Dysregulation of Astrocytic Glutamine Transport in Acute Hyperammonemic Brain Edema

Abstract

Acute liver failure (ALF) impairs ammonia clearance from blood, which gives rise to acute hyperammonemia and increased ammonia accumulation in the brain. Since in brain glutamine synthesis is the only route of ammonia detoxification, hyperammonemia is as a rule associated with increased brain glutamine content (glutaminosis) which correlates with and contributes along with ammonia itself to hyperammonemic brain edema-associated with ALF. This review focuses on the effects of hyperammonemia on the two glutamine carriers located in the astrocytic membrane: Slc38a3 (SN1, SNAT3) and Slc7a6 (y + LAT2). We emphasize the contribution of the dysfunction of either of the two carriers to glutaminosis- related aspects of brain edema: retention of osmotically obligated water (Slc38a3) and induction of oxidative/nitrosative stress (Slc7a6). The changes in glutamine transport link glutaminosis- evoked mitochondrial dysfunction to oxidative-nitrosative stress as formulated in the “Trojan Horse” hypothesis.

Metabolic Characteristics of Glutamine in Mammalian Tissues: A Brief Account

The presence and roles of glutamine common to all mammalian tissues have been dealt with in many excellent reviews (Häussinger, 1990; Labow and Souba, 2000; Tapiero et al., 2002; Oehler and Roth, 2003; Bak et al., 2006; Hakvoort et al., 2017), and therefore are mentioned here only briefly. Glutamine is the most abundant free amino acid and accounts for ∼50% of the total free amino acids in the human body (Spodenkiewicz et al., 2016). In peripheral tissues, glutamine is most abundantly represented in muscles (more than 40% of the free amino acid pool) and blood plasma (more than 20%, concentrations ranging from 0.4 to 0.7 mM) (Bergström et al., 1974; Kuhn et al., 1999). Glutamine participates in a variety of metabolic pathways, thereby controlling an abundance of biological processes. Ubiquitously, it serves as a precursor of purines and pyrimidines, is involved in the synthesis of amino sugars, regulation of pH, glutathione homeostasis, energy production, etc. (Cory and Cory, 2006; Albrecht et al., 2010). Systemically, enhanced glutamine synthesis exerts beneficial effects on the immune system (Castell et al., 2004) or gut barrier (Krishna Rao, 2012; Wang et al., 2015). Glutamine also stimulates branched-chain amino acids catabolism in skeletal muscle (Mann et al., 2021).

Glutamine Functioning in the Brain Depends on Its Mobility

In the mammalian brain, glutamine is a conditionally essential amino acid, synthesized from glutamate and ammonia, in a reaction mediated by glutamine synthetase (GS), an enzyme overwhelmingly (Martinez-Hernandez et al., 1977), albeit not exclusively (Amaral et al., 2013), located in astrocytes. Astrocytic glutamine is a precursor of the releasable pool of the excitatory neurotransmitter amino acid glutamate and the inhibitory amino acid, γ-aminobutyric acid (GABA), a sequence of reactions characterized by rapid cellular turnover rates (Bak et al., 2006; Rose et al., 2013). Glutamine released by astrocytes is taken up by neurons. In the mitochondria of neurons, glutamine is transformed by phosphate-activated glutaminase (PAG) into glutamate, released as a neurotransmitter into the synaptic space, from where it is taken up by astrocytes, and conjugates with ammonia to form glutamine, coined the glutamine/glutamate cycle (GGC) (see reviews by Yudkoff et al., 2000; Rothman et al., 2003; Bak et al., 2006; Albrecht et al., 2010). Of note, a significant portion glutamate is not converted to glutamine, but is taken up by astrocytes undergoes oxidation subsequent to its conversion to TCA cycle intermediates (McKenna et al., 2016). A portion of glutamine not utilized in GGC leaves the brain via the blood-brain barrier (Hawkins and Viña, 2016; Zaragozá, 2020) or blood-CSF barrier (Dolgodilina et al., 2020), by a mechanism involving exchange with large neutral amino acids leucine or tryptophan (Mans et al., 1982; del Pino et al., 1995).

Transport of glutamine within GGC involves transporter members belonging to A and N transport systems that differ in their properties (Bröer, 2007; Leke and Schousboe, 2016). Of note, the issue of the specific, GGC-related roles of glutamine will not be dealt with here, as the effects of hyperammonemia-related excess of glutamine on amino acidergic neurotransmission have so far escaped conclusive elaboration. Here we focus on the implications of the involvement of glutamine in brain ammonia turnover. Because in the brain the urea cycle is incomplete, glutamine synthesis remains the only efficient route of ammonia neutralization and, along with glutamine efflux from the brain to blood, constitutes the critical mechanism for excreting excess ammonia (Cooper and Jeitner, 2016). Since an overwhelming proportion (up to 80%) of astrocytic glutamate is converted to glutamine, glutamate uptake is a critical factor in regulation of glutamine efflux (McKenna et al., 1996, 2016). In line with the above, under controlled ammonia load, glutamine transporters localized on the astrocytic side suffice with facilitated diffusion controlled by the intracellular concentration of glutamine. However, in the setting of ALF, or of acute hyperammonemia evoked by other causes, increased glutamine accumulation resulting from ammonia overload per se induces astrocytic swelling, which leads to the often-mortal cytotoxic brain edema. This issue will form a specific theme of the review.

Both ammonia detoxification and the GGC put high demands on the availability of glutamine at its destination loci and rapid escape from its locus of synthesis (Daikhin and Yudkoff, 2000; Schousboe et al., 2014). As discussed in further sections of this review, the escape routes are critical for preventing excessive, edema-inducing accumulation in astrocytes under conditions of ammonia overload. Intercellular mobility of glutamine is facilitated, by its extraordinary abundance in the extracellular space. While brain tissue glutamine concentrations are more or less equal to other amino acids, its concentrations in the extracellular fluid or the cerebrospinal fluid (∼0.5–1 mM) exceeds by one order of magnitude other amino acids in these compartments (Perry et al., 1975; Jacobson et al., 1985; Xu et al., 1998). Most importantly, glutamine mobility is secured by active, highly controlled transport between different cell types of the CNS, at the brain-blood and blood-CSF barrier, executed by glutamine transporters.

Cell Membrane Glutamine Transporting Systems

Glutamine membrane transporters belong to different protein families that differ in properties, and most of them also accept other neutral or cationic amino acids (Albrecht and Zielińska, 2019). Glutamine transporters share an affinity toward glutamine but show differences in transport modes concerning Na⁺ or H⁺ coupling. The cotransporters efficiently accumulate glutamine while antiporters determine the balance between glutamine and other amino acids. The most acknowledged glutamine transporters belong to the Slc1, 6, 7, and 38 families (Pochini et al., 2014). The pleiotropic role of glutamine may be a reason why glutamine transporters, belonging to several protein families, are both redundant and ubiquitous. In general, none of the proteins is unequivocally specific (Pochini et al., 2014). Glutamine transporter classification originally was based on functional properties, such as substrate specificity, ion and pH dependence, kinetics, and regulatory properties, and led to clustering the transporters in systems. In the mammalian brain, glutamine transport systems are classified into two distinct groups termed sodium-dependent (systems A, ASC, and N) and sodium-independent (system L and y + L). System A and system L, the first defined, indicate carriers’ “alanine-preference” and “leucine-preference,” respectively (Kanai and Endou, 2001; Solbu, 2010). The systems include one or even more transporters, still not identified as specific proteins, due to the difficulties in discriminating a single function in entire cells. Neither system A nor system N-mediated transport requires counter-transport of other amino acids and determines the actual net amino acid flux (Meier, 2002). Table 1 presents astrocyte-localized glutamine transporting moieties with their transport features and, so far identified, functional importance.

Glutamine Cell Membrane Transporters in Focus of This Review

We specifically focus in this review on the ammonia-induced changes in the operation of astrocytic glutamine transporters that, with the evidence presented, have a contributing impact on the development of brain edema in the setting of ALF. Among the glutamine transporting moieties present on the membranes of astrocytes (Table 1), two, according to current data (Table 2), have attracted attention in this context. One of these, Slc38a3, is responsible for effective egress of newly synthesized glutamine from astrocytes and, this is well suited to prevent its excessive intra-astrocytic accumulation. The other one, Slc7A6, promotes glutamine exchange for essential cationic amino acids including, arginine (Bröer et al., 2000).

Glutamine Transport in Astrocytic Mitochondria

Intracellular transport from cytoplasm to mitochondria is one other factor contributing to intracellular (especially intra-astrocytic) glutamine homeostasis. It was demonstrated before that glutamine enters through the mitochondrial outer membrane (Zalman et al., 1980) and passes through the inner mitochondrial membrane using the mitochondrial glutamine carrier (Matés et al., 2009). The transport has been characterized in peripheral mammalian tissues e.g., kidneys (Indiveri et al., 1998), liver (Kovacević et al., 1970; Kovacević and Bajin, 1982; Haussinger et al., 1985), and tumor cells (Molina et al., 1995). Recently, the SLC1A5 carrier variant transporting glutamine has been characterized in mitochondria of cancer cells (Yoo et al., 2020). Although its in-depth characterization in brain mitochondria is pending, there is firm evidence of a saturable, carrier-mediated transport of glutamine in both synaptic and non-synaptic, astrocytic mitochondria (Minn, 1982; Steib et al., 1986; Roberg, 1995; Dolińska et al., 1996). However, the molecular identity of mitochondrial glutamine transporter in control brain tissue has not yet been definitively revealed. Most interestingly glutamine uptake to mitochondrial fractions enriched in large, astrocytic mitochondria is strongly inhibited by histidine (Albrecht et al., 2000; Ziemińska et al., 2000a), and is coupled to its intra-mitochondrial degradation to glutamate and ammonia by PAG (Albrecht et al., 2000; Ziemińska et al., 2004).

Glutaminosis: A Consistent Neuropathological Component Of Hyperammonemic Encephalopathies

Hyperammonemia defines metabolic disorders characterized by elevated levels of ammonia in the blood. Hyperammonemia occurs in a course of many and often causally unrelated diseases, such as chronic and acute encephalopathy, Reye’s syndrome, congenital deficits in urea cycle enzymes (UCDs), uremic encephalopathy, diabetic encephalopathy, or hypoglycemic encephalopathy.

Typically and most frequently, hyperammonemia is a secondary complication of primary liver disease, a leading factor in hepatic encephalopathy (HE). HE is a multi-symptomatic neurological syndrome related to acute (drug-induced) or chronic (cirrhosis associated) liver failure, where blood-derived ammonia (Ong et al., 2003; Jayakumar and Norenberg, 2018), and blood-derived and endogenous inflammatory intermediates, are the key pathogens (Rodrigo et al., 2010; Coltart et al., 2013; Balzano et al., 2020).

By definition, in hyperammonemic encephalopathies circulating ammonia concentration is significantly increased, reaching high micromolar or even millimolar concentrations in UCDs (Michalak et al., 1996) and ALF patients (Clemmesen et al., 1999). However, biochemical analysis of these patients’ brain tissue, neuroimaging (Kreis et al., 1990; Binesh et al., 2005) and brain microdialysis (Bjerring et al., 2008) showed significantly increased cerebral glutamine concentrations, consistent with the conversion of ammonia into glutamine. While, this did not per se prove the pathogenic role of glutamine, more recent studies do. In patients with acute-upon-chronic liver failure, a condition where stable liver cirrhosis undergoes instant exacerbation, the severity of clinical symptoms correlated well with brain glutamine as quantitated by NMR (Laubenberger et al., 1997). In line with the above, in patients with hepatic coma awaiting liver transplantation, the brain’s extracellular level of glutamine measured by microdialysis correlated as faithfully as arterial blood ammonia with intracranial pressure (Tofteng et al., 2006). Of note, increased glutamine content in the extracellular space content is thought to faithfully reflect the excess of glutamine that leaves astrocytes (Bosman et al., 1992; Rao et al., 1995; Hilgier et al., 1999). Notably, the high activity of GS and efficient incorporation of ammonia into glutamine result in a large ammonia concentration gradient between the brain and blood, which, together with the pH difference between the brain (∼7.1) and blood (∼7.4), promotes the penetration of ammonia into the brain (Ott and Larsen, 2004).

Brain Edema: The Ultimate Phase of Acute Hyperammonemia

The most life-threatening complication associated with acute HE is cerebral edema, in extreme cases resulting in intracranial hypertension severe enough to cause a patient’s death by brain herniation (reviewed in Blei, 2007; Bosoi and Rose, 2013; Scott, 2013). It has been documented that in ALF patients, intracranial pressure positively correlates with arterial ammonia levels (Bernal et al., 2007). The cerebral edema development in ALF progresses quickly and remains the leading cause of high patient mortality (∼50–80% of deaths). To this date, no specific treatment of acute HE-associated brain edema and coma other than whole-body cooling is available (Vaquero and Blei, 2004).

Histopathologic evaluation of ALF patient’s brain tissue revealed characteristic features of brain edema encompassing alterations in the morphology of astrocyte and endothelial cells (Martinez, 1968; Norenberg, 1977; Kato et al., 1992). Increased number of vacuoles and thickened basement membrane were visible in the endothelial cells whereas, swollen astrocytes with swollen mitochondria in the cytoplasm, and enlarged basal membrane, were observed in regard to the astrocyte cell population (Martinez, 1968; Norenberg, 1977; Kato et al., 1992). Of note in this context, characteristic pathomorphologic features of astrocytes, with swollen nuclei, glycogen deposition, and margination of chromatin, known as Alzheimer type 2 astrocytosis, are observed irrespective of the duration of hyperammonemia and its origin (inherited vs. acquired) (Norenberg, 1987). Moreover, imaging studies based on T2-weighted MRI scans in patients with ALF displayed decreased value of an apparent diffusion coefficient, indicating an increase in intracellular water in the brain and the cytotoxic nature of brain edema in ALF (Chavarria et al., 2010). Morphological (Traber et al., 1987, 1989; Kato et al., 1989; Chadipiralla et al., 2012) and MRI-derived evidence obtained in animal models of ALF (Obara-Michlewska et al., 2018; Hamdani et al., 2021) corroborated with observations on patients, further supporting the cytotoxic mechanism of ALF-induced brain edema.

Acute Hyperammonemic Brain Edema Is Primarily Cytotoxic in Nature

By analogy to other edema-associated brain pathologies, the relative roles of cytotoxic and vasogenic factors in the development of brain edema associated with acute HE has long remained a matter of debate (Blei, 2007). In agreement with the long-held view that HE is primarily an “astrogliopathy” (Norenberg, 1987; Albrecht et al., 2010), current evidence supports its primarily cytotoxic nature, primarily reflecting swelling of astrocytes by mechanisms related to intracellular metabolic and ion imbalance and the ensuing intracellular accumulation of water (Haussinger and Schliess, 2008; Bémeur et al., 2016). The current view of edema pathophysiology, is that ammonia induces astrocytic swelling by a complex interplay of (i) impairment of in- and out-transport of different osmolytes leading to intracellular osmotic imbalance, (ii) mitochondrial dysfunction related to excessive accumulation of ammonia-derived glutamine and successive intra-mitochondrial release of toxic levels of ammonia, (iii) oxidative/nitrosative stress. Evidence presented below strongly suggests that glutamine is involved in a vicious cycle of (i), (ii), and (iii).

Glutaminosis: A Causative Factor In Cytotoxic Brain Edema And Its Mechanistic Basis

As mentioned in the section: “Glutaminosis: a consistent neuropathological component of hyperammonemic encephalopathies,” clinical studies revealed a good correlation between brain glutamine content and the severity of edema-related manifestations of ALF. While correlation strongly suggested a mechanistic link, it could not be interpreted as causal nexus. A proof of concept came from experimental ALF or acute-upon-chronic liver failure models, inhibition of GS activity by a GS inhibitor, methionine sulfoximine, alleviated astrocytic swelling, brain edema, and a set of other pathophysiological symptoms of acute HE (Takahashi et al., 1991; Willard-Mack et al., 1996; Master et al., 1999; Tanigami et al., 2005). Contrary to efficient ammonia-lowering treatments, which are effective in reducing brain edema in animal models of ALF, a decrease in high cerebral glutamine levels were not observed (Zwingmann et al., 2004; Ytrebø et al., 2009).

Slc38A3: The Transporter Involved in Glutamine Trapping Within Astrocytes

Studies in vitro on primary astrocyte cultures indicated that the contribution of system N in glutamine transport varies from 10 to 50% of the total glutamine transport capacity (Nagaraja and Brookes, 1996; Deitmer et al., 2003; Heckel et al., 2003; Dolińska et al., 2004; Sidoryk-Węgrzynowicz et al., 2009). System N silencing in neonatal astrocytes inhibited glutamine efflux out of the cells and documented its prevailing functioning in the direction of glutamine release (Zielińska et al., 2016). Glutamine efflux is preferably mediated by the Slc38a3 system N glutamine transporter, much more so than by one other system N transporter Slc38a2, as the latter shows relatively high affinity for serine, alanine, and glycine (Nakanishi et al., 2001a,b; Hamdani et al., 2012). Immunohistochemical data revealed localization of the system N transporters Slc38a3 (Boulland et al., 2002) and Slc38a5 (Cubelos et al., 2005) on astrocytic processes located adjacent to glutamatergic and GABAergic synapses, confirming the presence of the protein in native tissue. More recently, Slc38a5 was shown to be located intracellularly (Hamdani et al., 2012), and functional expression of Slcs8a3 was demonstrated in the astrocytic plasma membrane in situ (Todd et al., 2017). Hence, over thirty years after its initial discovery, it has become clear that Slc38a3 plays a critical role in regulating the astrocytic leg of GGC.

Evidence implicates Slc38a3 transporter to act as a hub for glutamine transport, recruiting a range of accessory complexes that enhance and regulate its function in response to different protein (Boulland et al., 2002; Rubio-Aliaga and Wagner, 2016). Interestingly enough, the physical coupling of Slc1a3-Slc38a3 proteins demonstrated in cultured Bergmann glia (Martínez-Lozada et al., 2013) and kinetics data of glutamine fluxes driven mainly by the increased astrocytic [Na⁺] (Todd et al., 2017) support Slc38a3-mediated glutamine transport in glutamate recycling. Since Slc38a3 preferentially controls the efflux of newly synthesized glutamine from astrocytes (Chaudhry et al., 1999), it prevents excessive accumulation in there and, subsequently, retention of osmotically obligated water. Accordingly, its decreased activity in ALF leads to enhanced intracellular glutamine trapping, in this way contributing to cytotoxic brain edema (Hamdani et al., 2021).

Kanamori and Ross (2005) were the first to hint, albeit indirectly, at the possibility that system N-mediated glutamine transport may be controlled by hyperammonemia. In their study, continuous infusion of [¹⁵N]ammonium acetate resulted increased glutamine accumulation in brain microdialysate. Since extracellular glutamine sufficiently saturated system A-mediated glutamine transport, the authors interpreted their finding as reflecting inhibition of glutamine efflux from astrocytes by reversal of system N transport. Our recent studies extended this original finding and directly implicated the involvement Slc38a3 in the sequence of events leading to astrocytic swelling and brain edema. Decreased Slc38a3 expression was recorded in the cerebral cortex of rats with thioacetamide-induced ALF, but not in those with ammonium-acetate-induced simple hyperammonemia (Zielińska et al., 2014). Most interestingly, thioacetamide-induced ALF, but not hyperammonemia was earlier found associated with increased cerebro-cortical volume (Hilgier et al., 1996). In azoxymethan-induced mice model of ALF, decreased expression of Slc38a3 in the brain coincided with (i) excessive brain glutamine (ii) increased astrocytic cell volume and (iii) decreased apparent diffusion coefficient marking cytotoxic brain edema (Hamdani et al., 2021). As a proof of concept, local Slc38a3 silencing using vivo morpholino technique resulted in astrocytic swelling and increased volume of the brain region subjected to silencing (Hamdani et al., 2021).

The mechanism underlying reduction of Slc38a3 expression in the ammonia- (or otherwise glutamine)- overexposed brain may be subject to regulation by a wide spectrum of transcriptional, translational, or epigenetic factor which remain to be analyzed in detail. Ammonia treatment in vitro strongly inhibited the release of newly loaded radiolabeled glutamine from cultured astrocytes (Dąbrowska et al., 2018) and the inhibition involved changes in protein kinase C signaling (Dąbrowska et al., 2018), Sp1-Nrf2 transcription factor complex formation (Dąbrowska and Zielińska, 2019), and activation of Nrf2 transcription factor per se (Dąbrowska et al., 2021). Of note in this context, the study by Lister et al. (2018) identified Nrf2 transcription factor control in the regulation of Slc38a3mRNA expression (Lister et al., 2018). In addition, in vitro experiments on Slc38a3 transfected oocytes revealed that depression Slc38a3-mediated glutamine transport engages direct interaction of ammonium ions with the Slc38a3 protein moiety (Hamdani et al., 2021). Clearly, the mechanisms underlying the responses of Slc38a3 to ammonia at the transcriptional/translational/posttranslational levels deserve further investigation.

Slc38a3 carrier is believed to bridge inactivation of glutamate in astrocytes to neurotransmitter glutamate synthesis in the nerve endings (Todd et al., 2017; Verkhratsky et al., 2021). Therefore, its excessive involvement in glutamine trapping may contribute to the imbalance between excitatory and inhibitory neurotransmission as well. However, proper glutamatergic transmission seems to be less dependent and may occur after inhibition or reduction of GS (Liang et al., 2006; Kam and Nicoll, 2007) or after local knock out-induced reduction of astrocytic Slc38a3 transporter, mediating glutamine efflux (Popek et al., 2020). It remains to be seen whether structural and electrophysiological impairment of glutamatergic synapse noted in ALF mice is in anyway related to Slc38a3 depletion in the same model (Popek et al., 2018).

Glutamine: An Osmotic Stress- Inducing Factor

Cerebral glutamine concentration above 2 mM saturates active glutamine transport out of the brain (O’Kane and Hawkins, 2003) and, thereby, favors its accumulation. Accumulation of synthesized in glial cells glutamine, might cause the osmotic pressure increase and generate glutamine concentration gradient leading to the development of intracranial pressure (ICP) (Master et al., 1999; Tofteng et al., 2002, 2006). In the brain, the difference between 1 mmol/L in blood and 4 mmol/L would cause a pressure gradient of 35 mmHg that is well above the critical level to cause brain edema. Thus, simultaneously triggered brain compensatory mechanisms are critical and encompass a removal from the brain other osmotically active compounds, e.g., myo-inositol, choline, or taurine, which at least partially reduce brain osmotic effects (Sterns and Silver, 2006; Heins and Zwingmann, 2010; Jiménez et al., 2017). Importantly, biochemical changes of different osmotically active substances in the brain are frequently observed even before the onset of clinical symptoms (Larsen, 2002). Studies performed by proton magnetic resonance spectroscopy (¹H MRS) in symptomatic patients with severe ornithine transcarbamylase deficiency showed that a significantly elevated level of glutamine was accompanied by a simultaneous decrease in myo-inositol and choline, which is considered compensatory in nature (Gropman et al., 2009; Sen et al., 2021). However, at a very high concentration of ammonia, osmoregulation may be insufficient to compensate for the rapid cerebral glutamine increase. The above is supported by the results delivered from animal models: as outlined in the previous section, brain edema caused by acute ammonia poisoning was prevented by the inhibition of glutamine synthesis. However, arguments may be raised against the contribution of excess glutamine to increased intracellular osmotic pressure. Mild hypothermia prevented brain edema development although, glutamine brain content remained relatively stable under these conditions (Vaquero and Butterworth, 2007; Stravitz and Larsen, 2009). Moreover, in the healthy brain glutamine accounts for less than 2% of the total pool of organic osmolytes and electrolytes (Pasantes-Morales et al., 2002). Therefore, the ∼3–4-fold increase of brain glutamine observed in ALF patients (Bjerring et al., 2010), and experimental animals (Takahashi et al., 1991; Master et al., 1999), is unlikely to be enough to significantly account for brain edema, even if not compensated by the efflux of other osmolytes. Of note, water flow through the cell membrane is at least in part regulated by the activity of aquaporin water channels which additionally may modify the cell’s osmotic status (Papadopoulos and Verkman, 2007; Thrane et al., 2011). All in all, although perhaps significant locally, on a global scale, the osmotic effect of excess glutamine alone is unlikely to be the predominating edema-eliciting factor.

Glutamine: Inducer of Mitochondrial Dysfunction and Swelling in the “Trojan Horse” Hypothesis

According to the “Trojan Horse” hypothesis (Albrecht and Norenberg, 2006), glutamine accumulating in excess in the cytoplasm enters mitochondria and opens the megachannel in the inner mitochondrial membrane, mitochondrial permeability transition pore (mPTP), which is sensitive to cyclosporine A (Ziemińska et al., 2000b). Available evidence suggests that glutamine enters mitochondria by active transport rather than by diffusion. It was shown that glutamine entry to astrocytic mitochondria is stimulated by pathopysiologically relevant concentrations of glutamine (Dolińska et al., 1996). Histidine, the strongest inhibitor of mitochondrial glutamine among all the amino acids (see section “Glutamine Transport in Astrocytic Mitochondria”), attenuated opening of mPTP and mitochondrial swelling in isolated astrocytic mitochondria (Ziemińska et al., 2000a), in cultured astrocytes (Pichili et al., 2007) and in the brain of ALF-affected rats (Rama Rao et al., 2010).

In mammalian cells, mPTP elicits a rapid increase in the permeability of e.g., protons, ions, and other molecules of MW < 1,500 Da through the inner mitochondrial membrane. The mega-channels opening leads to a collapse of the mitochondrial inner membrane potential, created by protons through the mitochondrial electron transport chains (Guo et al., 2018; Fernandez-Vizarra and Zeviani, 2021). This causes osmotic swelling of the mitochondrial matrix and movement of metabolites through the inner membrane that leads to defective oxidative phosphorylation decrease of ATP synthesis (Vercellino and Sazanov, 2022). Consequently, the mitochondrial membrane potential loss leads to reactive oxygen species production that further stimulates the mPTP process.

In astrocytes, mitochondrial dysfunction elicited by glutamine leads to the formation of reactive oxygen species and astrocytic cell swelling (Norenberg et al., 2004; Albrecht and Norenberg, 2006; Rama Rao and Norenberg, 2012). Upon entry to mitochondria, glutamine is metabolized by the mitochondrial enzyme PAG to ammonia and glutamate and, ammonia is the trigger of subsequent deleterious events. This sequence of events has been documented in cultured astrocytes, where the glutamine-induced intra-astrocytic accumulation of reactive oxygen species (Jayakumar et al., 2004) and astrocytic swelling (Jayakumar et al., 2006) were attenuated, by the PAG synthetic inhibitor, DON (Crosby, 2015).

Evidence that served to formulate the “Trojan Horse” hypothesis has been considered somewhat ambiguous. The criticism raised was that the hypothesis was overwhelmingly based on results of ex vivo experiments (isolated mitochondria), or in vitro (cultured astrocytes treated with 5 mM ammonia for 24 h) (see the above paras). As a step forward, in one in vivo the mPTP induction was detected in brain homogenates of rats with thioacetamide-induced ALF, and reduced after the administration of glutamine transport competitor, histidine. Histidine also attenuated oxidative stress, and brain edema (Rama Rao et al., 2010). Toward the same end, intracellular lactate accumulation in the brain and elevated ICP occurred notwithstanding unchanged mitochondrial function in hyperammonemia brain tissue (Witt et al., 2017). In support of the “Trojan Horse” glutamine mode of action, elevated concentrations of ATP degradation products hypoxanthine and inosine, markers of mitochondrial dysfunction, in brain dialysates from ALF patients, have been found to correlate with extracellular glutamine (Bjerring et al., 2010). Less directly supportive of, but consistent with the hypothesis, reduced metabolic rates of oxygen were very previously noted in the brain of rats with thioacetamide-induced ALF (Pluta and Albrecht, 1986), and more recently in the brain of patients with overt hepatic encephalopathy (Iversen et al., 2009).

One other criticism of the Trojan Horse hypothesis has been raised based on the purported absence of PAG in native astrocytes and its exclusive location in neurons (Laake et al., 1999). In line with the discussed view, ameliorating effects of astrocyte swelling in vitro, induced by the PAG inhibitor, were interpreted as solely reflecting phenotypic alteration of astrocytes upon culturing. However, the skepticism was balanced by solid evidence that both PAG isoforms abound in the rat and human brain (Cardona et al., 2015; Milewski et al., 2019).

Slc7A6: Contributor to Ammonia-Induced Oxidative/Nitrosative Stress in Astrocytic Swelling

Compelling evidence documents that ammonia generates free radicals (Murthy et al., 2001; Görg et al., 2008) and ammonia-induced astrocytic swelling that per se appears to be a trigger of oxidative/nitrosative stress and subsequent protein tyrosine nitration, is a critical event en route to astrocytic and neuronal dysfunction (Schliess et al., 2002; Kruczek et al., 2011). Induction of peroxynitrite activates volume-regulated anion channels in astrocytes and induces astrocytic swelling which was coupled to enhanced release of the glutamate surrogate [³H]D-aspartate (Haskew et al., 2002). Free radicals formation was observed in a rat model of hyperammonemia (Kosenko et al., 1997, 1998), and was associated with decreased activity of antioxidant enzymes (glutathione peroxidase, superoxide dismutase and catalase) (Kosenko et al., 1997). Ammonia-induced cerebrocortical tissue swelling was ameliorated by the NMDA/nitric oxide (NO) pathway inhibitors, indicating involvement of oxidative-nitrosative stress (Zielińska et al., 2003).

The system y + L member, Slc7a6 (4F2hc/y + LAT2) carrier is a heterodimer, composed of a glycosylated heavy chain (SLC3a2/4F2hc/CD98 and a catalytic light chain subunit (SLC7) (Torrents et al., 1998). The heavy chain is necessary for trafficking of the light chain to the plasma membrane, whereas the light chain determines the transport characteristics of the respective heterodimer. Slc7a6 has a wide tissue distribution including brain, heart, kidney, and promotes glutamine exchange for essential cationic amino acids including arginine (Pfeiffer et al., 1998; Torrents et al., 1998; Bröer et al., 2000).

The role of Slc7a6-mediated glutamine-arginine exchange in the modulation of NO synthesis under hyperammonemic conditions in vivo has been demonstrated in this laboratory (Hilgier et al., 2008, 2009). Specifically, in ammonia perfused rat brain, pharmacological inhibition of extracellular glutamine degradation or glutamine transport to neurons reduced NO synthesis and its accumulation in the extracellular space (Hilgier et al., 2009). Attenuation of NO synthesis was reproduced by intracerebral administration of glutamine, or two other y + LAT2 substrates, leucine and cyclo-leucine (Hilgier et al., 2009), while inhibition of glutamine synthesis reversed this attenuating effect (Hilgier et al., 2009). Collectively the results underscored the contribution of y + LAT2 transporter to glutamine/arginine imbalance associated with hyperammonemia. The link of y + LAT2 activity to ammonia-induced oxidative-nitrosative stress came to light in studies on cultured astrocytes and animal models (Zielińska et al., 2011, 2012, 2014). Those studies documented reduced arginine delivery due to enhanced y + LAT2-mediated exchange of extracellular glutamine for intracellular arginine, contributing to decreased NO and cGMP formation in the rat brain by hyperammonemia.

More recent studies revealed that induction of iNOS in astrocytes and stimulation of NO synthesis by ammonia is coupled to increased arginine uptake, a process promoted by a selective increase of the expression and activity of y + LAT2, whereas the unidirectional basic amino acid carrier y + was not affected by ammonia (Zielińska et al., 2012, 2015). In cultured astrocytes, ammonia-evoked oxidative-nitrosative stress also involves induction of iNOS (Schliess et al., 2002), mediated by activation of the nuclear factor κB (Sinke et al., 2008). Of note, cytotoxic brain edema in ALF is also related to the central or peripheral inflammation (Wilkinson et al., 1974; Wyke et al., 1982; Odeh et al., 2004; Shawcross et al., 2007; Butterworth, 2011; Scott, 2013; Jayakumar et al., 2015), whose deleterious effects are mediated by oxidative-nitrosative stress. However, specific contribution of glutamine transport to this phenomenon has to our knowledge not been investigated as yet.

Concluding Remarks

In conclusion, data presented in this review support the view that altered functioning of glutamine transporting moieties residing in astrocytes, contribute in a vicious circle mode, to the glutamine-driven aspect of astrocytic swelling and cytotoxic brain edema associated with ALF (Figure 1). Decreased Slc38a3 activity reduces efflux of newly synthesized glutamine, augmenting its intra-astrocytic residence. The resulting glutamine surplus aggravates glutamine-induced osmotic stress in the cytoplasm, at the same time rendering more glutamine available for (i) its Slc7a6-mediated exchange for extracellular arginine, which increases intra-astrocytic accumulation of reactive nitrogen species (ii) glutamine transport to astrocytic mitochondria, which leads to mitochondrial dysfunction (the “Trojan Horse” mode of action). The effects of (i) and (ii) converge at the level of oxidative/nitrosative stress, a critical driver of astrocytic swelling. Clearly, evidence for the above reasoning, especially regarding glutamine transport to mitochondria needs to be fine-tuned to achieve full symmetry between the documentation in vivo and in vitro.

FIGURE 1

In astrocytes, hyperammonemia (ammonium ions, NH₄⁺) alters the functioning of glutamine transporters that contribute in a vicious circle mode to the glutamine-driven aspect of astrocytic swelling and cytotoxic brain edema. Decreased system N (Slc38a3) activity reduces efflux of synthesized by glutamine synthetase (GS) glutamine, augmenting its intra-astrocytic residence. The resulting glutamine surplus aggravates glutamine-induced osmotic stress in the cytoplasm, rendering more glutamine available for: (i) its system y + L (Slc7a6)-mediated exchange for extracellular arginine (Arg), which increases the intra-astrocytic accumulation of reactive oxygen-nitrogen species (ROS), (ii) glutamine enter to astrocytic mitochondria, where, hydrolyzed to glutamate and NH₄⁺ by PAG leads to open mitochondrial permeability transition pore (mPTP), and mitochondrial dysfunction (the “Trojan Horse” mode of action).

Publisher’s Note

All claims expressed in this article are solely those of the authors and do not necessarily represent those of their affiliated organizations, or those of the publisher, the editors and the reviewers. Any product that may be evaluated in this article, or claim that may be made by its manufacturer, is not guaranteed or endorsed by the publisher.

References

• 1

  Albrecht J. Norenberg M. D. (2006). Glutamine: a Trojan horse in ammonia neurotoxicity.Hepatology44788–794. 10.1002/hep.21357

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 2

  Albrecht J. Zielińska M. (2019). Exchange-mode glutamine transport across CNS cell membranes.Neuropharmacology161:107560. 10.1016/j.neuropharm.2019.03.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 3

  Albrecht J. Dolińska M. Hilgier W. Lipkowski A. W. Nowacki J. (2000). Modulation of glutamine uptake and phosphate-activated glutaminase activity in rat brain mitochondria by amino acids and their synthetic analogues.Neurochem. Int.36341–347. 10.1016/S0197-0186(99)00142-4

  • CrossRef
  • Google Scholar

• 4

  Albrecht J. Sidoryk-Węgrzynowicz M. Zielińska M. Aschner M. (2010). Roles of glutamine in neurotransmission.Neuron Glia Biol.6263–276. 10.1017/S1740925X11000093

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 5

  Amaral A. I. Meisingset T. W. Kotter M. R. Sonnewald U. (2013). Metabolic aspects of neuron-oligodendrocyte-astrocyte interactions.Front. Endocrinol.4:54. 10.3389/fendo.2013.00054

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 6

  Bak L. K. Schousboe A. Waagepetersen H. S. (2006). The glutamate/GABA-glutamine cycle: aspects of transport, neurotransmitter homeostasis and ammonia transfer.J. Neurochem.98641–653. 10.1111/j.1471-4159.2006.03913.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 7

  Balzano T. Dadsetan S. Forteza J. Cabrera-Pastor A. Taoro-Gonzalez L. Malaguarnera M. et al (2020). Chronic hyperammonemia induces peripheral inflammation that leads to cognitive impairment in rats: reversed by anti-TNF-α treatment.J. Hepatol.73582–592. 10.1016/j.jhep.2019.01.008

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 8

  Barollo S. Bertazza L. Watutantrige-Fernando S. Censi S. Cavedon E. Galuppini F. et al (2016). Overexpression of L-Type Amino acid transporter 1 (LAT1) and 2 (LAT2): novel markers of neuroendocrine tumors.PLoS One11:e0156044. 10.1371/journal.pone.0156044

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 9

  Bémeur C. Cudalbu C. Dam G. Thrane A. S. Cooper A. J. L. Rose C. F. (2016). Brain edema: a valid endpoint for measuring hepatic encephalopathy?Metab. Brain Dis.311249–1258. 10.1007/s11011-016-9843-9

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 10

  Bergström J. Fürst P. Norée L. O. Vinnars E. (1974). Intracellular free amino acid concentration in human muscle tissue.J. Appl. Physiol.36693–697. 10.1152/jappl.1974.36.6.693

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 11

  Bernal W. Hall C. Karvellas C. J. Auzinger G. Sizer E. Wendon J. (2007). Arterial ammonia and clinical risk factors for encephalopathy and intracranial hypertension in acute liver failure.Hepatology461844–1852. 10.1002/hep.21838

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 12

  Bhutia Y. D. Babu E. Ramachandran S. Ganapathy V. (2015). Amino acid transporters in cancer and their relevance to “glutamine addiction”: novel targets for the design of a new class of anticancer drugs.Cancer Res.751782–1788. 10.1158/0008-5472.CAN-14-3745

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 13

  Binesh N. Huda A. Bugbee M. Gupta R. Rasgon N. Kumar A. et al (2005). Adding another spectral dimension to1H magnetic resonance spectroscopy of hepatic encephalopathy.J. Magn. Reson. Imaging21398–405. 10.1002/jmri.20291

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 14

  Bjerring P. N. Hauerberg J. Frederiksen H.-J. Jorgensen L. Hansen B. A. Tofteng F. et al (2008). Cerebral glutamine concentration and lactate–pyruvate ratio in patients with acute liver failure.Neurocrit. Care93–7. 10.1007/s12028-008-9060-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 15

  Bjerring P. N. Hauerberg J. Jørgensen L. Frederiksen H.-J. Tofteng F. Hansen B. A. et al (2010). Brain hypoxanthine concentration correlates to lactate/pyruvate ratio but not intracranial pressure in patients with acute liver failure.J. Hepatol.531054–1058. 10.1016/j.jhep.2010.05.032

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 16

  Blei A. T. (2007). Brain edema in acute liver failure: can it be prevented? Can it be treated?J. Hepatol.46564–569. 10.1016/j.jhep.2007.01.011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 17

  Bosman D. K. Deutz N. E. P. Maas M. A. W. Eijk H. M. H. Smit J. J. H. Haan J. G. et al (1992). Amino acid release from cerebral cortex in experimental acute liver failure. studied by in vivo cerebral cortex microdialysis.J. Neurochem.59591–599. 10.1111/j.1471-4159.1992.tb09410.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 18

  Bosoi C. R. Rose C. F. (2013). Brain edema in acute liver failure and chronic liver disease: similarities and differences.Neurochem. Int.62446–457. 10.1016/j.neuint.2013.01.015

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 19

  Boulland J.-L. Osen K. K. Levy L. M. Danbolt N. C. Edwards R. H. Storm-Mathisen J. et al (2002). Cell-specific expression of the glutamine transporter SN1 suggests differences in dependence on the glutamine cycle: glutamine transporter SN1 and transmitter recycling.Eur. J. Neurosci.151615–1631. 10.1046/j.1460-9568.2002.01995.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 20

  Braun D. Kinne A. Bräuer A. U. Sapin R. Klein M. O. Köhrle J. et al (2011). Developmental and cell type-specific expression of thyroid hormone transporters in the mouse brain and in primary brain cells.Glia59463–471. 10.1002/glia.21116

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 21

  Bröer A. Brookes N. Ganapathy V. Dimmer K. S. Wagner C. A. Lang F. et al (1999). The astroglial ASCT2 amino acid transporter as a mediator of glutamine efflux.J. Neurochem.732184–2194.

  • Pubmed Abstract
  • Google Scholar

• 22

  Bröer A. Rahimi F. Bröer S. (2016). Deletion of amino acid transporter ASCT2 (SLC1A5) reveals an essential role for transporters SNAT1 (SLC38A1) and SNAT2 (SLC38A2) to sustain glutaminolysis in cancer cells.J. Biol. Chem.29113194–13205. 10.1074/jbc.M115.700534

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 23

  Bröer A. Wagner C. A. Lang F. Bröer S. (2000). The heterodimeric amino acid transporter 4F2hc/y+LAT2 mediates arginine efflux in exchange with glutamine.Biochem. J.349(Pt 3)787–795. 10.1042/bj3490787

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 24

  Bröer S. (2007). “SLC38 family of transporters for neutral amino acids,”,” in Handbook of Neurochemistry and Molecular Neurobiology, edsLajthaA.ReithM. E. A. (Boston, MA: Springer US), 327–338. 10.1007/978-0-387-30380-2_16

  • CrossRef
  • Google Scholar

• 25

  Butterworth R. F. (2011). Hepatic encephalopathy: a central neuroinflammatory disorder?Hepatology531372–1376. 10.1002/hep.24228

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 26

  Cabrera-Pastor A. Arenas Y. M. Taoro-Gonzalez L. Montoliu C. Felipo V. (2019). Chronic hyperammonemia alters extracellular glutamate, glutamine and GABA and membrane expression of their transporters in rat cerebellum. Modulation by extracellular cGMP.Neuropharmacology161:107496. 10.1016/j.neuropharm.2019.01.011

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 27

  Cardona C. Sánchez-Mejías E. Dávila J. C. Martín-Rufián M. Campos-Sandoval J. A. Vitorica J. et al (2015). Expression of Gls and Gls2 glutaminase isoforms in astrocytes: functional glutaminase expression in astroglia.Glia63365–382. 10.1002/glia.22758

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 28

  Castell L. Vance C. Abbott R. Marquez J. Eggleton P. (2004). Granule localization of glutaminase in human neutrophils and the consequence of glutamine utilization for neutrophil activity.J. Biol. Chem.27913305–13310. 10.1074/jbc.M309520200

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 29

  Chadipiralla K. Reddanna P. Chinta R. M. Reddy P. V. B. (2012). Thioacetamide-Induced fulminant hepatic failure induces cerebral mitochondrial dysfunction by altering the electron transport chain complexes.Neurochem. Res.3759–68. 10.1007/s11064-011-0583-2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 30

  Chaudhry F. A. (2001). Coupled and uncoupled proton movement by amino acid transport system N.EMBO J.207041–7051. 10.1093/emboj/20.24.7041

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 31

  Chaudhry F. A. Reimer R. J. Krizaj D. Barber D. Storm-Mathisen J. Copenhagen D. R. et al (1999). Molecular analysis of system N suggests novel physiological roles in nitrogen metabolism and synaptic transmission.Cell99769–780. 10.1016/s0092-8674(00)81674-8

  • CrossRef
  • Google Scholar

• 32

  Chavarria L. Oria M. Romero-Gimenez J. Alonso J. Lope-Piedrafita S. Cordoba J. (2010). Diffusion tensor imaging supports the cytotoxic origin of brain edema in a rat model of acute liver failure.Gastroenterology1381566–1573. 10.1053/j.gastro.2009.10.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 33

  Clemmesen J. O. Larsen F. S. Kondrup J. Hansen B. A. Ott P. (1999). Cerebral herniation in patients with acute E liver failure is correlated with arterial ammonia concentration.Hepatology29648–653. 10.1002/hep.510290309

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 34

  Coltart I. Tranah T. H. Shawcross D. L. (2013). Inflammation and hepatic encephalopathy.Arch. Biochem. Biophys.536189–196. 10.1016/j.abb.2013.03.016

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 35

  Cooper A. Jeitner T. (2016). Central role of glutamate metabolism in the maintenance of nitrogen homeostasis in normal and hyperammonemic brain.Biomolecules6:16. 10.3390/biom6020016

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 36

  Coothankandaswamy V. Cao S. Xu Y. Prasad P. D. Singh P. K. Reynolds C. P. et al (2016). Amino acid transporter SLC6A14 is a novel and effective drug target for pancreatic cancer: SLC6A14 is a drug target for pancreatic cancer.Br. J. Pharmacol.1733292–3306. 10.1111/bph.13616

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 37

  Cory J. G. Cory A. H. (2006). Critical roles of glutamine as nitrogen donors in purine and pyrimidine nucleotide synthesis: asparaginase treatment in childhood acute lymphoblastic leukemia.Vivo20587–589.

  • Pubmed Abstract
  • Google Scholar

• 38

  Crosby H. (2015). Evaluating the toxicity of the analgesic glutaminase inhibitor 6-Diazo-5-Oxo-L-norleucine in vitro and on rat dermal skin fibroblasts.MOJT1:5. 10.15406/mojt.2015.01.00005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 39

  Cubelos B. González-González I. M. Giménez C. Zafra F. (2005). Amino acid transporter SNAT5 localizes to glial cells in the rat brain.Glia49230–244. 10.1002/glia.20106

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 40

  Czeredys M. Mysiorek C. Kulikova N. Samluk L. Berezowski V. Cecchelli R. et al (2008). A polarized localization of amino acid/carnitine transporter B0,+ (ATB0,+) in the blood–brain barrier.Biochem. Biophys. Res. Commun.376267–270. 10.1016/j.bbrc.2008.08.122

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 41

  Dąbrowska K. Albrecht J. Zielińska M. (2018). Protein kinase C-mediated impairment of glutamine outward transport and SN1 transporter distribution by ammonia in mouse cortical astrocytes.Neurochem. Int.118225–232. 10.1016/j.neuint.2018.07.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 42

  Dąbrowska K. Zielińska M. (2019). Silencing of transcription factor Sp1 promotes SN1 transporter regulation by ammonia in mouse cortical astrocytes.IJMS20:234. 10.3390/ijms20020234

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 43

  Dąbrowska K. Skowrońska K. Popek M. Albrecht J. Zielińska M. (2021). The role of Nrf2 transcription factor and Sp1-Nrf2 protein complex in glutamine transporter sn1 regulation in mouse cortical astrocytes exposed to ammonia.IJMS22:11233. 10.3390/ijms222011233

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 44

  Daikhin Y. Yudkoff M. (2000). Compartmentation of brain glutamate metabolism in neurons and glia.J. Nutr.1301026S–1031S. 10.1093/jn/130.4.1026S

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 45

  Deitmer J. W. Bröer A. Bröer S. (2003). Glutamine efflux from astrocytes is mediated by multiple pathways.J. Neurochem.87127–135. 10.1046/j.1471-4159.2003.01981.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 46

  del Pino M. M. S. Peterson D. R. Hawkins R. A. (1995). Neutral amino acid transport characterization of isolated luminal and abluminal membranes of the blood-brain barrier.J. Biol. Chem.27014913–14918. 10.1074/jbc.270.25.14913

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 47

  Desjardins P. Du T. Jiang W. Peng L. Butterworth R. F. (2012). Pathogenesis of hepatic encephalopathy and brain edema in acute liver failure: role of glutamine redefined.Neurochem. Int.60690–696. 10.1016/j.neuint.2012.02.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 48

  Dolgodilina E. Camargo S. M. Roth E. Herzog B. Nunes V. Palacín M. et al (2020). Choroid plexus LAT2 and SNAT3 as partners in CSF amino acid homeostasis maintenance.Fluids Barriers CNS17:17. 10.1186/s12987-020-0178-x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 49

  Dolińska M. Hilgier W. Albrecht J. (1996). Ammonia stimulates glutamine uptake to the cerebral non-synaptic mitochondria of the rat.Neurosci. Lett.21345–48. 10.1016/0304-3940(96)12827-5

  • CrossRef
  • Google Scholar

• 50

  Dolińska M. Zabłocka B. Sonnewald U. Albrecht J. (2004). Glutamine uptake and expression of mRNA’s of glutamine transporting proteins in mouse cerebellar and cerebral cortical astrocytes and neurons.Neurochem. Int.4475–81. 10.1016/s0197-0186(03)00123-2

  • CrossRef
  • Google Scholar

• 51

  Feng M. Xiong G. Cao Z. Yang G. Zheng S. Qiu J. et al (2018). LAT2 regulates glutamine-dependent mTOR activation to promote glycolysis and chemoresistance in pancreatic cancer.J. Exp. Clin. Cancer Res.37:274. 10.1186/s13046-018-0947-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 52

  Fernandez-Vizarra E. Zeviani M. (2021). Mitochondrial disorders of the OXPHOS system.FEBS Lett.5951062–1106. 10.1002/1873-3468.13995

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 53

  Fotiadis D. Kanai Y. Palacín M. (2013). The SLC3 and SLC7 families of amino acid transporters.Mol. Aspects Med.34139–158. 10.1016/j.mam.2012.10.007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 54

  Gliddon C. M. Shao Z. LeMaistre J. L. Anderson C. M. (2009). Cellular distribution of the neutral amino acid transporter subtype ASCT2 in mouse brain.J. Neurochem.108372–383. 10.1111/j.1471-4159.2008.05767.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 55

  Görg B. Qvartskhava N. Keitel V. Bidmon H. J. Selbach O. Schliess F. et al (2008). Ammonia induces RNA oxidation in cultured astrocytes and brain in vivo.Hepatology48567–579. 10.1002/hep.22345

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 56

  Gropman A. L. Sailasuta N. Harris K. C. Abulseoud O. Ross B. D. (2009). Ornithine transcarbamylase deficiency with persistent abnormality in cerebral glutamate metabolism in adults.Radiology252833–841. 10.1148/radiol.2523081878

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 57

  Guo R. Gu J. Zong S. Wu M. Yang M. (2018). Structure and mechanism of mitochondrial electron transport chain.Biomed. J.419–20. 10.1016/j.bj.2017.12.001

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 58

  Hakvoort T. B. M. He Y. Kulik W. Vermeulen J. L. M. Duijst S. Ruijter J. M. et al (2017). Pivotal role of glutamine synthetase in ammonia detoxification.Hepatology65281–293. 10.1002/hep.28852

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 59

  Hamdani E. H. Gudbrandsen M. Bjørkmo M. Chaudhry F. A. (2012). The system N transporter SN2 doubles as a transmitter precursor furnisher and a potential regulator of NMDA receptors.Glia601671–1683. 10.1002/glia.22386

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 60

  Hamdani E. H. Popek M. Frontczak-Baniewicz M. Utheim T. P. Albrecht J. Zielińska M. et al (2021). Perturbation of astroglial Slc38 glutamine transporters by NH₄⁺ contributes to neurophysiologic manifestations in acute liver failure.FASEB J.35:e21588. 10.1096/fj.202001712RR

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 61

  Haskew R. E. Mongin A. A. Kimelberg H. K. (2002). Peroxynitrite enhances astrocytic volume-sensitive excitatory amino acid release via a src tyrosine kinase-dependent mechanism: peroxynitrite enhances EAA release.J. Neurochem.82903–912. 10.1046/j.1471-4159.2002.01037.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 62

  Häussinger D. (1990). Liver glutamine metabolism.J. Parenter. Enteral Nutr.1456S–62S. 10.1177/014860719001400405

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 63

  Haussinger D. Schliess F. (2008). Pathogenetic mechanisms of hepatic encephalopathy.Gut571156–1165. 10.1136/gut.2007.122176

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 64

  Haussinger D. Soboll S. Meijer A. J. Gerok W. Tager J. M. Sies H. (1985). Role of plasma membrane transport in hepatic glutamine metabolism.Eur. J. Biochem.152597–603. 10.1111/j.1432-1033.1985.tb09237.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 65

  Hawkins R. Viña J. (2016). How glutamate is managed by the blood–brain barrier.Biology5:37. 10.3390/biology5040037

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 66

  Heckel T. Bröer A. Wiesinger H. Lang F. Bröer S. (2003). Asymmetry of glutamine transporters in cultured neural cells.Neurochem. Int.43289–298. 10.1016/s0197-0186(03)00014-7

  • CrossRef
  • Google Scholar

• 67

  Heins J. Zwingmann C. (2010). Organic osmolytes in hyponatremia and ammonia toxicity.Metab. Brain Dis.2581–89. 10.1007/s11011-010-9170-5

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 68

  Hilgier W. Fręśko I. Klemenska E. Beręsewicz A. Oja S. S. Saransaari P. et al (2009). Glutamine inhibits ammonia-induced accumulation of cGMP in rat striatum limiting arginine supply for NO synthesis.Neurobiol. Dis.3575–81. 10.1016/j.nbd.2009.04.004

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 69

  Hilgier W. Olson J. E. Albrecht J. (1996). Relation of taurine transport and brain edema in rats with simple hyperammonemia or liver failure.J. Neurosci. Res.4569–74. 10.1002/(SICI)1097-4547(19960701)45:1<69::AID-JNR6<3.0.CO;2-F

  • CrossRef
  • Google Scholar

• 70

  Hilgier W. Wegrzynowicz M. Maczewski M. Beresewicz A. Oja S. S. Saransaari P. et al (2008). Effect of glutamine synthesis inhibition with methionine sulfoximine on the nitric oxide-cyclic GMP pathway in the rat striatum treated acutely with ammonia: a microdialysis study.Neurochem. Res.33267–272. 10.1007/s11064-007-9455-1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 71

  Hilgier W. Zielińska M. Borkowska H. D. Gadamski R. Walski M. Oja S. S. et al (1999). Changes in the extracellular profiles of neuroactive amino acids in the rat striatum at the asymptomatic stage of hepatic failure.J. Neurosci. Res.5676–84. 10.1002/(SICI)1097-4547(19990401)56:1<76::AID-JNR10<3.0.CO;2-Y

  • CrossRef
  • Google Scholar

• 72

  Huttunen J. Peltokangas S. Gynther M. Natunen T. Hiltunen M. Auriola S. et al (2019). l-Type amino acid transporter 1 (LAT1/Lat1)-utilizing prodrugs can improve the delivery of drugs into neurons, astrocytes and microglia.Sci. Rep.9:12860. 10.1038/s41598-019-49009-z

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 73

  Indiveri C. Abruzzo G. Stipani I. Palmieri F. (1998). Identification and purification of the reconstitutively active glutamine carrier from rat kidney mitochondria.Biochem. J.333285–290. 10.1042/bj3330285

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 74

  Iversen P. Sørensen M. Bak L. K. Waagepetersen H. S. Vafaee M. S. Borghammer P. et al (2009). Low cerebral oxygen consumption and blood flow in patients with cirrhosis and an acute episode of hepatic encephalopathy.Gastroenterology136863–871. 10.1053/j.gastro.2008.10.057

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 75

  Jacobson I. Sandberg M. Hamberger A. (1985). Mass transfer in brain dialysis devices—a new method for the estimation of extracellular amino acids concentration.J. Neurosci. Methods15263–268. 10.1016/0165-0270(85)90107-4

  • CrossRef
  • Google Scholar

• 76

  Jayakumar A. R. Norenberg M. D. (2018). Hyperammonemia in hepatic encephalopathy.J. Clin. Exp. Hepatol.8272–280. 10.1016/j.jceh.2018.06.007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 77

  Jayakumar A. R. Rama Rao K. V. Norenberg M. D. (2015). Neuroinflammation in hepatic encephalopathy: mechanistic aspects.J. Clin. Exp. Hepatol.5S21–S28. 10.1016/j.jceh.2014.07.006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 78

  Jayakumar A. R. Rama Rao K. V. Schousboe A. Norenberg M. D. (2004). Glutamine-induced free radical production in cultured astrocytes.Glia46296–301. 10.1002/glia.20003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 79

  Jayakumar A. R. Rao K. V. R. Murthy C. R. K. Norenberg M. D. (2006). Glutamine in the mechanism of ammonia-induced astrocyte swelling.Neurochem. Int.48623–628. 10.1016/j.neuint.2005.11.017

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 80

  Jiménez J. V. Carrillo-Pérez D. L. Rosado-Canto R. García-Juárez I. Torre A. Kershenobich D. et al (2017). Electrolyte and acid–base disturbances in end-stage liver disease: a physiopathological approach.Dig. Dis. Sci.621855–1871. 10.1007/s10620-017-4597-8

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 81

  Kageyama T. Nakamura M. Matsuo A. Yamasaki Y. Takakura Y. Hashida M. et al (2000). The 4F2hc/LAT1 complex transports l-DOPA across the blood–brain barrier.Brain Res.879115–121. 10.1016/S0006-8993(00)02758-X

  • CrossRef
  • Google Scholar

• 82

  Kam K. Nicoll R. (2007). Excitatory synaptic transmission persists independently of the glutamate-glutamine cycle.J. Neurosci.279192–9200. 10.1523/JNEUROSCI.1198-07.2007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 83

  Kanai Y. Endou H. (2001). Heterodimeric amino acid transporters: molecular biology and pathological and pharmacological relevance.CDM2339–354. 10.2174/1389200013338324

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 84

  Kanamori K. Ross B. D. (2005). Suppression of glial glutamine release to the extracellular fluid studied in vivo by NMR and microdialysis in hyperammonemic rat brain. J. Neurochem.94, 74–85. 10.1111/j.1471-4159.2005.03170.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 85

  Kato M. Hughes R. D. Keays R. T. Williams R. (1992). Electron microscopic study of brain capillaries in cerebral edema from fulminant hepatic failure.Hepatology151060–1066. 10.1002/hep.1840150615

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 86

  Kato M. Sugihara J. Nakamura T. Muto Y. (1989). Electron microscopic study of the blood-brain barrier in rats with brain edema and encephalopathy due to acute hepatic failure.Gastroenterol. Jpn.24135–142. 10.1007/BF02774187

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 87

  Kosenko E. Felipo V. Montoliu C. Grisolía S. Kaminsky Y. (1997). Effects of acute hyperammonemia in vivo on oxidative metabolism in nonsynaptic rat brain mitochondria.Metab. Brain Dis.1269–82. 10.1007/BF02676355

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 88

  Kosenko E. Kaminsky Y. Lopata O. Muravyov N. Kaminsky A. Hermenegildo C. et al (1998). Nitroarginine, an inhibitor of nitric oxide synthase, prevents changes in superoxide radical and antioxidant enzymes induced by ammonia intoxication.Metab. Brain Dis.1329–41. 10.1023/a:1020626928259

  • CrossRef
  • Google Scholar

• 89

  Kovacević Z. Bajin K. (1982). Kinetics of glutamine efflux from liver mitochondria loaded with the 14C-labeled substrate.Biochim. Biophys. Acta687291–295. 10.1016/0005-2736(82)90557-0

  • CrossRef
  • Google Scholar

• 90

  Kovacević Z. McGivan J. D. Chappell J. B. (1970). Conditions for activity of glutaminase in kidney mitochondria.Biochem. J.118265–274. 10.1042/bj1180265

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 91

  Kreis R. Farrow N. Ross Brian D. (1990). Diagnosis of hepatic encephalopathy by proton magnetic resonance spectroscopy.Lancet336635–636. 10.1016/0140-6736(90)93439-V

  • CrossRef
  • Google Scholar

• 92

  Krishna Rao R. (2012). Role of glutamine in protection of intestinal epithelial tight junctions.JEBP547–54. 10.2174/1875044301205010047

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 93

  Kruczek C. Görg B. Keitel V. Bidmon H. J. Schliess F. Häussinger D. (2011). Ammonia increases nitric oxide, free Zn(2+), and metallothionein mRNA expression in cultured rat astrocytes.Biol. Chem.3921155–1165. 10.1515/BC.2011.199

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 94

  Kuhn K. S. Schuhmann K. Stehle P. Darmaun D. Fürst P. (1999). Determination of glutamine in muscle protein facilitates accurate assessment of proteolysis and de novo synthesis–derived endogenous glutamine production.Am. J. Clin. Nutr.70484–489. 10.1093/ajcn/70.4.484

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 95

  Laake J. H. Takumi Y. Eidet J. Torgner I. A. Roberg B. Kvamme E. et al (1999). Postembedding immunogold labelling reveals subcellular localization and pathway-specific enrichment of phosphate activated glutaminase in rat cerebellum.Neuroscience881137–1151. 10.1016/S0306-4522(98)00298-X

  • CrossRef
  • Google Scholar

• 96

  Labow B. I. Souba W. W. (2000). Glutamine.World J. Surg.241503–1513. 10.1007/s002680010269

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 97

  Larsen F. S. (2002). Cerebral blood flow in hyperammonemia: heterogeneity and starling forces in capillaries.Metab. Brain Dis.17229–235. 10.1023/a:1021941414605

  • CrossRef
  • Google Scholar

• 98

  Laubenberger J. Haussinger D. Bayer S. Gufler H. Hennig J. Langer M. (1997). Proton magnetic resonance spectroscopy of the brain in symptomatic and asymptomatic patients with liver cirrhosis.Gastroenterology1121610–1616. 10.1016/S0016-5085(97)70043-X

  • CrossRef
  • Google Scholar

• 99

  Leke R. Schousboe A. (2016). The glutamine transporters and their role in the glutamate/GABA-glutamine cycle.Adv. Neurobiol.13223–257. 10.1007/978-3-319-45096-4_8

  • CrossRef
  • Google Scholar

• 100

  Leke R. Escobar T. D. C. Rama Rao K. V. Silveira T. R. Norenberg M. D. Schousboe A. (2015). Expression of glutamine transporter isoforms in cerebral cortex of rats with chronic hepatic encephalopathy.Neurochem. Int.8832–37. 10.1016/j.neuint.2015.03.005

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 101

  Liang S.-L. Carlson G. C. Coulter D. A. (2006). Dynamic regulation of synaptic GABA release by the glutamate-glutamine cycle in hippocampal area CA1.J. Neurosci.268537–8548. 10.1523/JNEUROSCI.0329-06.2006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 102

  Lister A. Bourgeois S. Imenez Silva P. H. Rubio-Aliaga I. Marbet P. Walsh J. et al (2018). NRF2 regulates the glutamine transporter Slc38a3 (SNAT3) in kidney in response to metabolic acidosis.Sci. Rep.8:5629. 10.1038/s41598-018-24000-2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 103

  Liu R. Hong R. Wang Y. Gong Y. Yeerken D. Yang D. et al (2020). Defect of SLC38A3 promotes epithelial mesenchymal transition and predicts poor prognosis in esophageal squamous cell carcinoma.Chin. J. Cancer Res.32547–563. 10.21147/j.issn.1000-9604.2020.05.01

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 104

  Lyck R. Ruderisch N. Moll A. G. Steiner O. Cohen C. D. Engelhardt B. et al (2009). Culture-induced changes in blood—brain barrier transcriptome: implications for amino-acid transporters in vivo.J. Cereb. Blood Flow Metab.291491–1502. 10.1038/jcbfm.2009.72

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 105

  Mann G. Mora S. Madu G. Adegoke O. A. J. (2021). Branched-chain amino acids: catabolism in skeletal muscle and implications for muscle and whole-body metabolism.Front. Physiol.12:702826. 10.3389/fphys.2021.702826

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 106

  Mans A. M. Biebuyck J. F. Shelly K. Hawkins R. A. (1982). Regional blood-brain barrier permeability to amino acids after portacaval anastomosis.J. Neurochem.38705–717. 10.1111/j.1471-4159.1982.tb08689.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 107

  Martinez A. (1968). Electron microscopy in human hepatic encephalopathy.Acta Neuropathol.1182–86. 10.1007/BF00692797

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 108

  Martinez-Hernandez A. Bell K. P. Norenberg M. D. (1977). Glutamine synthetase: glial localization in brain.Science1951356–1358. 10.1126/science.14400

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 109

  Martínez-Lozada Z. Guillem A. M. Flores-Méndez M. Hernández-Kelly L. C. Vela C. Meza E. et al (2013). GLAST/EAAT1-induced glutamine release via SNAT3 in Bergmann glial cells: evidence of a functional and physical coupling.J. Neurochem.125545–554. 10.1111/jnc.12211

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 110

  Master S. Gottstein J. Blei A. T. (1999). Cerebral blood flow and the development of ammonia-induced brain edema in rats after portacaval anastomosis.Hepatology30876–880. 10.1002/hep.510300428

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 111

  Matés J. M. Segura J. A. Campos-Sandoval J. A. Lobo C. Alonso L. Alonso F. J. et al (2009). Glutamine homeostasis and mitochondrial dynamics.Int. J. Biochem. Cell Biol.412051–2061. 10.1016/j.biocel.2009.03.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 112

  McKenna M. C. Sonnewald U. Huang X. Stevenson J. Zielke H. R. (1996). Exogenous glutamate concentration regulates the metabolic fate of glutamate in astrocytes.J. Neurochem.66386–393. 10.1046/j.1471-4159.1996.66010386.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 113

  McKenna M. C. Stridh M. H. McNair L. F. Sonnewald U. Waagepetersen H. S. Schousboe A. (2016). Glutamate oxidation in astrocytes: roles of glutamate dehydrogenase and aminotransferases: role of GDH in glutamate oxidation in astrocytes.J. Neurosci. Res.941561–1571. 10.1002/jnr.23908

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 114

  Meier C. (2002). Activation of system L heterodimeric amino acid exchangers by intracellular substrates.EMBO J.21580–589. 10.1093/emboj/21.4.580

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 115

  Michalak A. Rose C. Butterworth J. Butterworth R. F. (1996). Neuroactive amino acids and glutamate (n.d.) receptors in frontal cortex of rats with experimental acute liver failure.Hepatology24908–913. 10.1002/hep.510240425

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 116

  Michalec K. Mysiorek C. Kuntz M. Bérézowski V. Szczepankiewicz A. A. Wilczyński G. M. et al (2014). Protein kinase C restricts transport of carnitine by amino acid transporter ATB0,+ apically localized in the blood–brain barrier.Arch. Biochem. Biophys.55428–35. 10.1016/j.abb.2014.05.006

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 117

  Milewski K. Bogacińska-Karaś M. Fręśko I. Hilgier W. Jaźwiec R. Albrecht J. et al (2017). Ammonia reduces intracellular asymmetric dimethylarginine in cultured astrocytes stimulating its y+LAT2 carrier-mediated loss.IJMS18:2308. 10.3390/ijms18112308

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 118

  Milewski K. Bogacińska-Karaś M. Hilgier W. Albrecht J. Zielińska M. (2019). TNFα increases STAT3-mediated expression of glutaminase isoform KGA in cultured rat astrocytes.Cytokine123:54774. 10.1016/j.cyto.2019.154774

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 119

  Minn A. (1982). Glutamine uptake by isolated rat brain mitochondria.Neuroscience72859–2865. 10.1016/0306-4522(82)90108-7

  • CrossRef
  • Google Scholar

• 120

  Molina M. Segura J. A. Aledo J. C. Medina M. A. Núnez de Castro I. Márquez J. (1995). Glutamine transport by vesicles isolated from tumour-cell mitochondrial inner membrane.Biochem. J.308629–633. 10.1042/bj3080629

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 121

  Murthy C. R. Rama Rao K. V. Bai G. Norenberg M. D. (2001). Ammonia-induced production of free radicals in primary cultures of rat astrocytes.J. Neurosci. Res.66282–288. 10.1002/jnr.1222

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 122

  Nagaraja T. N. Brookes N. (1996). Glutamine transport in mouse cerebral astrocytes.J. Neurochem.661665–1674. 10.1046/j.1471-4159.1996.66041665.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 123

  Nakanishi T. Kekuda R. Fei Y. J. Hatanaka T. Sugawara M. Martindale R. G. et al (2001a). Cloning and functional characterization of a new subtype of the amino acid transport system N.Am. J. Physiol. Cell Physiol.281C1757–C1768. 10.1152/ajpcell.2001.281.6.C1757

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 124

  Nakanishi T. Sugawara M. Huang W. Martindale R. G. Leibach F. H. Ganapathy M. E. et al (2001b). Structure, function, and tissue expression pattern of human SN2, a subtype of the amino acid transport system N.Biochem. Biophys. Res. Commun.2811343–1348. 10.1006/bbrc.2001.4504

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 125

  Nałęcz K. A. (2020). Amino acid transporter SLC6A14 (ATB0,+) – a target in combined anti-cancer therapy.Front. Cell Dev. Biol.8:594464. 10.3389/fcell.2020.594464

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 126

  Nicklin P. Bergman P. Zhang B. Triantafellow E. Wang H. Nyfeler B. et al (2009). Bidirectional transport of amino acids regulates mTOR and autophagy.Cell136521–534. 10.1016/j.cell.2008.11.044

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 127

  Nissen-Meyer L. S. H. Chaudhry F. A. (2013). Protein kinase c phosphorylates the system n glutamine transporter SN1 (Slc38a3) and regulates its membrane trafficking and degradation.Front. Endocrinol.4:138. 10.3389/fendo.2013.00138

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 128

  Norenberg M. D. (1977). A light and electron microscopic study of experimental portal-systemic (ammonia) encephalopathy. Progression and reversal of the disorder.Lab. Invest.36618–627.

  • Pubmed Abstract
  • Google Scholar

• 129

  Norenberg M. D. (1987). The role of astrocytes in hepatic encephalopathy.Neurochem. Pathol.613–33. 10.1007/BF02833599

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 130

  Norenberg M. D. Rama Rao K. V. Jayakumar A. R. (2004). Ammonia neurotoxicity and the mitochondrial permeability transition.J. Bioenerg. Biomembr.36303–307. 10.1023/B:JOBB.0000041758.20071.19

  • CrossRef
  • Google Scholar

• 131

  O’Brien K. B. Miller R. F. Bowser M. T. (2005). D-Serine uptake by isolated retinas is consistent with ASCT-mediated transport.Neurosci. Lett.38558–63. 10.1016/j.neulet.2005.05.009

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 132

  O’Kane R. L. Hawkins R. A. (2003). Na ⁺ –dependent transport of large neutral amino acids occurs at the abluminal membrane of the blood-brain barrier.Am. J. Physiol. Endocrinol. Metab.285E1167–E1173. 10.1152/ajpendo.00193.2003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 133

  Obara-Michlewska M. Ding F. Popek M. Verkhratsky A. Nedergaard M. Zielinska M. et al (2018). Interstitial ion homeostasis and acid-base balance are maintained in oedematous brain of mice with acute toxic liver failure.Neurochem. Int.118286–291. 10.1016/j.neuint.2018.05.007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 134

  Odeh M. Sabo E. Srugo I. Oliven A. (2004). Serum levels of tumor necrosis factor-alpha correlate with severity of hepatic encephalopathy due to chronic liver failure.Liver Int.24110–116. 10.1111/j.1478-3231.2004.0894.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 135

  Oehler R. Roth E. (2003). Regulative capacity of glutamine.Curr. Opin. Clin. Nutr. Metab. Care6277–282. 10.1097/01.mco.0000068962.34812.ac

  • CrossRef
  • Google Scholar

• 136

  Ong J. P. Aggarwal A. Krieger D. Easley K. A. Karafa M. T. Van Lente F. et al (2003). Correlation between ammonia levels and the severity of hepatic encephalopathy.Am. J. Med.114188–193. 10.1016/S0002-9343(02)01477-8

  • CrossRef
  • Google Scholar

• 137

  Ott P. Larsen F. S. (2004). Blood–brain barrier permeability to ammonia in liver failure: a critical reappraisal.Neurochem. Int.44185–198. 10.1016/S0197-0186(03)00153-0

  • CrossRef
  • Google Scholar

• 138

  Papadopoulos M. C. Verkman A. S. (2007). Aquaporin-4 and brain edema.Pediatr. Nephrol.22778–784. 10.1007/s00467-006-0411-0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 139

  Pasantes-Morales H. Franco R. Ordaz B. Ochoa L. D. (2002). Mechanisms counteracting swelling in brain cells during hyponatremia.Arch. Med. Res.33237–244. 10.1016/S0188-4409(02)00353-3

  • CrossRef
  • Google Scholar

• 140

  Perry T. L. Hansen S. Kennedy J. (1975). CSF amino acids and plasma-CSF amino acid ratios in adults.J. Neurochem.24587–589. 10.1111/j.1471-4159.1975.tb07680.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 141

  Pfeiffer R. Spindler B. Loffing J. Skelly P. J. Shoemaker C. B. Verrey F. (1998). Functional heterodimeric amino acid transporters lacking cysteine residues involved in disulfide bond.FEBS Lett.439157–162. 10.1016/S0014-5793(98)01359-3

  • CrossRef
  • Google Scholar

• 142

  Pichili V. B. R. Rao K. V. R. Jayakumar A. R. Norenberg M. D. (2007). Inhibition of glutamine transport into mitochondria protects astrocytes from ammonia toxicity.Glia55801–809. 10.1002/glia.20499

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 143

  Pluta R. Albrecht J. (1986). Changes in arterial and cerebral venous blood gases, cerebral blood flow and cerebral oxygen consumption at different stages of thioacetamide-induced hepatogenic encephalopathy in rat.Resuscitation14135–139. 10.1016/0300-9572(86)90117-6

  • CrossRef
  • Google Scholar

• 144

  Pochini L. Scalise M. Galluccio M. Indiveri C. (2014). Membrane transporters for the special amino acid glutamine: structure/function relationships and relevance to human health.Front. Chem.2:61. 10.3389/fchem.2014.00061

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 145

  Popek M. Bobula B. Sowa J. Hess G. Frontczak-Baniewicz M. Albrecht J. et al (2020). Physiology and morphological correlates of excitatory transmission are preserved in glutamine transporter SN1-depleted mouse frontal cortex.Neuroscience446124–136. 10.1016/j.neuroscience.2020.08.019

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 146

  Popek M. Bobula B. Sowa J. Hess G. Polowy R. Filipkowski R. K. et al (2018). Cortical synaptic transmission and plasticity in acute liver failure are decreased by presynaptic events.Mol. Neurobiol.551244–1258. 10.1007/s12035-016-0367-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 147

  Rama Rao K. V. Norenberg M. D. (2012). Brain energy metabolism and mitochondrial dysfunction in acute and chronic hepatic encephalopathy.Neurochem. Int.60697–706. 10.1016/j.neuint.2011.09.007

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 148

  Rama Rao K. V. Norenberg M. D. (2014). Glutamine in the pathogenesis of hepatic encephalopathy: the trojan horse hypothesis revisited.Neurochem. Res.39593–598. 10.1007/s11064-012-0955-2

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 149

  Rama Rao K. V. Reddy P. V. B. Tong X. Norenberg M. D. (2010). Brain edema in acute liver failure.Am. J. Pathol.1761400–1408. 10.2353/ajpath.2010.090756

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 150

  Rao V. L. Audet R. M. Butterworth R. F. (1995). Selective alterations of extracellular brain amino acids in relation to function in experimental portal-systemic encephalopathy: results of an in vivo microdialysis study.J. Neurochem.651221–1228. 10.1046/j.1471-4159.1995.65031221.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 151

  Roberg B. (1995). The orientation of phosphate activated glutaminase in the inner mitochondrial membrane of synaptic and non-synaptic rat brain mitochondria.Neurochem. Int.27367–376. 10.1016/0197-0186(95)00018-4

  • CrossRef
  • Google Scholar

• 152

  Rodrigo R. Cauli O. Gomez-Pinedo U. Agusti A. Hernandez-Rabaza V. Garcia-Verdugo J. et al (2010). Hyperammonemia induces neuroinflammation that contributes to cognitive impairment in rats with hepatic encephalopathy.Gastroenterology139675–684. 10.1053/j.gastro.2010.03.040

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 153

  Rose C. F. Verkhratsky A. Parpura V. (2013). Astrocyte glutamine synthetase: pivotal in health and disease.Biochem. Soc. Trans.411518–1524. 10.1042/BST20130237

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 154

  Rothman D. L. Behar K. L. Hyder F. Shulman R. G. (2003). In vivo NMR studies of the glutamate neurotransmitter flux and neuroenergetics: implications for brain function.Annu. Rev. Physiol.65401–427. 10.1146/annurev.physiol.65.092101.142131

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 155

  Rubio-Aliaga I. Wagner C. A. (2016). Regulation and function of the SLC38A3/SNAT3 glutamine transporter.Channels10440–452. 10.1080/19336950.2016.1207024

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 156

  Samluk L. Czeredys M. Nałęcz K. A. (2010). Regulation of amino acid/carnitine transporter B0,+ (ATB0,+) in astrocytes by protein kinase C: independent effects on raft and non-raft transporter subpopulations: regulation of ATB0,+ by protein kinase C.J. Neurochem.1151386–1397. 10.1111/j.1471-4159.2010.07040.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 157

  Scalise M. Galluccio M. Console L. Pochini L. Indiveri C. (2018a). The human SLC7A5 (LAT1): the intriguing histidine/large neutral amino acid transporter and its relevance to human health.Front. Chem.6:243. 10.3389/fchem.2018.00243

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 158

  Scalise M. Pochini L. Console L. Losso M. A. Indiveri C. (2018b). The human SLC1A5 (ASCT2) amino acid transporter: from function to structure and role in cell biology.Front. Cell Dev. Biol.6:96. 10.3389/fcell.2018.00096

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 159

  Schliess F. Görg B. Fischer R. Desjardins P. Bidmon H. J. Herrmann A. et al (2002). Ammonia induces MK-801-sensitive nitration and phosphorylation of protein tyrosine residues in rat astrocytes.FASEB J.16739–741. 10.1096/fj.01-0862fje

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 160

  Schousboe A. Scafidi S. Bak L. K. Waagepetersen H. S. McKenna M. C. (2014). “Glutamate metabolism in the brain focusing on astrocytes,” in Glutamate and ATP at the Interface of Metabolism and Signaling in the BrainAdvances in Neurobiology, edsParpuraV.SchousboeA.VerkhratskyA. (Cham: Springer International Publishing), 13–30. 10.1007/978-3-319-08894-5_2

  • CrossRef
  • Google Scholar

• 161

  Scott T. R. (2013). Pathophysiology of cerebral oedema in acute liver failure.WJG19:9240. 10.3748/wjg.v19.i48.9240

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 162

  Sen K. Castillo Pinto C. Gropman A. L. (2021). Expanding role of proton magnetic resonance spectroscopy: timely diagnosis and treatment initiation in partial ornithine transcarbamylase deficiency.J. Pediatr. Genet.1077–80. 10.1055/s-0040-1709670

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 163

  Shawcross D. L. Wright G. Olde Damink S. W. M. Jalan R. (2007). Role of ammonia and inflammation in minimal hepatic encephalopathy.Metab. Brain Dis.22125–138. 10.1007/s11011-006-9042-1

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 164

  Sidoryk-Węgrzynowicz M. Lee E. Albrecht J. Aschner M. (2009). Manganese disrupts astrocyte glutamine transporter expression and function.J. Neurochem.110822–830. 10.1111/j.1471-4159.2009.06172.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 165

  Sinke A. P. Jayakumar A. R. Panickar K. S. Moriyama M. Reddy P. V. B. Norenberg M. D. (2008). NFB in the mechanism of ammonia-induced astrocyte swelling in culture.J. Neurochem.1062302–2311. 10.1111/j.1471-4159.2008.05549.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 166

  Sivaprakasam S. Sikder M. O. F. Ramalingam L. Kaur G. Dufour J. M. Moustaid-Moussa N. et al (2021). SLC6A14 deficiency is linked to obesity, fatty liver, and metabolic syndrome but only under conditions of a high-fat diet.Biochim. Biophys. Acta1867:166087. 10.1016/j.bbadis.2021.166087

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 167

  Sloan J. L. Mager S. (1999). Cloning and functional expression of a human Na+and Cl–dependent neutral and cationic amino acid transporter B0+.J. Biol. Chem.27423740–23745. 10.1074/jbc.274.34.23740

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 168

  Solbu T. T. (2010). SAT1, a glutamine transporter, is preferentially expressed in GABAergic neurons.Front. Neuroanat4:1. 10.3389/neuro.05.001.2010

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 169

  Spodenkiewicz M. Diez-Fernandez C. Rüfenacht V. Gemperle-Britschgi C. Häberle J. (2016). Minireview on glutamine synthetase deficiency, an ultra-rare inborn error of amino acid biosynthesis.Biology5:40. 10.3390/biology5040040

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 170

  Steib A. Rendon A. Mark J. Borg J. (1986). Preferential glutamine uptake in rat brain synaptic mitochondria.FEBS Lett.20763–68. 10.1016/0014-5793(86)80013-8

  • CrossRef
  • Google Scholar

• 171

  Sterns R. H. Silver S. M. (2006). Brain volume regulation in response to hypo-osmolality and its correction.Am. J. Med.119S12–S16. 10.1016/j.amjmed.2006.05.003

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 172

  Stravitz R. T. Larsen F. S. (2009). Therapeutic hypothermia for acute liver failure.Crit. Care Med.37S258–S264. 10.1097/CCM.0b013e3181aa5fb8

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 173

  Takahashi H. Koehler R. C. Brusilow S. W. Traystman R. J. (1991). Inhibition of brain glutamine accumulation prevents cerebral edema in hyperammonemic rats.Am. J. Physiol.261H825–H829. 10.1152/ajpheart.1991.261.3.H825

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 174

  Tanigami H. Rebel A. Martin L. J. Chen T.-Y. Brusilow S. W. Traystman R. J. et al (2005). Effect of glutamine synthetase inhibition on astrocyte swelling and altered astroglial protein expression during hyperammonemia in rats.Neuroscience131437–449. 10.1016/j.neuroscience.2004.10.045

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 175

  Tapiero H. Mathé G. Couvreur P. Tew K. D. (2002). II. Glutamine and glutamate.Biomed. Pharmacother.56446–457. 10.1016/S0753-3322(02)00285-8

  • CrossRef
  • Google Scholar

• 176

  Tǎrlungeanu D. C. Deliu E. Dotter C. P. Kara M. Janiesch P. C. Scalise M. et al (2016). Impaired amino acid transport at the blood brain barrier is a cause of autism spectrum disorder.Cell1671481.e–1494.e. 10.1016/j.cell.2016.11.013

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 177

  Thrane A. S. Rappold P. M. Fujita T. Torres A. Bekar L. K. Takano T. et al (2011). Critical role of aquaporin-4 (AQP4) in astrocytic Ca2+ signaling events elicited by cerebral edema.Proc. Natl. Acad. Sci. U.S.A.108846–851. 10.1073/pnas.1015217108

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 178

  Todd A. C. Marx M.-C. Hulme S. R. Bröer S. Billups B. (2017). SNAT3-mediated glutamine transport in perisynaptic astrocytes in situ is regulated by intracellular sodium.Glia65900–916. 10.1002/glia.23133

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 179

  Tofteng F. Hauerberg J. Hansen B. A. Pedersen C. B. Jørgensen L. Larsen F. S. (2006). Persistent arterial hyperammonemia increases the concentration of glutamine and alanine in the brain and correlates with intracranial pressure in patients with fulminant hepatic failure.J. Cereb. Blood Flow Metab.2621–27. 10.1038/sj.jcbfm.9600168

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 180

  Tofteng F. Jorgensen L. Hansen B. A. Ott P. Kondrup J. Larsen F. S. (2002). Cerebral microdialysis in patients with fulminant hepatic failure: cerebral microdialysis in patients with fulminant hepatic failure.Hepatology361333–1340. 10.1002/hep.1840360607

  • CrossRef
  • Google Scholar

• 181

  Torrents D. Estévez R. Pineda M. Fernández E. Lloberas J. Shi Y. B. et al (1998). Identification and characterization of a membrane protein (y+L amino acid transporter-1) that associates with 4F2hc to encode the amino acid transport activity y+L. A candidate gene for lysinuric protein intolerance.J. Biol. Chem.27332437–32445. 10.1074/jbc.273.49.32437

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 182

  Traber P. G. Canto M. D. Ganger D. R. Blei A. T. (1987). Electron microscopic evaluation of brain edema in rabbits with galactosamine-induced fulminant hepatic failure: ultrastructure and integrity of the blood-brain barrier.Hepatology71272–1277. 10.1002/hep.1840070616

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 183

  Traber P. DalCanto M. Ganger D. Blei A. T. (1989). Effect of body temperature on brain edema and encephalopathy in the rat after hepatic devascularization.Gastroenterology96885–891.

  • Pubmed Abstract
  • Google Scholar

• 184

  Vaquero J. Blei A. T. (2004). Cooling the patient with acute liver failure.Gastroenterology1271626–1629. 10.1053/j.gastro.2004.09.058

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 185

  Vaquero J. Butterworth R. F. (2007). Mechanisms of brain edema in acute liver failure and impact of novel therapeutic interventions.Neurol. Res.29683–690. 10.1179/016164107X240099

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 186

  Vercellino I. Sazanov L. A. (2022). The assembly, regulation and function of the mitochondrial respiratory chain.Nat. Rev. Mol. Cell Biol.23141–161. 10.1038/s41580-021-00415-0

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 187

  Verkhratsky A. Parpura V. Li B. Scuderi C. (2021). “Astrocytes: the housekeepers and guardians of the CNS,” in Astrocytes in Psychiatric DisordersAdvances in Neurobiology, edsLiB.ParpuraV.VerkhratskyA.ScuderiC. (Cham: Springer International Publishing), 21–53. 10.1007/978-3-030-77375-5_2

  • CrossRef
  • Google Scholar

• 188

  Wagner C. A. Lang F. Bröer S. (2001). Function and structure of heterodimeric amino acid transporters.Am. J. Physiol.281C1077–C1093. 10.1152/ajpcell.2001.281.4.C1077

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 189

  Wang B. Wu G. Zhou Z. Dai Z. Sun Y. Ji Y. et al (2015). Glutamine and intestinal barrier function.Amino Acids472143–2154. 10.1007/s00726-014-1773-4

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 190

  Wang Q. Holst J. (2015). L-type amino acid transport and cancer: targeting the mTORC1 pathway to inhibit neoplasia.Am. J. Cancer Res.51281–1294.

  • Pubmed Abstract
  • Google Scholar

• 191

  Wang Y. Fu L. Cui M. Wang Y. Xu Y. Li M. et al (2017). Amino acid transporter SLC38A3 promotes metastasis of non-small cell lung cancer cells by activating PDK1.Cancer Lett.3938–15. 10.1016/j.canlet.2017.01.036

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 192

  Wilkinson S. P. Arroyo V. Moodie H. Williams R. (1974). Proceedings: endotoxaemia in fulminant hepatic failure.Clin. Sci. Mol. Med.4630–31. 10.1042/cs046030pb

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 193

  Willard-Mack C. L. Koehler R. C. Hirata T. Cork L. C. Takahashi H. Traystman R. J. et al (1996). Inhibition of glutamine synthetase reduces ammonia-induced astrocyte swelling in rat.Neuroscience71589–599. 10.1016/0306-4522(95)00462-9

  • CrossRef
  • Google Scholar

• 194

  Wise D. R. DeBerardinis R. J. Mancuso A. Sayed N. Zhang X.-Y. Pfeiffer H. K. et al (2008). Myc regulates a transcriptional program that stimulates mitochondrial glutaminolysis and leads to glutamine addiction.Proc. Natl. Acad. Sci. U.S.A.10518782–18787. 10.1073/pnas.0810199105

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 195

  Witt A. M. Larsen F. S. Bjerring P. N. (2017). Accumulation of lactate in the rat brain during hyperammonaemia is not associated with impaired mitochondrial respiratory capacity.Metab. Brain Dis.32461–470. 10.1007/s11011-016-9934-7

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 196

  Wyke R. J. Canalese J. C. Gimson A. E. Williams R. (1982). Bacteraemia in patients with fulminant hepatic failure.Liver245–52. 10.1111/j.1600-0676.1982.tb00177.x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 197

  Xu G.-Y. McAdoo D. J. Hughes M. G. Robak G. de Castro R. (1998). Considerations in the determination by microdialysis of resting extracellular amino acid concentrations and release upon spinal cord injury.Neuroscience861011–1021. 10.1016/S0306-4522(98)00063-3

  • CrossRef
  • Google Scholar

• 198

  Yoo H. C. Park S. J. Nam M. Kang J. Kim K. Yeo J. H. et al (2020). A Variant of SLC1A5 is a mitochondrial glutamine transporter for metabolic reprogramming in cancer cells.Cell Metab.31267.e–283.e. 10.1016/j.cmet.2019.11.020

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 199

  Ytrebø L. M. Kristiansen R. G. Maehre H. Fuskevåg O. M. Kalstad T. Revhaug A. et al (2009). L-ornithine phenylacetate attenuates increased arterial and extracellular brain ammonia and prevents intracranial hypertension in pigs with acute liver failure.Hepatology50165–174. 10.1002/hep.22917

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 200

  Yudkoff M. Daikhin Y. Nissim I. Nissim I. (2000). Acidosis and astrocyte amino acid metabolism.Neurochem. Int.36329–339. 10.1016/S0197-0186(99)00141-2

  • CrossRef
  • Google Scholar

• 201

  Zalman L. S. Nikaido H. Kagawa Y. (1980). Mitochondrial outer membrane contains a protein producing nonspecific diffusion channels.J. Biol. Chem.2551771–1774.

  • Pubmed Abstract
  • Google Scholar

• 202

  Zaragozá R. (2020). Transport of amino acids across the blood-brain barrier.Front. Physiol.11:973. 10.3389/fphys.2020.00973

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 203

  Zielińska M. Dąbrowska K. Hadera M. G. Sonnewald U. Albrecht J. (2016). System N transporters are critical for glutamine release and modulate metabolic fluxes of glucose and acetate in cultured cortical astrocytes: changes induced by ammonia.J. Neurochem.136329–338. 10.1111/jnc.13376

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 204

  Zielińska M. Law R. O. Albrecht J. (2003). Excitotoxic mechanism of cell swelling in rat cerebral cortical slices treated acutely with ammonia.Neurochem. Int.43299–303. 10.1016/s0197-0186(03)00015-9

  • CrossRef
  • Google Scholar

• 205

  Zielińska M. Milewski K. Skowrońska M. Gajos A. Ziemińska E. Beręsewicz A. et al (2015). Induction of inducible nitric oxide synthase expression in ammonia-exposed cultured astrocytes is coupled to increased arginine transport by upregulated y(+)LAT2 transporter.J. Neurochem.1351272–1281. 10.1111/jnc.13387

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 206

  Zielińska M. Popek M. Albrecht J. (2014). Roles of changes in active glutamine transport in brain edema development during hepatic encephalopathy: an emerging concept.Neurochem. Res.39599–604. 10.1007/s11064-013-1141-x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 207

  Zielińska M. Ruszkiewicz J. Hilgier W. Fręśko I. Albrecht J. (2011). Hyperammonemia increases the expression and activity of the glutamine/arginine transporter y+LAT2 in rat cerebral cortex: implications for the nitric oxide/cGMP pathway.Neurochem. Int.58190–195. 10.1016/j.neuint.2010.11.015

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 208

  Zielińska M. Skowrońska M. Fręśko I. Albrecht J. (2012). Upregulation of the heteromeric y+LAT2 transporter contributes to ammonia-induced increase of arginine uptake in rat cerebral cortical astrocytes.Neurochem. Int.61531–535. 10.1016/j.neuint.2012.02.021

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 209

  Ziemińska E. Dolińska M. Łazarewicz J. W. Albrecht J. (2000a). Induction of permeability transition and swelling of rat brain mitochondria by glutamine.Neurotoxicology21295–300.

  • Pubmed Abstract
  • Google Scholar

• 210

  Ziemińska E. Matyja E. Nałecz M. Salińska E. Ziembowicz A. Łazarewicz J. W. (2000b). In vivo brain microdialysis as a tool in studies of neuroprotective effects of cyclosporin A in acute excitotoxicity.Acta Pol. Pharm.57(Suppl.)129–133.

  • Pubmed Abstract
  • Google Scholar

• 211

  Ziemińska E. Hilgier W. Waagepetersen H. S. Hertz L. Sonnewald U. Schousboe A. et al (2004). Analysis of glutamine accumulation in rat brain mitochondria in the presence of a glutamine uptake inhibitor. histidine, reveals glutamine pools with a distinct access to deamidation.Neurochem. Res.292121–2123. 10.1007/s11064-004-6885-x

  • Pubmed Abstract
  • CrossRef
  • Google Scholar

• 212

  Zwingmann C. Chatauret N. Rose C. Leibfritz D. Butterworth R. F. (2004). Selective alterations of brain osmolytes in acute liver failure: protective effect of mild hypothermia.Brain Res.999118–123. 10.1016/j.brainres.2003.11.048

  • Pubmed Abstract
  • CrossRef
  • Google Scholar