated with specific structures and behaviors tailored to a specific environment. At the molecular level different strategies exist that are used by cells and systems to respond and adapt to environmental changes such as changes of oxygen availability and temperature fluctuations. Environmental variations exceeding certain levels define “environmental stress.”

Intrinsic developmental stress

An additional cause of physiological stress can be assigned to developmental events. As living organisms develop, they face a variety of challenges associated with morphogenesis and changes in inner chemistry. Indeed, rapid development of embryos causes massive internal changes to an organism as it grows and changes morphology. Different developmental events can cause different stressful conditions with some being harsher than others. Therefore adaptation to developmental stress is equally crucial for the survival of individuals and species.

Aging

When development completes and organismal maturation is achieved, environmental stress is only one aspect of the physiological stress that challenges individuals. Aging constitutes another burden that living organisms have to cope with during their life. Even though aging has often been considered as the deteriorative result of different stresses, it can also be seen as an extra layer of stress throughout life due to the thermodynamic properties of biological materials that lead to the stochastic accumulation of molecular damage over time. The capacity of each organism to cope with aging and other stresses defines its longevity. Thus, functional decline through aging, which occurs even under physiologically perfect environmental conditions, may partly constitute the impact of entropy on organisms and reveals possible imperfections in homeostatic mechanisms.

Role of neurons

Research over the years has identified neurons as major players in stress responses. Neurons do not only receive and process information from the environment but they also have an important direct impact on different aspects of the stress response (Figure 2). In order for neurons to fulfill their roles in stress responses, specific molecules are temporally regulated in response to changes in internal or external conditions.

Figure 2

Aim of the review

This review aims to provide examples that demonstrate the important role of neurons in physiological stress responses as well as the impact of physiological stress on neurons at the intercellular, cellular, and molecular level.

Neuronal Responses

Environmental stress and neuronal circuits

Hypoxia

Sensory neurons form cellular networks through which information from the environment is processed. In lower organisms these networks are relatively simple and stereotypic, and therefore they constitute attractive models to study the effects of physiological stress on neuronal information processing. From studies in C. elegans, in which the entire neuronal circuitry has been mapped (White et al., 1986), it has been found that stress can alter the processing of sensory information. In particular, under hypoxia, a latent circuit is engaged in the processing of gustatory information that is not normally used in normoxic conditions (Pocock and Hobert, 2010). In contrast, the aerotaxis neuronal circuit becomes simplified and less flexible after a hypoxic insult in the same organism (Chang and Bargmann, 2008). Interestingly, food-sensing and O₂-sensing circuits in C. elegans can be altered by a natural gene variation underlining the specific adaptation of the neuronal circuits of different strains in diverse local environments (Cheung et al., 2005). Such plasticity described here alters behavioral responses that may provide the organism with advantages under stress. In higher organisms, where neuronal networks are extremely complex, there is a lack of information as to whether stress can alter the information flow through alternative neuronal networks in a similar way. However, in rats and other animals the so-called “cross phrenic phenomenon” has been observed where a latent respiratory motor pathway is activated by hypoxia, mediating faster recovery from spinal injury (Zhou et al., 2001). Together these examples show the functional plasticity of neuronal circuits and how they can alter information processing in response to environmental stress.

Preconditioning

The functionality of neuronal circuits under harsh environmental conditions can also be dependent on the prior exposure to different stresses (Robertson, 2004). Neurons that have been exposed previously to acute sub-lethal stress appear to retain a memory that allows them to survive and respond to higher doses of this stress than before their initial exposure. This phenomenon is called “preconditioning” or “neurohormesis” (Mattson and Cheng, 2006). Characteristic examples are the enhanced thermotolerance of neurons by prior heat shock in Drosophila (Karunanithi et al., 1999), in locusts (Dawson-Scully and Meldrum Robertson, 1998; Wu et al., 2001), and in C. elegans (Kourtis et al., 2012). Other examples include neuroprotection by prior hypoxic insult to subsequent ischemic conditions in mice (Miller et al., 2001), gerbils (Kitagawa et al., 1991), and in neuronal cell culture (Bruer et al., 1997). Recently it was shown that in piglets, ischemic preconditioning of a distant ischemic tolerant tissue protects the brain against ischemic injury, a phenomenon that is called “remote ischemic preconditioning,” and highlights the complexity of preconditioning mechanisms (Jensen et al., 2011). Interestingly, preconditioning of neurons can also be achieved by low doses of toxins naturally present in fruits and vegetables (Mattson and Cheng, 2006). In addition, exposure to a stress can induce tolerance to a different stress, a phenomenon that is called “cross-tolerance.” For example, in locusts, prior exposure to anoxia induces thermotolerance in neurons that control flight (Wu et al., 2002). In rats, prior exposure to high temperature enhances tolerance to spinal cord ischemia (Zhang et al., 2000). Finally, heat stress in murine cortical cell cultures enhance tolerance to combined oxygen and glucose deprivation (Snider et al., 1998). Preconditioning of neuronal circuits consist of an adaptive mechanism that uses prior experience to better confront hostile conditions. Moreover, stress cross-tolerance is a natural demonstration of the existence of common response mechanisms to different stresses such as high temperature and lack of oxygen.

Synaptic and neuronal network remodeling/plasticity

Another way that neurons respond to physiological stress is by altering their synaptic strength (functional plasticity) and/or connectivity pattern (structural plasticity) in a manner that promotes adaptation. In contrast to organisms like C. elegans where the neuronal connectivity appears to be stereotypical between individuals (White et al., 1986), the adult brain of higher animals exhibits a remarkable level of plasticity and the neuronal networks of certain regions can be altered under different conditions during and after their development (Pascual-Leone et al., 2011). Although this phenomenon has been mainly associated with learning and memory, it can also occur as a response to external stimuli and contributes to the homeostasis of the nervous system. For instance, sensory experience promotes the synaptic integration of new neurons into olfactory circuits in the mouse (Arenkiel et al., 2011). Moreover, chronic intermittent hypoxia alters the synaptic properties in a hub sensory circuit in rats (Kline et al., 2007), and in the peripheral chemoreceptor cells in the mollusk Lymnaea stagnalis synapses develop in vitro that exhibit a form of short-term synaptic plasticity in response to hypoxia (Bell et al., 2007). Finally, it is also characteristic that short-term plasticity of synapses is strongly dependent on temperature (Klyachko and Stevens, 2006). These examples show functional and structural plasticity of the nervous system in response to external stimuli.

Environmental stress and individual neurons

Hypoxia

In addition to different responses that neurons exhibit upon particular stresses, they also exhibit various stress-related phenotypes. Because neurons are highly active cells, they require high amounts of oxygen in order to survive and function. Thus, hypoxia can have a tremendous impact on the physiology of animal brains. Limited oxygen availability during development (Lipton, 1999), at birth (Arpino et al., 2005; Gozzo et al., 2009), and later in life (Lipton, 1999) can cause irreversible damage to neuronal tissue. Hypoxia can also have an effect on axon outgrowth in a rat neuronal cell line (O’Driscoll and Gorman, 2005). In addition, specific in vivo developmental defects of individual neurons caused by hypoxia have been demonstrated in C. elegans. In this model, axon guidance and neuronal migration is defective in specific types of neurons under hypoxic conditions as a result of hypoxia inducible factor-1 hypoxia inducible factor (HIF)-1 stabilization (Pocock and Hobert, 2008). A recent study has also shown that similar defects are observed in the central nervous system of zebrafish via a similar pathway, providing strong evidence that this mechanism is conserved (Stevenson et al., 2012). Thus, hypoxia can have a pleiotropic impact on diverse neurons in different organisms.

Heat shock response

Increase in temperature (hyperthermia) is also known to affect many cell types. However, neurons are particularly susceptible to elevations in temperature, and organismal death under high temperature can be a result of neuronal malfunction before other cells fail (Robertson, 2004). High temperature mainly causes protein misfolding, which triggers cell autonomous and cell-non-autonomous responses (Ramirez et al., 1999). Certain sensory neurons are responsible for sensing the optimal temperature in freely moving animals as well as for the mediation of thermonociception (Clark et al., 2007; Liu et al., 2012). An interesting study in C. elegans has shown that such sensory neurons play a critical role in the cell-non-autonomous heat shock response of somatic cells (Prahlad et al., 2008). In addition, these neurons have also been shown to regulate a response to chronic stress caused by intracellular accumulation of misfolded proteins in remote somatic cells (Prahlad and Morimoto, 2011). Finally, the ciliated ASI chemosensory neurons in the same organism remotely regulate the proliferation vs. differentiation decision in gonads by secreting DAF-7/TGFβ when environmental conditions are favorable (Dalfo et al., 2012). In these ways, sensory neurons regulate systemic stress non-cell autonomously by integrating environmental inputs.

DNA damage response

Genotoxic factors such as UV and other electromagnetic radiations can also cause serious damage to neurons by damaging both their nuclear (Ide et al., 2000) and mitochondrial DNA (LeDoux et al., 2007). In contrast to other cell types that undergo cell cycle checkpoint arrest upon DNA damage, neurons seem to engage components of the cell cycle machinery in response to such insults (Park et al., 1997), as well as in response to other stresses such as ischemic hypoxia (Li et al., 1997; Timsit et al., 1999). Such cell cycle entry of neurons upon stress has been correlated with the apoptotic death after extensive DNA damage (Park et al., 1998; Herrup et al., 2004; Kruman et al., 2004). Moreover, entry of neurons into the cell cycle has also been correlated to neuronal cell death as an early disease related process (Herrup, 2012).

The majority of information on different DNA repair mechanisms available in cells comes from studies in non-neuronal mammalian cell systems. Despite the existence of diverse DNA repair pathways, base excision repair (BER) and nucleotide excision repair (NER) are the major mechanisms responsible for repairing oxidative-induced and UV-induced damage respectively, in both nuclear and mitochondrial DNA (Seeberg et al., 1995; Lagerwerf et al., 2011). Details of NER (Lagerwerf et al., 2011) and BER (Robertson et al., 2009) pathways have been recently reviewed. The gradual maturation of such repair mechanisms in neurons is shown by the fact that mature neurons appear to be more resistant to UV- and IR-induced DNA damage than their younger counterparts (Romero et al., 2003; Shirai et al., 2006). Neurons are also more resistant to IR-induced apoptosis compared to neuronal precursor cells (Kameyama and Inouye, 1994) and other cell types (Li et al., 1996). This highlights the importance of efficient DNA damage response (DDR) mechanisms to maintain mature post-mitotic cells, like neurons, which cannot be replenished (Romero et al., 2003). IR irradiation also affects multiple behavioral outputs of different species by affecting neurons (Sakashita et al., 2010 and references herein). Particularly in C. elegans, IR differentially affects neuron subtypes (Sakashita et al., 2010), which could also suggest that DNA repair efficiency varies between neuron types. Endogenous DNA damage also occurs in neurons. Neurons are highly active cells producing high levels of reactive oxygen species (ROS) that results in increased DNA damage in nuclear and mitochondrial DNA (LeDoux et al., 2007; Barzilai et al., 2008). Responses to endogenous DNA damage are crucial to enable correct neuronal development, and subsequent neuronal maintenance (LeDoux et al., 2007; Lee and McKinnon, 2007; Barzilai et al., 2008). The importance of the DDR in the absence of external mutagenic factors is also supported by genetic conditions in humans that cause developmental defects (O’Driscoll and Jeggo, 2006; Barzilai et al., 2008). Finally, neurons can remotely protect other tissues from insults such as ionizing irradiation. A striking example comes from C. elegans where DNA damage-induced apoptosis in the worm gonad is negatively regulated by a pathway involving HIF-1. Specifically, HIF-1 acts in ASJ amphid sensory neurons to upregulate the tyrosinase family member TYR-2. TYR-2 is subsequently secreted from these neurons and downregulates CEP-1, the homolog of p53, in gonads thereby suppressing radiation-induced apoptosis (Sendoel et al., 2010). It is thus clear that neurons are especially susceptible to both exogenous and endogenous genotoxic reagents and cells can react in both a cell autonomous and non-cell autonomous manner to promote survival.

Intrinsic developmental stress and the nervous system

Stressful conditions in the internal somatic microenvironment of organisms can be caused by development (Simon and Keith, 2008). Even though development has been recognized as an additional layer of stress, there is limited knowledge as to how it influences the nervous system. Developmental stress is unique in its nature by being stereotypical during embryonic and postembryonic life. Therefore, the responses to this stress have to be embedded into neurons and in some cases may serve as a necessary part of their development. The most well studied stressor during development is intrinsic hypoxia. In the developing embryo, hypoxic regions naturally occur as a result of limited O₂ distribution (Simon and Keith, 2008) where the major hypoxia regulator, HIF-1 plays extensive roles (Dunwoodie, 2009). Interestingly, low oxygen levels during development are important for differentiation of many cells and tissues (Morriss and New, 1979; Maltepe and Simon, 1998; Simon et al., 2002) and studies in neuronal cell culture suggest that this might also be true for neurons (Morrison et al., 2000; Studer et al., 2000). Therefore, it seems that development uses an inherent stressful condition, such as embryonic hypoxia, as a signal to form various structures. Thus, it has been suggested that O₂ functions as a developmental morphogen (Simon and Keith, 2008). In addition, the observed hypoxic tolerance of developmentally immature neurons compared to mature neurons is indicative of the adaptation of neurons to developmentally derived hypoxia (Bickler and Buck, 1998).

Neurons can also help the embryo to overcome developmental stress at the behavioral level. In the pond snail Helisoma trivolvis the cilia-driven rotational behavior of early embryos facilitates gas exchange with the surrounding liquid and is regulated by a pair of serotonergic sensory-motor cells that sense oxygen levels (Kuang and Goldberg, 2001; Kuang et al., 2002). This embryonic behavior has also been observed in other species such as in the pond snail Lymnaea stagnalis (Byrne et al., 2009). Other stressors can also be present during development. For example, oxidative stress is produced as a result of routine adult neurogenesis (Walton et al., 2012). The developing brain has adopted a variety of different defenses against developmentally derived oxidative stress (Ikonomidou and Kaindl, 2011), such as differential expression of antioxidant systems during brain development (Aspberg and Tottmar, 1992). Finally, the nervous system is subjected to mechanical stress via movement and from the increasing mass of the brain during development (Van Essen, 1997; Benard and Hobert, 2009). This developmentally derived mechanical stress results in a variety of neuronal responses at different levels (Benard and Hobert, 2009). The above examples describe the existence of developmental stress as an important aspect of development and stress biology. Neurons not only adapt to stress but they also require specific stressors for correct development to occur.

Aging and the nervous system

Aging is perceived as the deteriorative effect of time on different structures of living organisms and many theories have been developed to date to explain how aging evolved in different organisms (Kirkwood and Austad, 2000). Early studies showed a relation between sensory neurons and longevity (Apfeld and Kenyon, 1999). Different types of sensory neurons have been found to regulate C. elegans lifespan in both positive and negative manner, emphasizing the underlying complexity of such regulation (Alcedo and Kenyon, 2004; Bishop and Guarente, 2007; Lee and Kenyon, 2009; Shen et al., 2010a,b). Neurons can impact on longevity in a non-cell autonomous manner. For example, upon neuronal specific mitochondrial stress a cue from the nervous system in C. elegans induces the mitochondria-specific unfolded protein response in intestinal cells, thus increasing the lifespan of the animals (Durieux et al., 2011). In addition, neuroprotection plays a critical role in longevity and aging (Murakami, 2007) and the regulation of aging via neurons appears to be conserved in Drosophila (Parkes et al., 1999; Libert et al., 2007). This association between sensory neurons and longevity shows the non-cell autonomous impact that environmental cues have in organismal aging.

Aging is also known to impact on individual neurons. Beyond pathological conditions, e.g., Alzheimer’s disease and Parkinson disease, which have been well documented over the years (Yankner et al., 2008; Hung et al., 2010), neurons undergo important morphological and functional changes during normal aging. Invertebrate models have been extensively used and have revealed a number of age-related neuronal events. For example, C. elegans touch receptor and cholinergic neurons display age-dependent morphological defects such as cytoskeletal disorganization, axon beading, and defasciculation (Pan et al., 2011). Moreover, unexpected ectopic branching of neurites has been recently observed in C. elegans neurons as a result of aging (Tank et al., 2011). Although this branching was linked to impaired mechanosensory perception and decreased mobility, it seems to be regulated independently of organismal lifespan (Tank et al., 2011). Based on this notion, we could hypothesize that neuronal branching plays a survival role in aged worms in the wild, but not under laboratory conditions and that it is not just a result of aging. This hypothesis would also explain why the branching is regulated by age-related pathways, such as the Jun kinase and the insulin/IGF-1 pathways (Tank et al., 2011). As these pathways are known to affect neuronal plasticity across species (Sherrin et al., 2011; Antoniou and Borsello, 2012; Fernandez and Torres-Aleman, 2012), it is not surprising that they also affect C. elegans neurite branching. Finally, the protection of neurons from aging relies heavily on the general lifestyle of individuals, e.g., diet and exercise, which highlights further the complexity of aging mechanisms (Stranahan and Mattson, 2012).

In higher organisms normal aging influences different parts of the brain at different rates (Woodruff-Pak et al., 2010) and impacts on synaptic connectivity of specific areas of the brain. For example, in the olfactory bulb in mice, the synaptic density of olfactory sensory neurons decreases with age in the glomerular layer but not the external plexiform layer (Richard et al., 2010). Interestingly, other neuronal characteristics, as well as neuronal populations are unaffected in the same region during aging (Richard et al., 2010). Such a selective effect of aging on different synaptic populations is not well understood. However, synaptic dysfunction during aging is conserved and it has been observed in different monkey species (Page et al., 2002; Duan et al., 2003) and in rats, where a study estimated a 27% decrease in axodendritic synapse number in the middle molecular layer of the dentate gyrus in 25 month old individuals compared to those of 3 months old (Bondareff and Geinisman, 1976). The relation between aging-related neuronal phenotypes and cognitive impairment is also not clear. An interesting study in Drosophila has recently made a functional connection between memory loss and impairment in specific neurons during normal aging (Tonoki and Davis, 2012). The authors were also able to retrieve lost memories due to aging by prior stimulation of these neurons (Tonoki and Davis, 2012). Despite the high number of different neuronal defects associated with aging, relatively few neurons die during normal aging (Herndon et al., 2002; Burke and Barnes, 2006). However, a recent study has shown that there is a significant and specific loss of hyperploidic neurons (neurons that contain more than a diploid number of chromosomes) with aging in the cerebral cortex of normal human brain (Fischer et al., 2012). Such specific neuronal loss is yet to show whether it contributes to age-related impairments. In general, neuronal decline rather than neuronal loss seems to be responsible for the negative manifestations of normal aging such as memory loss.

The cause of neuronal changes during aging is not completely understood. A common suspect appears to be increased oxidative stress and is in accordance with the “oxidative stress theory of aging” (Gerschman et al., 1954; Harman, 1956; Cadet, 1988). Oxidative stress is the negative impact of ROS on different aspects of cellular function and can lead to molecular defects such as DNA and mitochondria damage. It is characteristic that genes associated with stress responses and DNA repair are upregulated in the aging human brain (Lu et al., 2004). In normal aging, generation of ROS is elevated due to alterations in neuronal calcium handling and changes in lipid peroxidation (Stranahan and Mattson, 2012). These molecular events can lead to suppression of adult neurogenesis and implementation of alternative plasticity mechanisms to compensate for the damaged tissue (Stranahan and Mattson, 2012). Neurons are particularly vulnerable to oxidative stress, which can lead to neuronal cell death associated with many age-related neurodegenerative diseases (Coyle and Puttfarcken, 1993; Andersen, 2004). Nevertheless, recent studies question the role of oxidative stress in aging (Doonan et al., 2008; Yen et al., 2009; Van Raamsdonk and Hekimi, 2010, 2012; Hekimi et al., 2011). In addition, although it is not known whether any neurons are involved, mild elevations of ROS can be beneficial for a longer lifespan in C. elegans (Lee et al., 2010).

Thus, in general, aging is actively regulated by the nervous system and aging in turn influences neuronal properties. The nature of aging as a stressor appears to go beyond the result of environmental stress and can extend to an inevitable decline of repair mechanisms possibly due to physical entropy.

Neuronal homeostasis

Much of the ability of nervous system to fulfill its role relies on its homeostatic capability. This process is known as “homeostasis” and has been defined as “the maintenance of the constancy of the internal environment” (Turrigiano and Nelson, 2004). Regardless of changes in their environment, the structural and functional integrity of neurons must be conserved throughout life. When homeostatic mechanisms go awry, neurons decline and become unable to respond to external disturbances. This leads to many age-related neurodegenerative diseases, as well as other neuronal defects (Ramocki and Zoghbi, 2008). During development, neurons and neuronal networks put in place a variety of regulatory mechanisms in order to maintain their function despite changes in their microenvironment (Turrigiano and Nelson, 2004). The nervous system is also subjected to a variety of physical stresses throughout life. For example, the addition of new cells into adult neuronal circuits during neurogenesis tends to destabilize the functionality of circuits and dictates homeostatic adaptations in different levels (Meltzer et al., 2005). Neurons can also be challenged from physical body movements, muscle contractions, and injury, all of which have to be confronted by homeostatic mechanisms (Benard and Hobert, 2009). To this end neurons utilize extracellular matrix components, cell adhesion molecules and cytoskeletal proteins to maintain architectural integrity (Benard and Hobert, 2009). Thus, homeostatic mechanisms seem to act in the opposite direction to aging and disease in a complex and dynamic manner.

Key Molecules Involved

The regulation of protein expression under stress is complex and includes mechanisms such as epigenetic gene regulation, transcriptional regulation, and post-transcriptional regulation. Many molecules have been reported in many different species to mediate the cellular responses to stress. However, only a fraction of them have specific roles in neurons during these responses (Table 1). We summarize here studies for some key molecules involved in neuronal stress responses.

Transcription factors

Hypoxia inducible factors

Hypoxia inducible factors are the key modulators of hypoxic stress responses. They function as heterodimers consisting of an oxygen regulated α and a stable β subunit. The HIF heterodimer binds to the promoter of target genes via hypoxia response elements (HREs) with the consensus sequence G/ACGTG (Figure 3A; Majmundar et al., 2010). These target genes regulate a vast array of processes that enable cellular adaptation to hypoxia. HIFα is primarily regulated by oxygen-dependent prolyl hydroxylase-domain enzymes (PHDs) that lead to its degradation via the von Hippel–Lindau tumor suppressor protein (VHL) under normoxia (Epstein et al., 2001). In hypoxic conditions PHD activity is diminished and HIFα is stabilized (Figure 3A; Epstein et al., 2001; Majmundar et al., 2010). A recent study in C. elegans has also implicated the homolog of sulfhydrylases/cysteine (CYSL-1) in stabilizing HIF-1α in neurons via EGL-9, the worm PHD homolog, as a response to hypoxia-derived intracellular hydrogen sulfide (H₂S; Figure 3A; Ma et al., 2012).

Figure 3

Various studies have shown a specific role of HIF-1 in neurons. Depletion of HIF-1α in the mouse brain and in neuronal cell cultures causes increased cell damage and lower survival rate after cerebral ischemia (Baranova et al., 2007). In rat cortical neurons, HIF-1α appears to play a protective role in early steps of responses to mild hypoxia (Lopez-Hernandez et al., 2012). HIF-1α has recently been shown to regulate prion protein expression in hippocampal neuronal cells to protect from cell damage (Jeong et al., 2012). Moreover, it is not clear whether HIF-1α plays a central role in hypoxic preconditioning as different studies argue for (Grimm et al., 2005; Shao et al., 2007; Ara et al., 2011) and against (Li et al., 2011) such a role. Although HIF-1 retains neuroprotective and anti-apoptotic properties, there is experimental evidence that point to a deteriorative impact of stabilized HIF-1α on neuronal tissue. For example, HIF-1 stabilization causes axon guidance and neuronal migration defects in C. elegans (Pocock and Hobert, 2008) and promotes neurodegeneration in neonatal rat brain (Jiang et al., 2012). In addition, HIF-1 in C. elegans negatively regulates lifespan extension by dietary restriction, acting in the serotonergic neurons ADF and NSM (Chen et al., 2009). However, studies from other groups report that in the same organism HIF-1 promotes longevity (Mehta et al., 2009; Zhang et al., 2009; Lee et al., 2010). This discrepancy was addressed in two more recent studies where it was shown that HIF-1 regulates longevity in a temperature-dependent manner (Hwang and Lee, 2011; Leiser et al., 2011). Thus, it is possible that the role of HIF-1 in longevity is context-dependent and may involve different neurons or other cells under the different conditions. While C. elegans neurons have also been recently found to sense and respond to hypoxia in a HIF-independent manner (Park et al., 2012), HIFs appear to be the main factors mediating neuronal responses to hypoxia through the regulation of many downstream effectors. This is despite the fact that neuroprotective properties of HIF may cause side effects on other aspects of neuronal physiology.

Heat shock factors and heat shock proteins

Heat shock factors (HSFs) are stress-inducible transcription factors that upon induction positively regulate the expression of heat shock proteins (HSPs) through direct binding to their promoters containing heat shock elements (HSEs; NGAAN; Shamovsky and Nudler, 2008). The master regulator of heat shock response is the HSF-1, which under normal conditions is in a monomeric inactive form (Shamovsky and Nudler, 2008). Upon different stress conditions HSF-1 forms an active trimer that enters the nucleus in order to activate HSPs (Figure 3B; Shamovsky and Nudler, 2008). The regulation of HSPs by HSFs is highly conserved from yeast to mammals (Liu et al., 1997). HSPs function as molecular chaperones to facilitate the proper folding of other cellular proteins. Protein misfolding can originate under normal cellular conditions, and under different stresses. It has also been shown that over-excitation of motor neurons can cause protein misfolding in post-synaptic muscle cells in C. elegans (Garcia et al., 2007). The induction of HSFs in neurons and in other cell types is not only stimulated by hyperthermia as its name implies, but also by other stresses, such as, hypoxia, alterations in the intracellular redox environment, and exposure to heavy metals and amino acid analogs (Morimoto et al., 1997). HSPs have also been shown to be upregulated in ischemic preconditioning (Liu et al., 1993; Kato et al., 1995). The neuroprotective properties of HSF-1, the principal regulator of heat shock response in C. elegans, have been demonstrated in two recent studies where upregulation of HSF-1 suppresses the defective neuronal phenotypes of a Machado–Joseph disease mutant model (Teixeira-Castro et al., 2011) and HSF-1 and the small heat shock protein HSP-16.1 mediate cytoprotection by heat preconditioning (Kourtis et al., 2012). In addition to HSPs, HSFs can induce the transcription of other proteins with various functions (Akerfelt et al., 2010). Some of them have neuroprotective functions under stress. For example, under heat shock in Drosophila, HSFs induce the expression of the NAD synthesis enzyme, nicotinamide mononucleotide adenylyltransferase (NMNAT), which is critical for neuronal maintenance under stress (Ali et al., 2011).

The expression of HSF-1 in neurons appears to be strictly controlled (Dirks et al., 2010) and the increased susceptibility of neurons to heat shock treatment is associated with the delayed onset of HSF-1 expression (Batulan et al., 2003; Kern et al., 2010). However, HSPs may have a more neuronal specific role under normal conditions, as some HSPs are constitutively more highly expressed in neurons than other cells (Chen and Brown, 2007). The beneficial role of the expression of HSPs was recently recognized (Rordorf et al., 1991) and can be induced by chemical compounds serving as medical drugs against different degenerative diseases (Katsuno et al., 2005; Chow and Brown, 2007). Many HSFs and HSPs are also up- and down-regulated during normal development of different species (Akerfelt et al., 2010), which may suggest a protective role for these proteins with regards to intrinsic developmental stress. Moreover, HSPs are related to normal and abnormal embryonic development (Evans et al., 2005; Brown et al., 2007) and the expression of HSPs has shown to be phase- and tissue-specific (Loones et al., 1997; Masuda et al., 1998). HSFs and HSPs are also implicated in aging. Hsp22, when over-expressed in motor neurons was shown to increase the lifespan of Drosophila by 30% (Morrow et al., 2004) and the flies maintained their locomotory activity longer and were more resistant to oxidative stress and hyperthermia (Morrow et al., 2004). In C. elegans HSF-1 promotes longevity by acting in neurons and other tissues (Lithgow et al., 1995; Hsu et al., 2003; Morley and Morimoto, 2004). Finally, the heat shock response of AFD and AIY thermosensory neurons in C. elegans involves upregulation of Hsp70 protein (Prahlad et al., 2008). It is thus apparent that HSFs and HSPs are involved in the core of the response mechanisms against many different stresses with particular importance in neuronal cell function.

Signaling molecules

Mitogen-activated protein kinases

Mitogen-activated protein (MAP) kinases are essential signal transduction molecules that mediate the response to environmental cues in virtually all cell types and play key roles in cellular functions such as differentiation, cell survival, and apoptosis (Gehart et al., 2010). These and other general roles of certain MAP kinases in neurons was demonstrated several years ago (Fukunaga and Miyamoto, 1998). Sub-families of MAPKs have been recognized to date such as the extracellular signal-regulated kinases (ERK1/2), ERK5 (also known as BMK1 or MAPK7), the Jun amino-terminal kinases (JNK) 1–3, and the p38 kinases (p38α, β, γ, and δ; Gehart et al., 2010). The exact content and features of the different MAPK pathways have been described elsewhere (Dhillon et al., 2007). However, the general scheme of MAPK signaling follows the sequence “stimulus – G-protein – MAPKKK – MAPKK – MAPK- final response” (Dhillon et al., 2007). The stress-activated MAPK pathways are essentially the JNK and the p38 kinases (Figure 3D; Dhillon et al., 2007).

The JNK pathway can be induced by oxidative and osmotic stress, UV radiation, and other DNA-damaging agents to modulate the Activator protein-1 (AP1) and other transcription factors, such as HSF-1 and HIF-1 (Park and Liu, 2001; Antoniou and Borsello, 2012) in order to regulate the cellular stress responses. Neuronal apoptosis after stress is positively regulated by the JNK pathway (Weston and Davis, 2002; Biteau et al., 2011) and JNK/MAPK signaling is also involved in axon regeneration after injury in C. elegans (Hammarlund et al., 2009; Yan et al., 2009; Li et al., 2012). Moreover, the JNK pathway in neurons promotes organismal longevity by activating neuroprotective mechanisms in Drosophila (Lee et al., 2009; Biteau et al., 2011; Takahama et al., 2012), and in C. elegans (Oh et al., 2005). Finally, the JNK pathway can act by modulating FOXO transcription factors and antagonizes Insulin/IGF-1 factors to regulate different aspects of stress resistance and aging (Wang et al., 2005; Neumann-Haefelin et al., 2008).

p38 kinase pathway can be induced by stresses such as hypoxia, oxidative stress, IR, and UV irradiation and it is mainly implicated in the induction of neuronal apoptosis under different stresses (Horstmann et al., 1998; Namgung and Xia, 2000; Choi et al., 2004; Guo and Bhat, 2007). The p38 pathway also appears to play a role in neuroprotection against ischemia after isoflurane preconditioning (Zheng and Zuo, 2004). However, the p38 pathway has other roles in neurons beyond stress responses (Takeda and Ichijo, 2002).

Target of rapamycin

Target of rapamycin (TOR) is an evolutionary conserved serine/threonine kinase important predominantly in regulating cell growth and proliferation, with implications in many different aspects of development, aging, and disease (Wullschleger et al., 2006). TOR functions as a sensor of extracellular signals, including stressors such as hypoxia and nutrient deprivation, and is found in two functionally distinct complexes, namely TORC1 and TORC2 (Figure 3D). Inhibition of TOR signaling increases lifespan in many organisms, including mice and Drosophila, partly by reducing mRNA translation (Harrison et al., 2009; Bjedov et al., 2010). Even though mammalian TOR is ubiquitously expressed, it plays an extensive role in neuronal development and plasticity (Jaworski and Sheng, 2006; Chong et al., 2010; Hoeffer and Klann, 2010). TOR has also been recently found to be important for synaptic homeostasis in Drosophila (Penney et al., 2012) and for synaptic plasticity after ischemia in rats (Ghiglieri et al., 2010). mTOR may also be involved in the regulation of HIF-1alpha in the developing rat brain with hypoxia-ischemia (Chen et al., 2012). However, the role of TOR signaling in mediating stress responses in neurons has not been fully elucidated.

Insulin/IGF-1 signaling

The insulin/IGF-1 pathway is a very well characterized pathway that regulates aging and longevity in many different species (van Heemst et al., 2005). The complexity of Insulin/IGF-1 signaling (IIS) pathway has been greatly increased during evolution (van Heemst et al., 2005). In the nematode C. elegans, where the involvement of this pathway in aging was first discovered and extensively studied, the insulin-like growth factor receptor DAF-2 is activated by insulin-like peptides (ILP; 40 encoded in worm genome) that are primarily expressed in neurons (Pierce et al., 2001; Li et al., 2003; Husson et al., 2007; Cornils et al., 2011). After ligand binding, the signal is transduced directly or via the insulin receptor substrate homolog protein-1 (IST-1) to the phosphatidylinositol 3-kinase (PI-3K) consisting of the catalytic subunit AGE-1 (aging alteration-1) and the regulatory subunit AAP-1 (phosphoinositide kinase AdAPter subunit), which converts phosphatidylinositol 4,5-bisphosphate (PIP₂) into phosphatidylinositol 3,4,5-trisphosphate (PIP₃; van Heemst, 2010). PIP₃ activates the 3-phosphoinositide-dependent protein kinase-1 (PDK1) and the protein kinases B (known as AKT-1/2), leading to the phosphorylation of DAF-16, a homolog of the mammalian FoxO family of transcription factors (van Heemst, 2010). Phosphorylated DAF-16 is retained in the cytoplasm whereas unphosphorylated DAF-16 enters the nucleus to regulate a battery of stress response genes (Figure 3D; Lin et al., 2001; Lee et al., 2003a; Murphy et al., 2003).

Although the insulin receptor was found expressed in neuronal tissue (Havrankova et al., 1978; Unger et al., 1989), and its distribution appears to be enriched in particular brain areas (Schulingkamp et al., 2000), its role in neurons was not clear. As neurons can take up glucose without the involvement of insulin or insulin receptor, these cells were believed to be “insulin insensitive.” Cline and colleagues provided the first in vivo evidence that the insulin pathway regulates neuronal circuit function and synaptic maintenance in the central nervous system of Xenopus tadpoles (Chiu et al., 2008). Previous studies had also demonstrated the role of insulin signaling in the regulation of lifespan in C. elegans neurons (Kenyon et al., 1993; Kimura et al., 1997; Apfeld and Kenyon, 1998; Wolkow et al., 2000), in Drosophila neuroendocrine cells (Tatar et al., 2001), and in the mammalian brain (Kappeler et al., 2008). A number of other studies have identified roles of the neuronal insulin pathway in energy homeostasis (Konner et al., 2011; Freude et al., 2012), synaptic plasticity (Oda et al., 2011; Costello et al., 2012), and neuronal apoptosis following hypoxic insult (Liu et al., 2011). Interestingly, IIS has also been shown to regulate salt chemotaxis learning in C. elegans (Tomioka et al., 2006). The insulin pathway can also act on neurons non-cell autonomously to regulate neuronal aging (Pan et al., 2011) and has also been shown to act in neurons to suppress organismal survival under hypoxia (Scott et al., 2002). In general, the insulin pathway has extended roles in neuronal tissues of many organisms that can span from the regulation of aging to hypoxia sensitivity.

Nitric oxide

Nitric oxide (NO) is a free radical important for cell signaling with a number of physiological roles such as synaptic plasticity and neurotransmission. The enzyme responsible for NO production in neurons is the neuronal nitric oxide synthase (nNOS) that mediates the generation of l-citrulline from l-arginine (Figure 3D; Zhou and Zhu, 2009). nNOS responds to oxygen levels and is upregulated by hypoxia in different neurons (AbuSoud et al., 1996; Prabhakar et al., 1996). NO regulates a variety of stress-related transcription factors such as HIF-1 and NF-κB (Contestabile, 2008; Keswani et al., 2011) and can lead to neuronal death under different stress conditions (Brown, 2010). Interestingly, NO in neurons can also be induced by extremely low frequency magnetic fields (ELF-MF) in the rat brain, a usual stressor emanated from electrical devices (Cho et al., 2012). Therefore, NO appears to be an important inorganic molecule for neuronal stress responses.

MicroRNAs

MicroRNAs (miRNAs) are small non-coding RNA molecules with a length of approximately 22 nucleotides that act as post-transcriptional regulators of gene expression (Ebert and Sharp, 2012). They have the ability to fine-tune expression to ensure stability under sudden external or internal perturbations or, if needed, enforce a new gene expression program that enables an organism to tolerate a new environment (Ebert and Sharp, 2012). miRNAs are transcribed, mostly by RNA polymerase II (Pol II), as capped and polyadenylated primary miRNAs (pri-miRNAs) that fold in extended hairpin structures. The pri-miRNAs are cleaved in the nucleus by the RNase III enzyme Drosha, creating the shorter precursor miRNA (pre-miRNA; Lee et al., 2003b). The pre-miRNA is transported by exportin-5 (XPO5) via the nucleopore complex (NPC; Yi et al., 2003) out of the nucleus (Lee et al., 2011) where is further processed by the RNase II enzyme, Dicer, and is incorporated into an Argonaute-containing RNA-induced silencing complex (RISC; Lee et al., 2002). In the RISC complex, the miRNA associates with a specific target mRNA by imperfectly base-pairing with its 3′ UTR and mediates post-transcriptional repression (PTR) or decay of specific mRNA targets (Figure 3C; Lee et al., 2002, 2003b, 2011; Pasquinelli, 2012). Robustness in systems that control cell fate, developmental transitions, and stress responses is required under changing conditions as fluctuations in the internal or external environment can be fatal for an organism. miRNAs can generate rapid and reversible responses and, in this way, are ideal molecules for mediating stress responses. As deletion of individual miRNAs (Miska et al., 2007) or whole miRNA families in C. elegans (Alvarez-Saavedra and Horvitz, 2010) have little to no effect on viability and development and as most of the miRNA knock-out mice do not show any gross phenotypes (Park et al., 2010), it is believed that the main function of miRNAs may be to buffer gene expression when an organism is challenged under stressful conditions. Supporting this idea Zhang and colleagues showed that deletion of mir-71 impaired the long-term survival of nematodes during starvation-induced L1 diapause (Zhang et al., 2011b). In addition, miR-7 was shown to be essential for the maintenance of regulatory stability under temperature stress during development of a Drosophila sensory organ (Li et al., 2009b). miRNAs are abundantly expressed in the nervous system and a relation between miRNAs and neuronal responses to stress has been demonstrated in different model systems. Most recently, mir-71 has also been associated with an increase in lifespan in C. elegans (Boulias and Horvitz, 2012). This study showed that expression of mir-71 in neurons alone was sufficient to promote germline-mediated longevity and proposed a model in which mir-71 mediates lifespan-extending signals through the DAF-16/FOXO transcription factor in the nervous system. The direct mechanism by which the internal stress is sensed by the neurons is not clear; however the function of miR-71 was shown to be partly dependent on expression of TCER-1 (Boulias and Horvitz, 2012), a transcription elongation factor shown to promote the transcriptional activity of DAF-16 in the intestine (Ghazi et al., 2009). Systemic stress can also be triggered by alcohol and neuronal adaptation to this stress was shown to cause a rapid increase in miR-9 expression in neurons (Pietrzykowski et al., 2008). This led to transcription of a voltage-activated potassium channel isoform associated with an increase in alcohol tolerance. This process may represent a general mechanism of neuronal adaptation to alcohol and suggests that miR-9 has an important role in neuronal plasticity (Pietrzykowski et al., 2008). A study in primary rat hippocampal neuronal cells has also shown that under hypoxia, the miR-130 family is highly expressed (Saito et al., 2011). In particular, miR-130a appears to decrease DDX6 protein levels, the normal function of which is to restrict HIF 1α (HIF-1α) mRNA to P-bodies of hippocampus neuronal cells of mice (Saito et al., 2011). Under hypoxia, HIF-1α mRNA is released from these foci and the protein can regulate oxygen homeostasis (Saito et al., 2011). The expression of miRNAs in response to stress has also been demonstrated to be cell specific. In a primary cell culture-based assay, astrocytes and neurons were subjected to oxygen-glucose deprivation to mimic ischemia, which is an essential feature of traumatic brain injuries (Ziu et al., 2011). In this model, different panels of miRNAs were upregulated in the two cell types, indicating that different neurons utilize different biochemical pathways to respond to physiological stress (Ziu et al., 2011). Together these studies suggest that miRNAs are implicated in neuronal stress responses. However, further research is expected to address more questions as to how miRNAs regulate neuronal responses to stress, and determine their impact on organismal homeostasis.

Discussion

The physical world is built around principles that dictate the usage and management of energy. These principles are all connected by the basic laws of physics, and obey the same basic restrictions and limitations. We can think of living organisms as biological engines using their structures to utilize energy in order to survive and reproduce in a certain environment. The negative biological impact of stress on living systems relies on the inability of the latter to function and continue utilizing energy under certain conditions. This may either reflect the limitations of certain basic principles when, for example, no life can thrive at a temperature of absolute zero (−273°C), or a lack of adaptation of a particular organism to a given environment when, for example, an elephant cannot survive in Antarctica, while a polar bear cannot survive in the African savannah. Apart from such extreme mismatches between life and environmental conditions, there are milder ones that define stress as we discuss here. Stressful conditions often differ between organisms as different species have adapted to different environments. The extent to which each species has adopted defense mechanisms against stressors may reflect the extent of the presence of the relevant conditions during evolution.

Intrinsic developmental stress and aging can also count as selective factors for genes that give a survival advantage in the course of evolution, in the same manner as external environmental stress does. Stress derived from development may have led organisms to adopt particular developmental programs that lead to the final structures; and aging may have selected molecular pathways that lead different organisms to achieve a health span that fits their ecological role. Considering the cellular properties of neurons and their documented implication in stress responses, the nervous system could constitute a “hot-spot” for the evolutionary adaptation of organisms to different stresses. In this sense, stress can be seen as a driving force of biodiversity in the long term that may have been particularly applied on the different levels of neuronal organization to select for the variety of the adaptation mechanisms to stress we presented here. However, the role of neurons on aging of higher organisms is not yet well understood. Much of our knowledge in this field comes from invertebrate models where it is characteristic that long-lived animal mutants show tolerance in different stresses (Kourtis and Tavernarakis, 2011). Yet there is clearly an additional level of active regulation of aging and longevity by neurons that is beyond a simple resistance to environmental stress.

During the life of an organism, stress conditions subject a burden that needs to be confronted and overcome in order to survive and reproduce. We have described mechanisms that have been developed for this purpose; however, stress often leads to disease and death. This stress can be termed as “pathophysiological stress” and it is beyond the scope of this review. Moreover, bacterial and other infections consist a form of environmental stress that leads to neuronal inputs of immune responses, which have been discussed elsewhere (Rosas-Ballina and Tracey, 2009).

Despite the plethora of harsh conditions present in the life of an organism, living systems are remarkably adept at coping with internal and external stress and preserve their homeostatic balance. A big part of this ability relies on the nervous system as we described in this review. As neurons sense fluctuations in conditions, they use this information to orchestrate appropriate defense and adaptation responses at different levels (Figure 2). In addition, neurons can systemically act on other cells to regulate their response to stress. The importance of the role of the nervous system in stress responses is simply highlighted by the well-known ability of neurons to quickly respond to environmental changes. This ability integrates external inputs to the several different lines of defense that span from cell protection to behavioral strategies. The extent to which neurons have adapted to different stresses during their development is also demonstrated by the fact that developmentally immature neurons are more resistant to hypoxia (Romero et al., 2003; Shirai et al., 2006) than their mature counterparts, whereas mature neurons are more resistant to UV and IR than immature ones (Bickler and Buck, 1998). This resistance of neurons to different stresses at different developmental stages may reflect the exposure of the organisms to these stresses in the course of their life.

There is also an inherent element of stress in natural systems that is connected to aging. Regardless of how perfect an environment is and how well an organism is adapted to this environment, eventually the organism will functionally decline. Instead of considering aging as an event that comes late in the biological “equation” of living systems, we propose that aging is an extra layer of stress that applies throughout life and is related to the physical entropy (Figure 1). As energy cannot be transformed from one form to another without a qualitative loss (second law of thermodynamics), every single chemical reaction performed by a cell may contribute to aging. Similar ideas have been supported by others (Hayflick, 2007 and references therein).

Currently, aging is defined as a post-reproductive process precluding the selection for and transmission of the relevant genes to the next generation. However, a number of studies have now shown that many molecular pathways have an impact on organismal longevity and that these pathways are conserved among species. Our hypothesis that aging occurs before, during and after reproduction, could provide a basis for the evolution of a genetic program regulating aging. At the same time, the stochastic nature of aging due to physical entropy could explain the variations in lifespan and in expression of biomarkers of aging between genetically identical individuals, for example in cloned worm populations (Herndon et al., 2002). However, other explanations have been provided for such variations like epigenetic modifications occurring in early development and adulthood (Bell and Spector, 2011; Steves et al., 2012).

In addition to the active neuronal responses under certain stresses, neurons can experience several side effects under stressful conditions. The distinction between an active neuronal response and a stress-derived neuronal defect is often not clear. In the laboratory environment a potential beneficial advantage of a neuronal phenotype under a stressor can be missed due to the absence of the condition under which this phenotype promotes survival, and which is present in the natural habitat of the organism. However, strong deteriorative impact of stress on different structures can be recognized in many cases as we described.

The study of intrinsic developmental stress and its significance to embryonic and neuronal development is admittedly technically challenging. Very few studies have clearly shown the impact of such stress on normal development (Zhang et al., 2011a) and fewer of them have focused on neurons (Benard and Hobert, 2009). However, the information derived from these studies provide the basis for further investigations and provide a first glance as to the importance of the different aspects of intrinsic developmental stress on normal development.

In the field of human and murine biology, “stress” has mainly been associated with the psychological reaction of an individual to stressful external stimuli, and has been connected to the central nervous system, which generates sentiments like fear and anxiety. Although this consists a very important aspect of the biology of “stress,” it is extremely complex in its origin and manifestation. Therefore, we think that studying primary “stress” in a reductionist manner using models like C. elegans will provide us with more detailed information on how neurons survive and respond under “stress,” and how they are affected by it. Supportive of this approach are many examples where the psychological stress involves similar mechanism to other more basic aspects of stress (Yao et al., 2007).

References

• 1

  AbrahamR. T. (2001). Cell cycle checkpoint signaling through the ATM and ATR kinases. Genes Dev.15, 2177–2196.10.1101/gad.914401

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 2

  AbuSoudH. M.RousseauD. L.StuehrD. J. (1996). Nitric oxide binding to the heme of neuronal nitric-oxide synthase links its activity to changes in oxygen tension. J. Biol. Chem.271, 32515–32518.10.1074/jbc.271.1.104

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 3

  AkerfeltM.MorimotoR. I.SistonenL. (2010). Heat shock factors: integrators of cell stress, development and lifespan. Nat. Rev. Mol. Cell Biol.11, 545–555.10.1038/nrm2938

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 4

  AlcedoJ.KenyonC. (2004). Regulation of C. elegans longevity by specific gustatory and olfactory neurons. Neuron41, 45–55.10.1016/S0896-6273(03)00816-X

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 5

  AliY. O.McCormackR.DarrA.ZhaiR. G. (2011). Nicotinamide mononucleotide adenylyltransferase is a stress response protein regulated by the heat shock factor/hypoxia-inducible factor 1alpha pathway. J. Biol. Chem.286, 19089–19099.10.1074/jbc.M111.219295

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 6

  Alvarez-SaavedraE.HorvitzH. R. (2010). Many families of C. elegans microRNAs are not essential for development or viability. Curr. Biol.20, 367–373.10.1016/j.cub.2009.12.051

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 7

  AnJ. H.BlackwellT. K. (2003). SKN-1 links C. elegans mesendodermal specification to a conserved oxidative stress response. Genes Dev.17, 1882–1893.10.1101/gad.1107803

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 8

  AndersenJ. K. (2004). Oxidative stress in neurodegeneration: cause or consequence?Nat. Med.10(Suppl.), S18–S25.10.1038/nrn1434

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 9

  AntoniouX.BorselloT. (2012). The JNK signalling transduction pathway in the brain. Front. Biosci. (Elite Ed.)4, 2110–2120.10.2741/528

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 10

  AntoniouX.GassmannM.OgunsholaO. O. (2011). Cdk5 interacts with Hif-1alpha in neurons: a new hypoxic signalling mechanism?Brain Res.1381, 1–10.10.1016/j.brainres.2010.10.071

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 11

  ApfeldJ.KenyonC. (1998). Cell nonautonomy of C. elegans daf-2 function in the regulation of diapause and life span. Cell95, 199–210.10.1016/S0092-8674(00)81751-1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 12

  ApfeldJ.KenyonC. (1999). Regulation of lifespan by sensory perception in Caenorhabditis elegans. Nature402, 804–809.10.1038/45544

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 13

  AraJ.FeketeS.FrankM.GoldenJ. A.PleasureD.ValenciaI. (2011). Hypoxic-preconditioning induces neuroprotection against hypoxia-ischemia in newborn piglet brain. Neurobiol. Dis.43, 473–485.10.1016/j.nbd.2011.04.021

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 14

  ArenkielB. R.HasegawaH.YiJ. J.LarsenR. S.WallaceM. L.PhilpotB. D.et al (2011). Activity-induced remodeling of olfactory bulb microcircuits revealed by monosynaptic tracing. PLoS ONE6, e29423.10.1371/journal.pone.0029423

  • CrossRef
  • Google Scholar

• 15

  ArpinoC.D’argenzioL.TicconiC.Di PaoloA.StellinV.LopezL.et al (2005). Brain damage in preterm infants: etiological pathways. Ann. Ist. Super. Sanita41, 229–237.

  • Pubmed Abstract
  • Google Scholar

• 16

  AspbergA.TottmarO. (1992). Development of antioxidant enzymes in rat-brain and in reaggregation culture of fetal brain-cells. Brain Res. Dev. Brain Res.66, 55–58.10.1016/0165-3806(92)90139-N

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 17

  BaranovaO.MirandaL. F.PichiuleP.DragatsisI.JohnsonR. S.ChavezJ. C. (2007). Neuron-specific inactivation of the hypoxia inducible factor 1 alpha increases brain injury in a mouse model of transient focal cerebral ischemia. J. Neurosci.27, 6320–6332.10.1523/JNEUROSCI.0449-07.2007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 18

  BarzilaiA.BitonS.ShilohY. (2008). The role of the DNA damage response in neuronal development, organization and maintenance. DNA Repair (Amst.)7, 1010–1027.10.1016/j.dnarep.2008.03.005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 19

  BatulanZ.ShinderG. A.MinottiS.HeB. P.DoroudchiM.NalbantogluJ.et al (2003). High threshold for induction of the stress response in motor neurons is associated with failure to activate HSF1. J. Neurosci.23, 5789–5798.

  • Pubmed Abstract
  • Google Scholar

• 20

  BellH. J.InoueT.ShumK.LukC.SyedN. I. (2007). Peripheral oxygen-sensing cells directly modulate the output of an identified respiratory central pattern generating neuron. Eur. J. Neurosci.25, 3537–3550.10.1111/j.1460-9568.2007.05607.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 21

  BellJ. T.SpectorT. D. (2011). A twin approach to unraveling epigenetics. Trends Genet.27, 116–125.10.1016/j.tig.2010.12.005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 22

  BenardC.HobertO. (2009). Looking beyond development: maintaining nervous system architecture. Curr. Top. Dev. Biol.87, 175–194.10.1016/S0070-2153(09)01206-X

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 23

  BenardC. Y.BoyanovA.HallD. H.HobertO. (2006). DIG-1, a novel giant protein, non-autonomously mediates maintenance of nervous system architecture. Development133, 3329–3340.10.1242/dev.02507

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 24

  BicklerP. E.BuckL. T. (1998). Adaptations of vertebrate neurons to hypoxia and anoxia: maintaining critical Ca2+ concentrations. J. Exp. Biol.201, 1141–1152.

  • Pubmed Abstract
  • Google Scholar

• 25

  BishopN. A.GuarenteL. (2007). Two neurons mediate diet-restriction-induced longevity in C. elegans. Nature447, 545–549.10.1038/nature05904

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 26

  BiteauB.KarpacJ.HwangboD.JasperH. (2011). Regulation of Drosophila lifespan by JNK signaling. Exp. Gerontol.46, 349–354.10.1016/j.exger.2010.11.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 27

  BjedovI.ToivonenJ. M.KerrF.SlackC.JacobsonJ.FoleyA.et al (2010). Mechanisms of life span extension by rapamycin in the fruit fly Drosophila melanogaster. Cell Metab.11, 35–46.10.1016/j.cmet.2009.11.010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 28

  BondareffW.GeinismanY. (1976). Loss of synapses in the dentate gyrus of the senescent rat. Am. J. Anat.145, 129–136.10.1002/aja.1001450110

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 29

  BouliasK.HorvitzH. R. (2012). The C. elegans microRNA mir-71 acts in neurons to promote germline-mediated longevity through regulation of DAF-16/FOXO. Cell Metab.15, 439–450.10.1016/j.cmet.2012.02.014

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 30

  BrownG. C. (2010). Nitric oxide and neuronal death. Nitric Oxide23, 153–165.10.1016/j.niox.2010.06.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 31

  BruerU.WeihM. K.IsaevN. K.MeiselA.RuscherK.BergkA.et al (1997). Induction of tolerance in rat cortical neurons: hypoxic preconditioning. FEBS Lett.414, 117–121.10.1016/S0014-5793(97)00954-X

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 32

  BurkeS. N.BarnesC. A. (2006). Neural plasticity in the ageing brain. Nat. Rev. Neurosci.7, 30–40.10.1038/nrn1809

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 33

  BurketC. T.HigginsC. E.HullL. C.BerninsoneP. M.RyderE. F. (2006). The C. elegans gene dig-1 encodes a giant member of the immunoglobulin superfamily that promotes fasciculation of neuronal processes. Dev. Biol.299, 193–205.10.1016/j.ydbio.2006.07.019

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 34

  BrownD. D.ChristineK. S.ShowellC.ConlonF. L. (2007). Small heat shock protein hsp27 is required for proper heart tube formation. Genesis45, 667–678.10.1002/dvg.20340

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 35

  ByrneR. A.RundleS. D.SmirthwaiteJ. J.SpicerJ. I. (2009). Embryonic rotational behaviour in the pond snail Lymnaea stagnalis: influences of environmental oxygen and development stage. Zoology (Jena)112, 471–477.

  • Pubmed Abstract
  • Google Scholar

• 36

  CadetJ. L. (1988). Free radical mechanisms in the central nervous system: an overview. Int. J. Neurosci.40, 13–18.10.3109/00207458808985722

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 37

  ChangA. J.BargmannC. I. (2008). Hypoxia and the HIF-1 transcriptional pathway reorganize a neuronal circuit for oxygen-dependent behavior in Caenorhabditis elegans. Proc. Natl. Acad. Sci. U.S.A.105, 7321–7326.10.1073/pnas.0709118105

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 38

  ChechlaczM.VemuriM. C.NaegeleJ. R. (2001). Role of DNA-dependent protein kinase in neuronal survival. J. Neurochem.78, 141–154.10.1046/j.1471-4159.2001.00380.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 39

  ChenD.ThomasE. L.KapahiP. (2009). HIF-1 modulates dietary restriction-mediated lifespan extension via IRE-1 in Caenorhabditis elegans. PLoS Genet.5, e1000486.10.1371/journal.pgen.1000486

  • CrossRef
  • Google Scholar

• 40

  ChenH.XiongT.QuY.ZhaoF.FerrieroD.MuD. (2012). mTOR activates hypoxia-inducible factor-1alpha and inhibits neuronal apoptosis in the developing rat brain during the early phase after hypoxia-ischemia. Neurosci. Lett.507, 118–123.10.1016/j.neulet.2011.11.033

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 41

  ChenS.BrownI. R. (2007). Neuronal expression of constitutive heat shock proteins: implications for neurodegenerative diseases. Cell Stress Chaperones12, 51–58.10.1379/CSC-236R.1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 42

  ChengI. H.LinY. C.HwangE.HuangH. T.ChangW. H.LiuY. L.et al (2011). Collagen VI protects against neuronal apoptosis elicited by ultraviolet irradiation via an Akt/phosphatidylinositol 3-kinase signaling pathway. Neuroscience183, 178–188.10.1016/j.neuroscience.2010.09.056

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 43

  CheungB. H.CohenM.RogersC.AlbayramO.De BonoM. (2005). Experience-dependent modulation of C. elegans behavior by ambient oxygen. Curr. Biol.15, 905–917.10.1016/j.cub.2005.04.017

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 44

  ChiuS. L.ChenC. M.ClineH. T. (2008). Insulin receptor signaling regulates synapse number, dendritic plasticity, and circuit function in vivo. Neuron58, 708–719.10.1016/j.neuron.2008.04.014

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 45

  ChoS. I.NamY. S.ChuL. Y.LeeJ. H.BangJ. S.KimH. R.et al (2012). Extremely low-frequency magnetic fields modulate nitric oxide signaling in rat brain. Bioelectromagnetics33, 568–574.10.1002/bem.21715

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 46

  ChoiW. S.EomD. S.HanB. S.KimW. K.HanB. H.ChoiE. J.et al (2004). Phosphorylation of p38 MAPK induced by oxidative stress is linked to activation of both caspase-8-and-9-mediated apoptotic pathways in dopaminergic neurons. J. Biol. Chem.279, 20451–20460.10.1074/jbc.M406831200

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 47

  ChongZ. Z.ShangY. C.ZhangL.WangS.MaieseK. (2010). Mammalian target of rapamycin: hitting the bull’s-eye for neurological disorders. Oxid. Med. Cell. Longev.3, 374–391.10.4161/oxim.3.6.14787

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 48

  ChowA. M.BrownI. R. (2007). Induction of heat shock proteins in differentiated human and rodent neurons by celastrol. Cell Stress Chaperones12, 237–244.10.1379/CSC-269.1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 49

  ClarkD. A.GabelC. V.GabelH.SamuelA. D. (2007). Temporal activity patterns in thermosensory neurons of freely moving Caenorhabditis elegans encode spatial thermal gradients. J. Neurosci.27, 6083–6090.10.1523/JNEUROSCI.1032-07.2007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 50

  ContestabileA. (2008). Regulation of transcription factors by nitric oxide in neurons and in neural-derived tumor cells. Prog. Neurobiol.84, 317–328.10.1016/j.pneurobio.2008.01.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 51

  CornilsA.GloeckM.ChenZ.ZhangY.AlcedoJ. (2011). Specific insulin-like peptides encode sensory information to regulate distinct developmental processes. Development138, 1183–1193.10.1242/dev.060905

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 52

  CostelloD. A.ClaretM.Al-QassabH.PlattnerF.IrvineE. E.ChoudhuryA. I.et al (2012). Brain deletion of insulin receptor substrate 2 disrupts hippocampal synaptic plasticity and metaplasticity. PLoS One7, e31124.10.1371/journal.pone.0031124

  • CrossRef
  • Google Scholar

• 53

  CoyleJ. T.PuttfarckenP. (1993). Oxidative stress, glutamate, and neurodegenerative disorders. Science262, 689–695.10.1126/science.7901908

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 54

  CulmseeC.MattsonM. P. (2005). p53 in neuronal apoptosis. Biochem. Biophys. Res. Commun.331, 761–777.10.1016/j.bbrc.2005.03.149

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 55

  DalfoD.MichaelsonD.HubbardE. J. (2012). Sensory regulation of the C. elegans germline through TGF-beta-dependent signaling in the niche. Curr. Biol.22, 712–719.10.1016/j.cub.2012.02.064

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 56

  Dawson-ScullyK.Meldrum RobertsonR. (1998). Heat shock protects synaptic transmission in flight motor circuitry of locusts. Neuroreport9, 2589–2593.10.1097/00001756-199808030-00030

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 57

  DhakaA.ViswanathV.PatapoutianA. (2006). Trp ion channels and temperature sensation. Annu. Rev. Neurosci.29, 135–161.10.1146/annurev.neuro.29.051605.112958

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 58

  DhillonA. S.HaganS.RathO.KolchW. (2007). MAP kinase signalling pathways in cancer. Oncogene26, 3279–3290.10.1038/sj.onc.1210421

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 59

  DirksR. P.Van GeelR.HensenS. M.Van GenesenS. T.LubsenN. H. (2010). Manipulating heat shock factor-1 in Xenopus tadpoles: neuronal tissues are refractory to exogenous expression. PLoS ONE5, e10158.10.1371/journal.pone.0010158

  • CrossRef
  • Google Scholar

• 60

  Domanska-JanikK.BongP.Bronisz-KowalczykA.ZajacH.ZablockaB. (1999). AP1 transcriptional factor activation and its relation to apoptosis of hippocampal CA1 pyramidal neurons after transient ischemia in gerbils. J. Neurosci. Res.57, 840–846.10.1002/(SICI)1097-4547(19990915)57:6<840::AID-JNR9>3.3.CO;2-Q

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 61

  DoonanR.McElweeJ. J.MatthijssensF.WalkerG. A.HouthoofdK.BackP.et al (2008). Against the oxidative damage theory of aging: superoxide dismutases protect against oxidative stress but have little or no effect on life span in Caenorhabditis elegans. Genes Dev.22, 3236–3241.10.1101/gad.504808

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 62

  DuanH.WearneS. L.RocherA. B.MacedoA.MorrisonJ. H.HofP. R. (2003). Age-related dendritic and spine changes in corticocortically projecting neurons in macaque monkeys. Cereb. Cortex13, 950–961.10.1093/cercor/13.9.950

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 63

  DunwoodieS. L. (2009). The role of hypoxia in development of the mammalian embryo. Dev. Cell17, 755–773.10.1016/j.devcel.2009.11.008

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 64

  DurieuxJ.WolffS.DillinA. (2011). The cell-non-autonomous nature of electron transport chain-mediated longevity. Cell144, 79–91.10.1016/j.cell.2010.12.016

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 65

  EbertM. S.SharpP. A. (2012). Roles for MicroRNAs in conferring robustness to biological processes. Cell149, 515–524.10.1016/j.cell.2012.04.005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 66

  EmotoK.ParrishJ. Z.JanL. Y.JanY. N. (2006). The tumour suppressor Hippo acts with the NDR kinases in dendritic tiling and maintenance. Nature443, 210–213.10.1038/nature05090

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 67

  EpsteinA. C. R.GleadleJ. M.McNeillL. A.HewitsonK. S.O’rourkeJ.MoleD. R.et al (2001). C-elegans EGL-9 and mammalian homologs define a family of dioxygenases that regulate HIF by prolyl hydroxylation. Cell107, 43–54.10.1016/S0092-8674(01)00507-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 68

  EvansT. G.YamamotoY.JefferyW. R.KroneP. H. (2005). Zebrafish Hsp70 is required for embryonic lens formation. Cell Stress Chaperones10, 66–78.10.1379/CSC-79R.1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 69

  FernandezA. M.Torres-AlemanI. (2012). The many faces of insulin-like peptide signalling in the brain. Nat. Rev. Neurosci.13, 225–239.10.1038/nrn3209

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 70

  FischerH. G.MorawskiM.BrucknerM. K.MittagA.TarnokA.ArendtT. (2012). Changes in neuronal DNA content variation in the human brain during aging. Aging Cell11, 628–633.10.1111/j.1474-9726.2012.00826.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 71

  FreudeS.SchilbachK.HettichM. M.BronnekeH. S.ZemvaJ.KroneW.et al (2012). Neuron-specific deletion of a single copy of the insulin-like growth factor-1 receptor gene reduces fat accumulation during aging. Horm. Metab. Res.44, 99–104.10.1055/s-0031-1298018

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 72

  FukunagaK.MiyamotoE. (1998). Role of MAP kinase in neurons. Mol. Neurobiol.16, 79–95.10.1007/BF02740604

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 73

  GanL.MuckeL. (2008). Paths of convergence: sirtuins in aging and neurodegeneration. Neuron58, 10–14.10.1016/j.neuron.2008.03.015

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 74

  GarciaS. M.CasanuevaM. O.SilvaM. C.AmaralM. D.MorimotoR. I. (2007). Neuronal signaling modulates protein homeostasis in Caenorhabditis elegans post-synaptic muscle cells. Genes Dev.21, 3006–3016.10.1101/gad.1575307

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 75

  GehartH.KumpfS.IttnerA.RicciR. (2010). MAPK signalling in cellular metabolism: stress or wellness?EMBO Rep.11, 834–840.10.1038/embor.2010.160

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 76

  GerschmanR.GilbertD. L.NyeS. W.DwyerP.FennW. O. (1954). Oxygen poisoning and x-irradiation: a mechanism in common. Science119, 623–626.10.1126/science.119.3097.623

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 77

  GhaziA.Henis-KorenblitS.KenyonC. (2009). A transcription elongation factor that links signals from the reproductive system to lifespan extension in Caenorhabditis elegans. PLoS Genet.5, e1000639.10.1371/journal.pgen.1000639

  • CrossRef
  • Google Scholar

• 78

  GhiglieriV.PendolinoV.BagettaV.SgobioC.CalabresiP.PicconiB. (2010). mTOR inhibitor rapamycin suppresses striatal post-ischemic LTP. Exp. Neurol.226, 328–331.10.1016/j.expneurol.2010.09.012

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 79

  GozzoY.VohrB.LacadieC.HampsonM.KatzK. H.Maller-KesselmanJ.et al (2009). Alterations in neural connectivity in preterm children at school age. Neuroimage48, 458–463.10.1016/j.neuroimage.2009.06.046

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 80

  GrimmC.HermannD. M.BogdanovaA.HotopS.KilicU.WenzelA.et al (2005). Neuroprotection by hypoxic preconditioning: HIF-1 and erythropoietin protect from retinal degeneration. Semin. Cell Dev. Biol.16, 531–538.10.1016/j.semcdb.2005.03.004

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 81

  GuoG.BhatN. R. (2007). p38alpha MAP kinase mediates hypoxia-induced motor neuron cell death: a potential target of minocycline’s neuroprotective action. Neurochem. Res.32, 2160–2166.10.1007/s11064-007-9408-8

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 82

  HaltermanM. W.GillM.DejesusC.OgiharaM.SchorN. F.FederoffH. J. (2010). The endoplasmic reticulum stress response factor CHOP-10 protects against hypoxia-induced neuronal death. J. Biol. Chem.285, 21329–21340.10.1074/jbc.M109.095299

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 83

  HammarlundM.NixP.HauthL.JorgensenE. M.BastianiM. (2009). Axon regeneration requires a conserved MAP kinase pathway. Science323, 802–806.10.1126/science.1165527

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 84

  HarmanD. (1956). Aging: a theory based on free radical and radiation chemistry. J. Gerontol.11, 298–300.

  • Pubmed Abstract
  • Google Scholar

• 85

  HarrisonD. E.StrongR.SharpZ. D.NelsonJ. F.AstleC. M.FlurkeyK.et al (2009). Rapamycin fed late in life extends lifespan in genetically heterogeneous mice. Nature460, 392–395.

  • Pubmed Abstract
  • Google Scholar

• 86

  HavrankovaJ.RothJ.BrownsteinM. (1978). Insulin receptors are widely distributed in the central nervous system of the rat. Nature272, 827–829.10.1038/272827a0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 87

  HayflickL. (2007). Entropy explains aging, genetic determinism explains longevity, and undefined terminology explains misunderstanding both. PLoS Genet.3, e220.10.1371/journal.pgen.0030220

  • CrossRef
  • Google Scholar

• 88

  HekimiS.LapointeJ.WenY. (2011). Taking a “good” look at free radicals in the aging process. Trends Cell Biol.21, 569–576.10.1016/j.tcb.2011.06.008

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 89

  HendersonC. E. (1996). Role of neurotrophic factors in neuronal development. Curr. Opin. Neurobiol.6, 64–70.10.1016/S0959-4388(96)80010-9

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 90

  HerndonL. A.SchmeissnerP. J.DudaronekJ. M.BrownP. A.ListnerK. M.SakanoY.et al (2002). Stochastic and genetic factors influence tissue-specific decline in ageing C. elegans. Nature419, 808–814.10.1038/nature01135

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 91

  HerrupK. (2012). The contributions of unscheduled neuronal cell cycle events to the death of neurons in Alzheimer’s disease. Front. Biosci. (Elite Ed.)4, 2101–2109.10.2741/527

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 92

  HerrupK.NeveR.AckermanS. L.CopaniA. (2004). Divide and die: cell cycle events as triggers of nerve cell death. J. Neurosci.24, 9232–9239.10.1523/JNEUROSCI.3347-04.2004

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 93

  HoefferC. A.KlannE. (2010). mTOR signaling: at the crossroads of plasticity, memory and disease. Trends Neurosci.33, 67–75.10.1016/j.tins.2009.11.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 94

  HoozemansJ. J.ScheperW. (2012). Endoplasmic reticulum: the unfolded protein response is tangled in neurodegeneration. Int. J. Biochem. Cell Biol.44, 1295–1298.10.1016/j.biocel.2012.04.023

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 95

  HorstmannS.KahleP. J.BorasioG. D. (1998). Inhibitors of p38 mitogen-activated protein kinase promote neuronal survival in vitro. J. Neurosci. Res.52, 483–490.10.1002/(SICI)1097-4547(19980515)52:4<483::AID-JNR12>3.0.CO;2-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 96

  HsuA. L.MurphyC. T.KenyonC. (2003). Regulation of aging and age-related disease by DAF-16 and heat-shock factor. Science300, 1142–1145.10.1126/science.1083701

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 97

  HungC. W.ChenY. C.HsiehW. L.ChiouS. H.KaoC. L. (2010). Ageing and neurodegenerative diseases. Ageing Res. Rev.9(Suppl. 1), S36–S46.10.1016/j.arr.2010.08.006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 98

  HussonS. J.MertensI.JanssenT.LindemansM.SchoofsL. (2007). Neuropeptidergic signaling in the nematode Caenorhabditis elegans. Prog. Neurobiol.82, 33–55.10.1016/j.pneurobio.2007.01.006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 99

  HwangA. B.LeeS. J. (2011). Regulation of life span by mitochondrial respiration: the HIF-1 and ROS connection. Aging (Albany NY)3, 304–310.

  • Pubmed Abstract
  • Google Scholar

• 100

  IdeF.IidaN.NakatsuruY.OdaH.NikaidoO.IshikawaT. (2000). In vivo detection of ultraviolet photoproducts and their repair in Purkinje cells. Lab. Invest.80, 465–470.

  • Pubmed Abstract
  • Google Scholar

• 101

  IkonomidouC.KaindlA. M. (2011). Neuronal death and oxidative stress in the developing brain. Antioxid. Redox Signal.14, 1535–1550.10.1089/ars.2010.3581

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 102

  IzumiN.YamashitaA.OhnoS. (2012). Integrated regulation of PIKK-mediated stress responses by AAA+ proteins RUVBL1 and RUVBL2. Nucleus3, 29–43.10.4161/nucl.18926

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 103

  JaworskiJ.ShengM. (2006). The growing role of mTOR in neuronal development and plasticity. Mol. Neurobiol.34, 205–219.10.1385/MN:34:3:205

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 104

  JensenH. A.LoukogeorgakisS.YannopoulosF.RimpilainenE.PetzoldA.TuominenH.et al (2011). Remote ischemic preconditioning protects the brain against injury after hypothermic circulatory arrest. Circulation123, 714–721.10.1161/CIRCULATIONAHA.110.986497

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 105

  JeongJ. K.SeoJ. S.MoonM. H.LeeY. J.SeolJ. W.ParkS. Y. (2012). Hypoxia-inducible factor-1 alpha regulates prion protein expression to protect against neuron cell damage. Neurobiol. Aging33, 1006 e1001–1010.10.1016/j.neurobiolaging.2011.09.037

  • CrossRef
  • Google Scholar

• 106

  JiangH.HuangY.XuH.SunY.HanN.LiQ. F. (2012). Hypoxia inducible factor-1alpha is involved in the neurodegeneration induced by isoflurane in the brain of neonatal rats. J. Neurochem.120, 453–460.10.1111/j.1471-4159.2011.07589.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 107

  JohnsonR. P.KramerJ. M. (2012). Neural maintenance roles for the matrix receptor dystroglycan and the nuclear anchorage complex in Caenorhabditis elegans. Genetics190, 1365–1377.10.1534/genetics.111.136184

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 108

  JollyS.JourniacN.NaudetF.GautheronV.MarianiJ.Vernet-Der GarabedianB. (2011). Cell-autonomous and non-cell-autonomous neuroprotective functions of RORalpha in neurons and astrocytes during hypoxia. J. Neurosci.31, 14314–14323.10.1523/JNEUROSCI.1443-11.2011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 109

  KameyamaY.InouyeM. (1994). Irradiation injury to the developing nervous system: mechanisms of neuronal injury. Neurotoxicology15, 75–80.

  • Pubmed Abstract
  • Google Scholar

• 110

  KappelerL.FilhoC. D. M.DupontJ.LeneuveP.CerveraP.PerinL.et al (2008). Brain IGF-1 receptors control mammalian growth and lifespan through a neuroendocrine mechanism. PLoS Biol.6, e254.10.1371/journal.pbio.0060254

  • CrossRef
  • Google Scholar

• 111

  KarunanithiS.BarclayJ. W.RobertsonR. M.BrownI. R.AtwoodH. L. (1999). Neuroprotection at Drosophila synapses conferred by prior heat shock. J. Neurosci.19, 4360–4369.

  • Pubmed Abstract
  • Google Scholar

• 112

  KatoH.ArakiT.ItoyamaY.KogureK.KatoK. (1995). An immunohistochemical study of heat shock protein-27 in the hippocampus in a gerbil model of cerebral ischemia and ischemic tolerance. Neuroscience68, 65–71.10.1016/0306-4522(95)00141-5

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 113

  KatsunoM.SangC.AdachiH.MinamiyamaM.WazaM.TanakaF.et al (2005). Pharmacological induction of heat-shock proteins alleviates polyglutamine-mediated motor neuron disease. Proc. Natl. Acad. Sci. U.S.A.102, 16801–16806.10.1073/pnas.0506249102

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 114

  KenyonC.ChangJ.GenschE.RudnerA.TabtiangR. (1993). A C-elegans mutant that lives twice as long as wild-type. Nature366, 461–464.10.1038/366461a0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 115

  KernA.AckermannB.ClementA. M.DuerkH.BehlC. (2010). HSF1-controlled and age-associated chaperone capacity in neurons and muscle cells of C. elegans. PLoS ONE5, e8568.10.1371/journal.pone.0008568

  • CrossRef
  • Google Scholar

• 116

  KeswaniS. C.Bosch-MarceM.ReedN.FischerA.SemenzaG. L.HokeA. (2011). Nitric oxide prevents axonal degeneration by inducing HIF-1-dependent expression of erythropoietin. Proc. Natl. Acad. Sci. U.S.A.108, 4986–4990.10.1073/pnas.1019591108

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 117

  KimuraK. D.TissenbaumH. A.LiuY. X.RuvkunG. (1997). daf-2, an insulin receptor-like gene that regulates longevity and diapause in Caenorhabditis elegans. Science277, 942–946.10.1126/science.277.5328.942

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 118

  KirkwoodT. B. L.AustadS. N. (2000). Why do we age?Nature408, 233–238.10.1038/35041682

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 119

  KitagawaK.MatsumotoM.KuwabaraK.TagayaM.OhtsukiT.HataR.et al (1991). Ischemic tolerance phenomenon detected in various brain-regions. Brain Res.561, 203–211.10.1016/0006-8993(91)91596-S

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 120

  KlineD. D.Ramirez-NavarroA.KunzeD. L. (2007). Adaptive depression in synaptic transmission in the nucleus of the solitary tract after in vivo chronic intermittent hypoxia: evidence for homeostatic plasticity. J. Neurosci.27, 4663–4673.10.1523/JNEUROSCI.4946-06.2007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 121

  KlyachkoV. A.StevensC. F. (2006). Temperature-dependent shift of balance among the components of short-term plasticity in hippocampal synapses. J. Neurosci.26, 6945–6957.10.1523/JNEUROSCI.1382-06.2006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 122

  KonnerA. C.HessS.TovarS.MesarosA.Sanchez-LasherasC.EversN.et al (2011). Role for insulin signaling in catecholaminergic neurons in control of energy homeostasis. Cell Metab.13, 720–728.10.1016/j.cmet.2011.03.021

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 123

  KourtisN.NikoletopoulouV.TavernarakisN. (2012). Small heat-shock proteins protect from heat-stroke-associated neurodegeneration. Nature490, 213–218.10.1038/nature11417

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 124

  KourtisN.TavernarakisN. (2011). Cellular stress response pathways and ageing: intricate molecular relationships. EMBO J.30, 2520–2531.10.1038/emboj.2011.162

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 125

  KrumanI. I.WerstoR. P.Cardozo-PelaezF.SmilenovL.ChanS. L.ChrestF. J.et al (2004). Cell cycle activation linked to neuronal cell death initiated by DNA damage. Neuron41, 549–561.10.1016/S0896-6273(04)00017-0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 126

  KuangS.GoldbergJ. I. (2001). Laser ablation reveals regulation of ciliary activity by serotonergic neurons in molluscan embryos. J. Neurobiol.47, 1–15.10.1002/neu.1011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 127

  KuangS. H.DoranS. A.WilsonR. J. A.GossG. G.GoldbergJ. I. (2002). Serotonergic sensory-motor neurons mediate a behavioral response to hypoxia in pond snail embryos. J. Neurobiol.52, 73–83.10.1002/neu.10071

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 128

  LagerwerfS.VrouweM. G.OvermeerR. M.FousteriM. I.MullendersL. H. (2011). DNA damage response and transcription. DNA Repair (Amst.)10, 743–750.10.1016/j.dnarep.2011.04.024

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 129

  LeDouxS. P.DruzhynaN. M.HollensworthS. B.HarrisonJ. F.WilsonG. L. (2007). Mitochondrial DNA repair: a critical player in the response of cells of the CNS to genotoxic insults. Neuroscience145, 1249–1259.10.1016/j.neuroscience.2006.10.002

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 130

  LeeK. S.Iijima-AndoK.IijimaK.LeeW. J.LeeJ. H.YuK.et al (2009). JNK/FOXO-mediated neuronal expression of fly homologue of peroxiredoxin II reduces oxidative stress and extends life span. J. Biol. Chem.284, 29454–29461.10.1074/jbc.C900014200

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 131

  LeeS. J.HwangA. B.KenyonC. (2010). Inhibition of respiration extends C. elegans life span via reactive oxygen species that increase HIF-1 activity. Curr. Biol.20, 2131–2136.10.1016/j.cub.2009.12.021

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 132

  LeeS. J.JikoC.YamashitaE.TsukiharaT. (2011). Selective nuclear export mechanism of small RNAs. Curr. Opin. Struct. Biol.21, 101–108.10.1016/j.sbi.2010.11.004

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 133

  LeeS. J.KenyonC. (2009). Regulation of the longevity response to temperature by thermosensory neurons in Caenorhabditis elegans. Curr. Biol.19, 715–722.10.1016/j.cub.2009.03.041

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 134

  LeeS. S.KennedyS.TolonenA. C.RuvkunG. (2003a). DAF-16 target genes that control C-elegans life-span and metabolism. Science300, 644–647.10.1126/science.1081846

  • CrossRef
  • Google Scholar

• 135

  LeeY.AhnC.HanJ.ChoiH.KimJ.YimJ.et al (2003b). The nuclear RNase III Drosha initiates microRNA processing. Nature425, 415–419.10.1038/nature01957

  • CrossRef
  • Google Scholar

• 136

  LeeY.JeonK.LeeJ. T.KimS.KimV. N. (2002). MicroRNA maturation: stepwise processing and subcellular localization. EMBO J.21, 4663–4670.10.1093/emboj/21.11.2692

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 137

  LeeY.McKinnonP. J. (2007). Responding to DNA double strand breaks in the nervous system. Neuroscience145, 1365–1374.10.1016/j.neuroscience.2006.07.026

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 138

  LeiserS. F.BegunA.KaeberleinM. (2011). HIF-1 modulates longevity and healthspan in a temperature-dependent manner. Aging Cell10, 318–326.10.1111/j.1474-9726.2011.00672.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 139

  LiC.HisamotoN.NixP.KanaoS.MizunoT.BastianiM.et al (2012). The growth factor SVH-1 regulates axon regeneration in C. elegans via the JNK MAPK cascade. Nat. Neurosci.15, 551–557.10.1038/nn.3126

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 140

  LiD.BaiT.BrorsonJ. R. (2011). Adaptation to moderate hypoxia protects cortical neurons against ischemia-reperfusion injury and excitotoxicity independently of HIF-1alpha. Exp. Neurol.230, 302–310.10.1016/j.expneurol.2011.05.009

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 141

  LiJ. L.HanY. R.PlummerM. R.HerrupK. (2009a). Cytoplasmic ATM in neurons modulates synaptic function. Curr. Biol.19, 2091–2096.10.1016/j.cub.2009.10.039

  • CrossRef
  • Google Scholar

• 142

  LiX.CassidyJ. J.ReinkeC. A.FischboeckS.CarthewR. W. (2009b). A microRNA imparts robustness against environmental fluctuation during development. Cell137, 273–282.10.1016/j.cell.2009.01.058

  • CrossRef
  • Google Scholar

• 143

  LiW. Q.KennedyS. G.RuvkunG. (2003). daf-28 encodes a C-elegans insulin superfamily member that is regulated by environmental cues and acts in the DAF-2 signaling pathway. Genes Dev.17, 844–858.10.1101/gad.1066503

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 144

  LiY.ChoppM.PowersC.JiangN. (1997). Immunoreactivity of cyclin D1/cdk4 in neurons and oligodendrocytes after focal cerebral ischemia in rat. J. Cereb. Blood Flow Metab.17, 846–856.

  • Pubmed Abstract
  • Google Scholar

• 145

  LiY. Q.GuoY. P.JayV.StewartP. A.WongC. S. (1996). Time course of radiation-induced apoptosis in the adult rat spinal cord. Radiother. Oncol.39, 35–42.10.1016/0167-8140(96)87941-2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 146

  LibertS.ZwienerJ.ChuX.VanvoorhiesW.RomanG.PletcherS. D. (2007). Regulation of Drosophila life span by olfaction and food-derived odors. Science315, 1133–1137.10.1126/science.1136610

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 147

  LinK.HsinH.LibinaN.KenyonC. (2001). Regulation of the Caenorhabditis elegans longevity protein DAF-16 by insulin/IGF-1 and germline signaling. Nat. Genet.28, 139–145.10.1038/88850

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 148

  LiptonP. (1999). Ischemic cell death in brain neurons. Physiol. Rev.79, 1431–1568.

  • Pubmed Abstract
  • Google Scholar

• 149

  LithgowG. J.WhiteT. M.MelovS.JohnsonT. E. (1995). Thermotolerance and extended life-span conferred by single-gene mutations and induced by thermal stress. Proc. Natl. Acad. Sci. U.S.A.92, 7540–7544.10.1073/pnas.92.16.7540

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 150

  LiuS.SchulzeE.BaumeisterR. (2012). Temperature- and touch-sensitive neurons couple CNG and TRPV channel activities to control heat avoidance in Caenorhabditis elegans. PLoS ONE7, e32360.10.1371/journal.pone.0032360

  • CrossRef
  • Google Scholar

• 151

  LiuW.D’ercoleJ. A.YeP. (2011). Blunting type 1 insulin-like growth factor receptor expression exacerbates neuronal apoptosis following hypoxic/ischemic injury. BMC Neurosci.12, 64.10.1186/1471-2202-12-64

  • CrossRef
  • Google Scholar

• 152

  LiuX. D.LiuP. C.SantoroN.ThieleD. J. (1997). Conservation of a stress response: human heat shock transcription factors functionally substitute for yeast HSF. EMBO J.16, 6466–6477.10.1093/emboj/16.21.6466

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 153

  LiuY.KatoH.NakataN.KogureK. (1993). Temporal profile of heat shock protein 70 synthesis in ischemic tolerance induced by preconditioning ischemia in rat hippocampus. Neuroscience56, 921–927.10.1016/0306-4522(93)90138-6

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 154

  LoonesM. T.RalluM.MezgerV.MorangeM. (1997). HSP gene expression and HSF2 in mouse development. Cell Mol. Life Sci.53, 179–190.10.1007/PL00000590

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 155

  Lopez-HernandezB.PosadasI.PodlesniyP.AbadM. A.TrullasR.CenaV. (2012). HIF-1alpha is neuroprotective during the early phases of mild hypoxia in rat cortical neurons. Exp. Neurol.233, 543–554.10.1016/j.expneurol.2011.11.040

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 156

  LuT.PanY.KaoS. Y.LiC.KohaneI.ChanJ.et al (2004). Gene regulation and DNA damage in the ageing human brain. Nature429, 883–891.10.1038/nature02661

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 157

  MaD. K.VozdekR.BhatlaN.HorvitzH. R. (2012). CYSL-1 interacts with the O2-sensing hydroxylase EGL-9 to promote H2S-modulated hypoxia-induced behavioral plasticity in C. elegans. Neuron73, 925–940.10.1016/j.neuron.2011.12.037

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 158

  MajmundarA. J.WongW. J.SimonM. C. (2010). Hypoxia-inducible factors and the response to hypoxic stress. Mol. Cell40, 294–309.10.1016/j.molcel.2010.09.022

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 159

  MaltepeE.SimonM. C. (1998). Oxygen, genes, and development: an analysis of the role of hypoxic gene regulation during murine vascular development. J. Mol. Med. (Berl.)76, 391–401.10.1007/s001090050231

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 160

  MassaP. T.AleyasinH.ParkD. S.MaoX.BargerS. W. (2006). NFkappaB in neurons? The uncertainty principle in neurobiology. J. Neurochem.97, 607–618.10.1111/j.1471-4159.2006.03810.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 161

  MasudaH.HosokawaN.NagataK. (1998). Expression and localization of collagen-binding stress protein Hsp47 in mouse embryo development: comparison with types I and II collagen. Cell Stress Chaperones3, 256–264.10.1379/1466-1268(1998)003<0256:EALOCB>2.3.CO;2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 162

  MattsonM. P.ChengA. W. (2006). Neurohormetic phytochemicals: low-dose toxins that induce adaptive neuronal stress responses. Trends Neurosci.29, 632–639.10.1016/j.tins.2006.09.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 163

  McGahanL.HakimA. M.NakabeppuY.RobertsonG. S. (1998). Ischemia-induced CA1 neuronal death is preceded by elevated FosB and Jun expression and reduced NGFI-A and JunB levels. Mol. Brain Res.56, 146–161.10.1016/S0169-328X(98)00039-4

  • CrossRef
  • Google Scholar

• 164

  MehtaR.SteinkrausK. A.SutphinG. L.RamosF. J.ShamiehL. S.HuhA.et al (2009). Proteasomal regulation of the hypoxic response modulates aging in C. elegans. Science324, 1196–1198.10.1126/science.1173507

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 165

  MeltzerL. A.YabaluriR.DeisserothK. (2005). A role for circuit homeostasis in adult neurogenesis. Trends Neurosci.28, 653–660.10.1016/j.tins.2005.09.007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 166

  MillerB. A.PerezR. S.ShahA. R.GonzalesE. R.ParkT. S.GiddayJ. M. (2001). Cerebral protection by hypoxic preconditioning in a murine model of focal ischemia-reperfusion. Neuroreport12, 1663–1669.10.1097/00001756-200106130-00030

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 167

  MiskaE. A.Alvarez-SaavedraE.AbbottA. L.LauN. C.HellmanA. B.McGonagleS. M.et al (2007). Most Caenorhabditis elegans microRNAs are individually not essential for development or viability. PLoS Genet.3, e215.10.1371/journal.pgen.0030215

  • CrossRef
  • Google Scholar

• 168

  MorimotoR. I.KlineM. P.BimstonD. N.CottoJ. J. (1997). The heat-shock response: regulation and function of heat-shock proteins and molecular chaperones. Essays Biochem.32, 17–29.

  • Pubmed Abstract
  • Google Scholar

• 169

  MorleyJ. F.MorimotoR. I. (2004). Regulation of longevity in Caenorhabditis elegans by heat shock factor and molecular chaperones. Mol. Biol. Cell15, 657–664.10.1091/mbc.E03-07-0532

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 170

  MorrisonS. J.CseteM.GrovesA. K.MelegaW.WoldB.AndersonD. J. (2000). Culture in reduced levels of oxygen promotes clonogenic sympathoadrenal differentiation by isolated neural crest stem cells. J. Neurosci.20, 7370–7376.

  • Pubmed Abstract
  • Google Scholar

• 171

  MorrissG. M.NewD. A. (1979). Effect of oxygen concentration on morphogenesis of cranial neural folds and neural crest in cultured rat embryos. J. Embryol. Exp. Morphol.54, 17–35.

  • Pubmed Abstract
  • Google Scholar

• 172

  MorrowG.SamsonM.MichaudS.TanguayR. M. (2004). Overexpression of the small mitochondrial Hsp22 extends Drosophila life span and increases resistance to oxidative stress. FASEB J.18, 598–599.

  • Pubmed Abstract
  • Google Scholar

• 173

  MurakamiS. (2007). Caenorhabditis elegans as a model system to study aging of learning and memory. Mol. Neurobiol.35, 85–94.10.1007/BF02700625

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 174

  MurphyC. T.McCarrollS. A.BargmannC. I.FraserA.KamathR. S.AhringerJ.et al (2003). Genes that act downstream of DAF-16 to influence the lifespan of Caenorhabditis elegans. Nature424, 277–284.10.1038/nature01789

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 175

  NamgungU.XiaZ. G. (2000). Arsenite-induced apoptosis in cortical neurons is mediated by c-Jun N-terminal protein kinase 3 and p38 mitogen-activated protein kinase. J. Neurosci.20, 6442–6451.

  • Pubmed Abstract
  • Google Scholar

• 176

  Neumann-HaefelinE.QiW.FinkbeinerE.WalzG.BaumeisterR.HertweckM. (2008). SHC-1/p52Shc targets the insulin/IGF-1 and JNK signaling pathways to modulate life span and stress response in C. elegans. Genes Dev.22, 2721–2735.10.1101/gad.478408

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 177

  OdaS.TomiokaM.IinoY. (2011). Neuronal plasticity regulated by the insulin-like signaling pathway underlies salt chemotaxis learning in Caenorhabditis elegans. J. Neurophysiol.106, 301–308.10.1152/jn.01029.2010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 178

  O’DriscollC. M.GormanA. M. (2005). Hypoxia induces neurite outgrowth in PC12 cells that is mediated through adenosine A2A receptors. Neuroscience131, 321–329.10.1016/j.neuroscience.2004.11.015

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 179

  O’DriscollM.JeggoP. A. (2006). The role of double-strand break repair – insights from human genetics. Nat. Rev. Genet.7, 45–54.10.1038/nrm1830

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 180

  OhS. W.MukhopadhyayA.SvrzikapaN.JiangF.DavisR. J.TissenbaumH. A. (2005). JNK regulates lifespan in Caenorhabditis elegans by modulating nuclear translocation of forkhead transcription factor/DAF-16. Proc. Natl. Acad. Sci. U.S.A.102, 4494–4499.10.1073/pnas.0507346102

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 181

  PageT. L.EinsteinM.DuanH.HeY.FloresT.RolshudD.et al (2002). Morphological alterations in neurons forming corticocortical projections in the neocortex of aged Patas monkeys. Neurosci. Lett.317, 37–41.10.1016/S0304-3940(01)02428-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 182

  PanC. L.PengC. Y.ChenC. H.McIntireS. (2011). Genetic analysis of age-dependent defects of the Caenorhabditis elegans touch receptor neurons. Proc. Natl. Acad. Sci. U.S.A.108, 9274–9279.10.1073/pnas.1100316108

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 183

  ParkC. Y.ChoiY. S.McManusM. T. (2010). Analysis of microRNA knockouts in mice. Hum. Mol. Genet.19, R169–R175.10.1093/hmg/ddq367

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 184

  ParkD. S.LevineB.FerrariG.GreeneL. A. (1997). Cyclin dependent kinase inhibitors and dominant negative cyclin dependent kinase 4 and 6 promote survival of NGF-deprived sympathetic neurons. J. Neurosci.17, 8975–8983.

  • Pubmed Abstract
  • Google Scholar

• 185

  ParkD. S.MorrisE. J.PadmanabhanJ.ShelanskiM. L.GellerH. M.GreeneL. A. (1998). Cyclin-dependent kinases participate in death of neurons evoked by DNA-damaging agents. J. Cell Biol.143, 457–467.10.1083/jcb.143.2.457

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 186

  ParkE. C.GhoseP.ShaoZ. Y.YeQ.KangL. J.XuX. Z. S.et al (2012). Hypoxia regulates glutamate receptor trafficking through an HIF-independent mechanism. EMBO J.31, 1379–1393.10.1038/emboj.2012.44

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 187

  ParkJ.LiuA. Y. (2001). JNK phosphorylates the HSF1 transcriptional activation domain: role of JNK in the regulation of the heat shock response. J. Cell. Biochem.82, 326–338.10.1002/jcb.1163

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 188

  ParkesT. L.HillikerA. J.PhillipsJ. P. (1999). Motorneurons, reactive oxygen, and life span in Drosophila. Neurobiol. Aging20, 531–535.10.1016/S0197-4580(99)00086-X

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 189

  Pascual-LeoneA.FreitasC.ObermanL.HorvathJ. C.HalkoM.EldaiefM.et al (2011). Characterizing brain cortical plasticity and network dynamics across the age-span in health and disease with TMS-EEG and TMS-fMRI. Brain Topogr.24, 302–315.10.1007/s10548-011-0196-8

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 190

  PasquinelliA. E. (2012). Non-coding RNA microRNAs and their targets: recognition, regulation and an emerging reciprocal relationship. Nat. Rev. Genet.13, 271–282.

  • Pubmed Abstract
  • Google Scholar

• 191

  PenneyJ.TsurudomeK.LiaoE. H.ElazzouziF.LivingstoneM.GonzalezM.et al (2012). TOR is required for the retrograde regulation of synaptic homeostasis at the Drosophila neuromuscular junction. Neuron74, 166–178.10.1016/j.neuron.2012.01.030

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 192

  PierceS. B.CostaM.WisotzkeyR.DevadharS.HomburgerS. A.BuchmanA. R.et al (2001). Regulation of DAF-2 receptor signaling by human insulin and ins-1, a member of the unusually large and diverse C. elegans insulin gene family. Genes Dev.15, 672–686.10.1101/gad.867301

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 193

  PietrzykowskiA. Z.FriesenR. M.MartinG. E.PuigS. I.NowakC. L.WynneP. M.et al (2008). Posttranscriptional regulation of BK channel splice variant stability by miR-9 underlies neuroadaptation to alcohol. Neuron59, 274–287.10.1016/j.neuron.2008.05.032

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 194

  PocockR.HobertO. (2008). Oxygen levels affect axon guidance and neuronal migration in Caenorhabditis elegans. Nat. Neurosci.11, 894–900.10.1038/nn.2152

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 195

  PocockR.HobertO. (2010). Hypoxia activates a latent circuit for processing gustatory information in C. elegans. Nat. Neurosci.13, 610–614.10.1038/nn.2537

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 196

  PotterW. B.O’riordanK. J.BarnettD.OstingS. M.WagonerM.BurgerC.et al (2010). Metabolic regulation of neuronal plasticity by the energy sensor AMPK. PLoS ONE5, e8996.10.1371/journal.pone.0008996

  • CrossRef
  • Google Scholar

• 197

  PrabhakarN. R.PieramiciS. F.PremkumarD. R. D.KumarG. K.KalariaR. N. (1996). Activation of nitric oxide synthase gene expression by hypoxia in central and peripheral neurons. Mol. Brain Res.43, 341–346.10.1016/S0169-328X(96)00222-7

  • CrossRef
  • Google Scholar

• 198

  PrahladV.CorneliusT.MorimotoR. I. (2008). Regulation of the cellular heat shock response in Caenorhabditis elegans by thermosensory neurons. Science320, 811–814.10.1126/science.1156093

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 199

  PrahladV.MorimotoR. I. (2011). Neuronal circuitry regulates the response of Caenorhabditis elegans to misfolded proteins. Proc. Natl. Acad. Sci. U.S.A.108, 14204–14209.10.1073/pnas.1106557108

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 200

  QiuJ.GrafeM. R.SchmuraS. M.GlasgowJ. N.KentT. A.RassinD. K.et al (2001). Differential NF-kappa B regulation of bcl-x gene expression in hippocampus and basal forebrain in response to hypoxia. J. Neurosci. Res.64, 223–234.10.1002/jnr.1070.abs

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 201

  RamirezJ. M.ElsenF. P.RobertsonR. M. (1999). Long-term effects of prior heat shock on neuronal potassium currents recorded in a novel insect ganglion slice preparation. J. Neurophysiol.81, 795–802.

  • Pubmed Abstract
  • Google Scholar

• 202

  RamockiM. B.ZoghbiH. Y. (2008). Failure of neuronal homeostasis results in common neuropsychiatric phenotypes. Nature455, 912–918.10.1038/nature07457

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 203

  RichardM. B.TaylorS. R.GreerC. A. (2010). Age-induced disruption of selective olfactory bulb synaptic circuits. Proc. Natl. Acad. Sci. U.S.A.107, 15613–15618.10.1073/pnas.1007931107

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 204

  RobertsonA. B.KlunglandA.RognesT.LeirosI. (2009). DNA repair in mammalian cells: base excision repair: the long and short of it. Cell. Mol. Life Sci.66, 981–993.10.1007/s00018-009-8736-z

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 205

  RobertsonR. M. (2004). Modulation of neural circuit operation by prior environmental stress. Integr. Comp. Biol.44, 21–27.10.1093/icb/44.1.21

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 206

  RomeroA. A.GrossS. R.ChengK. Y.GoldsmithN. K.GellerH. M. (2003). An age-related increase in resistance to DNA damage-induced apoptotic cell death is associated with development of DNA repair mechanisms. J. Neurochem.84, 1275–1287.10.1046/j.1471-4159.2003.01629.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 207

  RordorfG.KoroshetzW. J.BonventreJ. V. (1991). Heat shock protects cultured neurons from glutamate toxicity. Neuron7, 1043–1051.10.1016/0896-6273(91)90348-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 208

  Rosas-BallinaM.TraceyK. J. (2009). The neurology of the immune system: neural reflexes regulate immunity. Neuron64, 28–32.10.1016/j.neuron.2009.09.039

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 209

  SahaR. N.GhoshA.PalenciaC. A.FungY. K.DudekS. M.PahanK. (2009). TNF-alpha preconditioning protects neurons via neuron-specific up-regulation of CREB-binding protein. J. Immunol.183, 2068–2078.10.4049/jimmunol.0990087

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 210

  SaitoK.KondoE.MatsushitaM. (2011). MicroRNA 130 family regulates the hypoxia response signal through the P-body protein DDX6. Nucleic Acids Res.39, 6086–6099.10.1093/nar/gkr194

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 211

  SakashitaT.TakanamiT.YanaseS.HamadaN.SuzukiM.KimuraT.et al (2010). Radiation biology of Caenorhabditis elegans: germ cell response, aging and behavior. J. Radiat. Res.51, 107–121.10.1269/jrr.09100

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 212

  SammetaN.McClintockT. S. (2010). Chemical stress induces the unfolded protein response in olfactory sensory neurons. J. Comp. Neurol.518, 1825–1836.10.1002/cne.22305

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 213

  SchulingkampR. J.PaganoT. C.HungD.RaffaR. B. (2000). Insulin receptors and insulin action in the brain: review and clinical implications. Neurosci. Biobehav. Rev.24, 855–872.10.1016/S0149-7634(00)00040-3

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 214

  SchulzT. J.ZarseK.VoigtA.UrbanN.BirringerM.RistowM. (2007). Glucose restriction extends Caenorhabditis elegans life span by inducing mitochondrial respiration and increasing oxidative stress. Cell Metabolism6, 280–293.10.1016/j.cmet.2007.08.011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 215

  ScottB. A.AvidanM. S.CrowderC. M. (2002). Regulation of hypoxic death in C. elegans by the insulin/IGF receptor homolog DAF-2. Science296, 2388–2391.10.1126/science.1072302

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 216

  SeebergE.EideL.BjorasM. (1995). The base excision repair pathway. Trends Biochem. Sci.20, 391–397.10.1016/S0968-0004(00)89086-6

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 217

  SendoelA.KohlerI.FellmannC.LoweS. W.HengartnerM. O. (2010). HIF-1 antagonizes p53-mediated apoptosis through a secreted neuronal tyrosinase. Nature465, 577–583.10.1038/nature09141

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 218

  ShamovskyI.NudlerE. (2008). New insights into the mechanism of heat shock response activation. Cell. Mol. Life Sci.65, 855–861.10.1007/s00018-008-7458-y

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 219

  ShaoG.ZhouW. H.GaoC. Y.ZhangR.LuG. W. (2007). The effect of hypoxia preconditioning no binding activity of HIF-1 on the HRE with EPO in the hippocampus of mice. Zhongguo Ying Yong Sheng Li Xue Za Zhi23, 1–4.

  • Pubmed Abstract
  • Google Scholar

• 220

  ShenL.HuY.CaiT.LinX.WangD. (2010a). Regulation of longevity by genes required for the functions of AIY interneuron in nematode Caenorhabditis elegans. Mech. Ageing Dev.131, 732–738.10.1016/j.mad.2010.10.005

  • CrossRef
  • Google Scholar

• 221

  ShenL. L.DuM.LinX. F.CaiT.WangD. Y. (2010b). Genes required for the functions of olfactory AWA neuron regulate the longevity of Caenorhabditis elegans in an insulin/IGF signaling-dependent fashion. Neurosci. Bull.26, 91–103.10.1007/s12264-010-0162-6

  • CrossRef
  • Google Scholar

• 222

  SherrinT.BlankT.TodorovicC. (2011). c-Jun N-terminal kinases in memory and synaptic plasticity. Rev. Neurosci.22, 403–410.

  • Pubmed Abstract
  • Google Scholar

• 223

  ShihA. Y.ImbeaultS.BarakauskasV.ErbH.JiangL.LiP.et al (2005). Induction of the Nrf2-driven antioxidant response confers neuroprotection during mitochondrial stress in vivo. J. Biol. Chem.280, 22925–22936.10.1074/jbc.M414635200

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 224

  ShiraiK.MizuiT.SuzukiY.KobayashiY.NakanoT.ShiraoT. (2006). Differential effects of x-irradiation on immature and mature hippocampal neurons in vitro. Neurosci. Lett.399, 57–60.10.1016/j.neulet.2006.01.048

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 225

  SimonM. C.KeithB. (2008). The role of oxygen availability in embryonic development and stem cell function. Nat. Rev. Mol. Cell Biol.9, 285–296.10.1038/nrm2354

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 226

  SimonM. C.Ramirez-BergeronD.MackF.HuC. J.PanY.MansfieldK. (2002). Hypoxia, HIFs, and cardiovascular development. Cold Spring Harb. Symp. Quant. Biol.67, 127–132.10.1101/sqb.2002.67.127

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 227

  SniderB. J.LobnerD.YamadaK. A.ChoiD. W. (1998). Conditioning heat stress reduces excitotoxic and apoptotic components of oxygen-glucose deprivation-induced neuronal death in vitro. J. Neurochem.70, 120–129.10.1046/j.1471-4159.1998.70010120.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 228

  StevensonT. J.TrinhT.KogelschatzC.FujimotoE.LushM. E.PiotrowskiT.et al (2012). Hypoxia disruption of vertebrate CNS pathfinding through EphrinB2 is rescued by magnesium. PLoS Genet.8, e1002638.10.1371/journal.pgen.1002638

  • CrossRef
  • Google Scholar

• 229

  StevesC. J.SpectorT. D.JacksonS. H. (2012). Ageing, genes, environment and epigenetics: what twin studies tell us now, and in the future. Age Ageing41, 581–586.10.1093/ageing/afs097

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 230

  StranahanA. M.MattsonM. P. (2012). Recruiting adaptive cellular stress responses for successful brain ageing. Nat. Rev. Neurosci.13, 209–216.

  • Pubmed Abstract
  • Google Scholar

• 231

  StuderL.CseteM.LeeS. H.KabbaniN.WalikonisJ.WoldB.et al (2000). Enhanced proliferation, survival, and dopaminergic differentiation of CNS precursors in lowered oxygen. J. Neurosci.20, 7377–7383.

  • Pubmed Abstract
  • Google Scholar

• 232

  TakahamaK.TomitaJ.UenoT.YamazakiM.KumeS.KumeK. (2012). Pan-neuronal knockdown of the c-Jun N-terminal Kinase (JNK) results in a reduction in sleep and longevity in Drosophila. Biochem. Biophys. Res. Commun.417, 807–811.10.1016/j.bbrc.2011.12.040

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 233

  TakedaK.IchijoH. (2002). Neuronal p38 MAPK signalling: an emerging regulator of cell fate and function in the nervous system. Genes Cells7, 1099–1111.10.1046/j.1365-2443.2002.00591.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 234

  TankE. M.RodgersK. E.KenyonC. (2011). Spontaneous age-related neurite branching in Caenorhabditis elegans. J. Neurosci.31, 9279–9288.10.1523/JNEUROSCI.6606-10.2011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 235

  TatarM.KopelmanA.EpsteinD.TuM. P.YinC. M.GarofaloR. S. (2001). A mutant Drosophila insulin receptor homolog that extends life-span and impairs neuroendocrine function. Science292, 107–110.10.1126/science.1057987

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 236

  Teixeira-CastroA.AilionM.JallesA.BrignullH. R.VilacaJ. L.DiasN.et al (2011). Neuron-specific proteotoxicity of mutant ataxin-3 in C. elegans: rescue by the DAF-16 and HSF-1 pathways. Hum. Mol. Genet.20, 2996–3009.10.1093/hmg/ddr203

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 237

  TianB.YangQ.MaoZ. (2009). Phosphorylation of ATM by Cdk5 mediates DNA damage signalling and regulates neuronal death. Nat. Cell Biol.11, 211–218.10.1038/ncb1829

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 238

  TimsitS.RiveraS.OuaghiP.GuischardF.TremblayE.Ben-AriY.et al (1999). Increased cyclin D1 in vulnerable neurons in the hippocampus after ischaemia and epilepsy: a modulator of in vivo programmed cell death?Eur. J. Neurosci.11, 263–278.10.1046/j.1460-9568.1999.00434.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 239

  TomiokaM.AdachiT.SuzukiH.KunitomoH.SchaferW. R.IinoY. (2006). The insulin/PI 3-kinase pathway regulates salt chemotaxis learning in Caenorhabditis elegans. Neuron51, 613–625.10.1016/j.neuron.2006.07.024

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 240

  TonokiA.DavisR. L. (2012). Aging impairs intermediate-term behavioral memory by disrupting the dorsal paired medial neuron memory trace. Proc. Natl. Acad. Sci. U.S.A.109, 6319–6324.10.1073/pnas.1118126109

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 241

  TurrigianoG. G.NelsonS. B. (2004). Homeostatic plasticity in the developing nervous system. Nat. Rev. Neurosci.5, 97–107.10.1038/nrn1327

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 242

  UngerJ.McNeillT. H.MoxleyR. T.IIIWhiteM.MossA.LivingstonJ. N. (1989). Distribution of insulin receptor-like immunoreactivity in the rat forebrain. Neuroscience31, 143–157.10.1016/0306-4522(89)90036-5

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 243

  Van EssenD. C. (1997). A tension-based theory of morphogenesis and compact wiring in the central nervous system. Nature385, 313–318.10.1038/385313a0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 244

  van HeemstD. (2010). Insulin, IGF-1 and longevity. Aging Dis.1, 147–157.

  • Pubmed Abstract
  • Google Scholar

• 245

  van HeemstD.BeekmanM.MooijaartS. P.HeijmansB. T.BrandtB. W.ZwaanB. J.et al (2005). Reduced insulin/IGF-1 signalling and human longevity. Aging Cell4, 79–85.10.1111/j.1474-9728.2005.00148.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 246

  Van RaamsdonkJ. M.HekimiS. (2010). Reactive oxygen species and aging in Caenorhabditis elegans: causal or casual relationship?Antioxid. Redox Signal.13, 1911–1953.10.1089/ars.2010.3215

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 247

  Van RaamsdonkJ. M.HekimiS. (2012). Superoxide dismutase is dispensable for normal animal lifespan. Proc. Natl. Acad. Sci. U.S.A.109, 5785–5790.10.1073/pnas.1116158109

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 248

  WaltonN. M.ShinR.TajindaK.HeusnerC. L.KoganJ. H.MiyakeS.et al (2012). Adult neurogenesis transiently generates oxidative stress. PLoS ONE7, e35264.10.1371/journal.pone.0035264

  • CrossRef
  • Google Scholar

• 249

  WangM. C.BohmannD.JasperH. (2005). JNK extends life span and limits growth by antagonizing cellular and organism-wide responses to insulin signaling. Cell121, 115–125.10.1016/j.cell.2005.02.030

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 250

  WestonC. R.DavisR. J. (2002). The JNK signal transduction pathway. Curr. Opin. Genet. Dev.12, 14–21.10.1016/S0959-437X(01)00258-1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 251

  WhiteJ. G.SouthgateE.ThomsonJ. N.BrennerS. (1986). The structure of the nervous system of the nematode Caenorhabditis elegans. Philos. Trans. R. Soc. Lond. B Biol. Sci.314, 1–340.10.1098/rstb.1986.0056

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 252

  WilliamsT.CourchetJ.ViolletB.BrenmanJ. E.PolleuxF. (2011). AMP-activated protein kinase (AMPK) activity is not required for neuronal development but regulates axogenesis during metabolic stress. Proc. Natl. Acad. Sci. U.S.A.108, 5849–5854.10.1073/pnas.1013660108

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 253

  WolkowC. A.KimuraK. D.LeeM. S.RuvkunG. (2000). Regulation of C. elegans life-span by insulinlike signaling in the nervous system. Science290, 147–150.10.1126/science.290.5489.147

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 254

  Woodruff-PakD. S.FoyM. R.AkopianG. G.LeeK. H.ZachJ.NguyenK. P.et al (2010). Differential effects and rates of normal aging in cerebellum and hippocampus. Proc. Natl. Acad. Sci. U.S.A.107, 1624–1629.10.1073/pnas.0914207107

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 255

  WuB. S.LeeJ. K.ThompsonK. M.WalkerV. K.MoyesC. D.RobertsonR. M. (2002). Anoxia induces thermotolerance in the locust flight system. J. Exp. Biol.205, 815–827.

  • Pubmed Abstract
  • Google Scholar

• 256

  WuB. S.WalkerV. K.RobertsonR. M. (2001). Heat shock-induced thermoprotection of action potentials in the locust flight system. J. Neurobiol.49, 188–199.10.1002/neu.1074

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 257

  WullschlegerS.LoewithR.HallM. N. (2006). TOR signaling in growth and metabolism. Cell124, 471–484.10.1016/j.cell.2006.01.016

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 258

  YanD.WuZ.ChisholmA. D.JinY. (2009). The DLK-1 kinase promotes mRNA stability and local translation in C. elegans synapses and axon regeneration. Cell138, 1005–1018.10.1016/j.cell.2009.06.023

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 259

  YanknerB. A.LuT.LoerchP. (2008). The aging brain. Annu. Rev. Pathol.3, 41–66.10.1146/annurev.pathmechdis.2.010506.092044

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 260

  YaoS.PengM.ZhuX.ChengM.QiX. (2007). Heat shock protein72 protects hippocampal neurons from apoptosis induced by chronic psychological stress. Int. J. Neurosci.117, 1551–1564.10.1080/00207450701239285

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 261

  YeW. Z.BlainS. W. (2010). S phase entry causes homocysteine-induced death while ataxia telangiectasia and Rad3 related protein functions anti-apoptotically to protect neurons. Brain133, 2295–2312.10.1093/brain/awq139

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 262

  YenK.PatelH. B.LublinA. L.MobbsC. V. (2009). SOD isoforms play no role in lifespan in ad lib or dietary restricted conditions, but mutational inactivation of SOD-1 reduces life extension by cold. Mech. Ageing Dev.130, 173–178.10.1016/j.mad.2008.11.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 263

  YiR.QinY.MacaraI. G.CullenB. R. (2003). Exportin-5 mediates the nuclear export of pre-microRNAs and short hairpin RNAs. Genes Dev.17, 3011–3016.10.1101/gad.1158803

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 264

  ZhangH.LandmannF.ZahreddineH.RodriguezD.KochM.LabouesseM. (2011a). A tension-induced mechanotransduction pathway promotes epithelial morphogenesis. Nature471, 99–103.10.1038/nature09765

  • CrossRef
  • Google Scholar

• 265

  ZhangX.ZabinskyR.TengY.CuiM.HanM. (2011b). microRNAs play critical roles in the survival and recovery of Caenorhabditis elegans from starvation-induced L1 diapause. Proc. Natl. Acad. Sci. U.S.A.108, 17997–18002.10.1073/pnas.1113884108

  • CrossRef
  • Google Scholar

• 266

  ZhangP.AbrahamV. S.KraftK. R.RabchevskyA. G.ScheffS. W.SwainJ. A. (2000). Hyperthermic preconditioning protects against spinal cord ischemic injury. Ann. Thorac. Surg.70, 1490–1495.10.1016/S0003-4975(00)01851-8

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 267

  ZhangY.ShaoZ.ZhaiZ.ShenC.Powell-CoffmanJ. A. (2009). The HIF-1 hypoxia-inducible factor modulates lifespan in C. elegans. PLoS ONE4, e6348.10.1371/journal.pone.0006348

  • CrossRef
  • Google Scholar

• 268

  ZhengS.ZuoZ. (2004). Isoflurane preconditioning induces neuroprotection against ischemia via activation of P38 mitogen-activated protein kinases. Mol. Pharmacol.65, 1172–1180.10.1124/mol.65.5.1172

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 269

  ZhouL.ZhuD. Y. (2009). Neuronal nitric oxide synthase: structure, subcellular localization, regulation, and clinical implications. Nitric Oxide20, 223–230.10.1016/j.niox.2009.03.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 270

  ZhouS. Y.Castro-MoureF.GoshgarianH. G. (2001). Activation of a latent respiratory motor pathway by stimulation of neurons in the medullary chemoreceptor area of the rat. Exp. Neurol.171, 176–184.10.1006/exnr.2001.7740

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 271

  ZhuJ.LiW.MaoZ. (2011). Cdk5: mediator of neuronal development, death and the response to DNA damage. Mech. Ageing Dev.132, 389–394.10.1016/j.mad.2011.04.011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 272

  ZiuM.FletcherL.RanaS.JimenezD. F.DigicayliogluM. (2011). Temporal differences in microRNA expression patterns in astrocytes and neurons after ischemic injury. PLoS ONE6, e14724.10.1371/journal.pone.0014724

  • CrossRef
  • Google Scholar