Front. Behav. Neurosci. Frontiers in Behavioral Neuroscience Front. Behav. Neurosci. 1662-5153 Frontiers Media S.A. 10.3389/fnbeh.2021.699592 Neuroscience Review Functional Contribution of the Medial Prefrontal Circuitry in Major Depressive Disorder and Stress-Induced Depressive-Like Behaviors Bittar Thibault P. 1 2 Labonté Benoit 1 2 * 1CERVO Brain Research Centre, Québec, QC, Canada 2Department of Psychiatry and Neuroscience, Faculty of Medicine, Université Laval, Québec, QC, Canada

Edited by: Tiziana Rubino, University of Insubria, Italy

Reviewed by: Cecilia Hillard, Medical College of Wisconsin, United States; Bryan Kolb, University of Lethbridge, Canada

 *Correspondence: Benoit Labonté, benoit.labonte@fmed.ulaval.ca

This article was submitted to Pathological Conditions, a section of the journal Frontiers in Behavioral Neuroscience

 21 06 2021 2021 15 699592 23 04 2021 20 05 2021 Copyright © 2021 Bittar and Labonté. 2021 Bittar and Labonté

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Despite decades of research on the neurobiology of major depressive disorder (MDD), the mechanisms underlying its expression remain unknown. The medial prefrontal cortex (mPFC), a hub region involved in emotional processing and stress response elaboration, is highly impacted in MDD patients and animal models of chronic stress. Recent advances showed alterations in the morphology and activity of mPFC neurons along with profound changes in their transcriptional programs. Studies at the circuitry level highlighted the relevance of deciphering the contributions of the distinct prefrontal circuits in the elaboration of adapted and maladapted behavioral responses in the context of chronic stress. Interestingly, MDD presents a sexual dimorphism, a feature recognized in the molecular field but understudied on the circuit level. This review examines the recent literature and summarizes the contribution of the mPFC circuitry in the expression of MDD in males and females along with the morphological and functional alterations that change the activity of these neuronal circuits in human MDD and animal models of depressive-like behaviors.

 major depressive disorder functional studies neuronal circuit chronic stress (or “stress”) mouse model sex differences Introduction

Recent estimates from the World Health Organization (WHO) revealed that more than 300 million people of all ages suffer from major depressive disorder (MDD) worldwide (World Health Organization, 2018). Despite its enormous economic and human impact, MDD remains a highly pervasive and co-morbid disorder for which the scientific community has globally failed to provide underlying genetic and molecular etiologies (Fava and Kendler, 2000; Kendler et al., 2006; Flint and Kendler, 2014). This is particularly true considering low treatment efficacy despite the number of drugs that have been developed to treat MDD during the last 50 years (Nestler, 1998; Swedish Council on Health Technology Assessment, 2004). This persistent incapacity to treat the disease efficiently results in part from the heterogeneity of the disease and our poor understanding of the molecular and functional mechanisms underlying its expression.

MDD is a highly heterogeneous disorder characterized clinically by the expression of persistent depressed mood, anxiety, anhedonia, cognitive impairments, weight changes, fatigue, feeling of worthlessness, recurrent thoughts of death, and suicidal ideation (American Psychiatric Association, 2013, p. 5). These symptoms vary widely across patients and their expression evolves with the chronicity of the disease. Consequently, previous attempts at clustering patients based on their clinical profiles globally failed to identify more homogeneous groups of patients (Fried and Nesse, 2015). Another level of complexity and heterogeneity comes from the fact that MDD is a sexually dimorphic disease. Recent estimates have evaluated the prevalence of MDD to be 2–3 times higher in women compared to men (Weissman et al., 1993, 1996; Kim et al., 2015; World Health Organization, 2018). Clinical studies report women to exhibit higher scores of depression, younger age of onset, a higher number of depressive episodes, and relapse rates than men (Kessler et al., 1993, 2005; Nazroo et al., 1997; Parker et al., 2014; Breslau et al., 2017). Women have also been shown to exhibit higher rates of comorbid anxiety, cardiovascular disease risks, and atypical symptoms like sadness, sexual function impairment, susceptibility to physical pain, and vegetative state (Kornstein et al., 2000a; Lai, 2011; Shah et al., 2014; Bandelow and Michaelis, 2015; Kim et al., 2015; Karpyak et al., 2016). In contrast, men often exhibit comorbid substance abuse including alcohol and drugs (Grant et al., 2016; Karpyak et al., 2016). Men also display poorer impulse control and increased anger and aggressivity, and are more prone to take risks than women (Rice et al., 2013; Cavanagh et al., 2017; Athanasiadis et al., 2018). Furthermore, this sexual dimorphism is also observed at the treatment level with studies suggesting better responses in men treated with tricyclic antidepressant drugs (TCA), and selective serotonin reuptake inhibitors (SSRI) in women (Kornstein et al., 2000b; Khan et al., 2005; Young et al., 2009; Dalla et al., 2010), although these findings have been contested (Thase et al., 2005; Sramek et al., 2016).

A growing body of evidence now suggests that the expression of different symptoms in males and females may results from the alterations of distinct pathways and circuits in the brain with the medial prefrontal cortex (mPFC) acting as a hub structure. For instance, elevated functional connectivity of the mPFC with the posterior cingulate cortex and angular gyrus is associated with rumination while hypoactivation of the ventral striatum associates with the expression of anhedonia (Williams, 2016). Interestingly, hyperactivity of the ACC has also been associated with better responses to antidepressants in MDD patients (Phillips et al., 2015). Finally, functional studies in treatment-resistant MDD patients have consistently revealed hyperactivity in the mPFC (Hadas et al., 2019; Morris et al., 2020) which can be reversed by the stimulation of the subcallosal cingulate cortex along with a reversal of the depressive symptomatology (Holtzheimer et al., 2017). Interestingly, changes in the activity of these pathways have been consistently associated with morphological (Drevets et al., 2008; Zhao et al., 2014) and sex-specific molecular (Gray et al., 2015; Labonté et al., 2017; Seney et al., 2018) changes that further support the role of the mPFC as a hub region in mediating the expression of MDD in men and women.

The hub status of the mPFC is further strengthened by anatomical and functional studies performed in animal models of chronic stress. The mPFC integrates neuronal inputs from several brain regions (Zhang et al., 2010; Gabbott et al., 2012; Linley et al., 2013) and sends neuronal projections to several cortical and limbic structures (Gabbott et al., 2005; Kim et al., 2017). Through these functional connections, the mPFC controls several cognitive and behavioral functions such as attention, habit formation, decision making, long-term memory, working memory, aversive and appetitive stimuli processing, and emotional and inhibitory control (Bechara et al., 2000; Ridderinkhof et al., 2004; Euston et al., 2012; Kumar et al., 2013; Laubach et al., 2015; Moorman et al., 2015; Wellman and Moench, 2019). Importantly, alterations of these fundamental processes are believed to result in the expression of depressive-like behaviors (Keedwell et al., 2005; Murrough et al., 2011). This has been strongly supported by an increasing number of functional studies in animal models of chronic stress dissecting the contribution of the different neuronal circuits of the mPFC in the expression of depressive-like behaviors in males and females (Vialou et al., 2014; Bagot et al., 2015; Dolzani et al., 2018; Liu W.-Z. et al., 2020; Marcus et al., 2020; Bittar et al., 2021). Here, we review the literature on the involvement of the mPFC and its neuronal circuitry in mediating the expression of depressive-like behaviors. We start by defining the anatomical and cytoarchitectural organization of the mPFC circuitry. We then elaborate on the functional and morphological impact of chronic stress on excitatory pyramidal neurons and GABAergic interneurons in the mPFC. Finally, we provide an overview of the most recent studies supporting the role of mPFC circuits in mediating the expression of specific behavioral phenotypes in animal models of depressive-like behaviors.

 Cell Type-Specific Distribution and Anatomical Organization of the mPFC Anatomical Organization

Consistent with its crucial role in higher executive functions, the mPFC is more developed in higher order mammals, and exhibit more elaborate behaviors than rodents (Kerney et al., 2017; Noonan et al., 2018). In humans, the mPFC is composed of different structures from dorsal to ventral: the dorsal anterior cingulate cortex (dACC, Brodmann area 32), the pregenual anterior cingulate cortex (pACC, Brodmann area 24), and the subgenual cingulate cortex (sACC, Brodmann area 25) (aan het Rot et al., 2009). The dACC is involved in detecting and filtering salient stimuli (Menon and Uddin, 2010), while the pACC and sACC are relevant to emotion processing and regulation of attention (Palomero-Gallagher et al., 2019). In contrast, the rodent mPFC is subdivided into four anatomically and functionally distinct sub-regions (Heidbreder and Groenewegen, 2003). The dorsal part, named dorsomedial prefrontal cortex (dmPFC), encompasses the secondary motor area (M2) and the anterior cingulate cortex (ACC). The ventral part, named ventromedial prefrontal cortex (vmPFC), includes the prelimbic cortex (PLC) and the infralimbic cortex (ILC). The evolution of the brain complexity and morphology (curvature notably) across species renders the comparison between humans and rodents difficult although equivalent structures (functionally and anatomically) have been suggested. The rodent PLC is described as the human pACC and the rodent ILC as the human equivalent of the sACC (Bicks et al., 2015; Ko, 2017; Laubach et al., 2018). Therefore, these rodent structures fill the same functions as their human counterparts: attention, habit formation, decision making, long-term memory, working memory, emotional control, and inhibitory control (Bechara et al., 2000; Ridderinkhof et al., 2004; Euston et al., 2012; Kumar et al., 2013; Laubach et al., 2015; Moorman et al., 2015; Wellman and Moench, 2019). Additionally, the mPFC is also thought to exert top-down executive control over aversive and appetitive stimuli processing (Maroun, 2013) driven by limbic systems regulating stress responses (Price and Drevets, 2012; Riga et al., 2014).

 Cellular Heterogeneity

The mPFC is composed of two genetically distinct neuronal populations, consisting of excitatory pyramidal neurons (80–90%) and GABAergic inhibitory interneurons (10-20%) (Nieuwenhuys, 1994; Rudy et al., 2011). Pyramidal neurons in the mPFC produce glutamate as a neurotransmitter and express Ca2+/calmodulin kinase II (CaMKII) (Erondu and Kennedy, 1985; Burgin et al., 1990; Jones et al., 1994; Wang et al., 2013). Studies on rodents revealed that glutamatergic pyramidal neurons in the mPFC are derived from progenitors called radial glial cells (RGCs), located in the ventricular zone at early embryonic stages and maturating while migrating to the neocortical area including the mPFC (Meyer et al., 2000; Marín and Müller, 2014).

The remaining 10–20% are composed of different subtypes of inhibitory interneurons expressing gamma-aminobutyric acid (GABA) as a neurotransmitter (Markram et al., 2004; Narayanan and Laubach, 2017). GABA interneurons of the neocortex arise from RGCs located in the medial ganglionic eminence and the preoptic area during early embryonic stages (Zhu et al., 1999; Wonders and Anderson, 2006; Marín and Müller, 2014). GABA interneurons are composed of different subtypes with heterogeneous morphology, distribution, physiological properties, organization, and connectivity (Petilla Interneuron Nomenclature Group, 2008). These interneurons can be divided into one of the following three non-overlapping classes including those co-expressing the calcium-binding protein parvalbumin (PV, 40%), the neuropeptide somatostatin (SST, 30%), or the vasoactive intestinal peptide (VIP, 30%) (Rudy et al., 2011). VIP neurons are also expressing the specific serotonin receptor 5-HT3A (Rudy et al., 2011) and some PV neurons also express calretinin (Caballero et al., 2014). Interneuron subtypes follow an intracortical distribution and play different roles. VIP and a subset of SST interneurons are found in superficial layers I and II/III. Their role is to modulate excitatory inputs on the dendrites. They mediate lateral inhibition and regulate mPFC long-range inputs by contacting the dendritic tufts. PV interneurons located in deeper layers V and VI regulate the pyramidal neurons’ outputs by contacting the perisomatic regions of the pyramidal neurons. They control the firing synchronization and spike timing of the excitatory neurons in the area. A distinct population of SST interneurons in layers V and VI regulates the activity of these PV interneurons, contributing to the regulation of neuronal outputs. Finally, another population of SST neurons, also located in layers V and VI, assures negative feedback from the axon to the dendrites of pyramidal neurons (Murayama et al., 2009; Larkum, 2013). See the following review for more detailed information (Fee et al., 2017).

 Laminar Organization

The human mPFC is organized in six layers while rodents lack layer IV (Uylings et al., 2003). Pyramidal neurons are found in layers II/III, IV, V, and VI while GABAergic interneurons populate layers II/III and V predominantly (Douglas and Martin, 2004). Even though the mPFC mainly receives afferences in superficial layers I and II/III, the deep layers V and VI also receive long-range cortical and sub-cortical inputs (Douglas and Martin, 2004; Hoover and Vertes, 2007). These afferences communicate with mPFC neurons through different neurotransmitter systems such as glutamatergic projections from the hippocampus, amygdala, and thalamus (Goldman-Rakic et al., 1984; Barbas and Olmos, 1990; Gabbott et al., 2012), dopaminergic projections from the ventral tegmental area (VTA) (Christie et al., 1985), serotonergic projections from the dorsal raphe nuclei (DRN) (Van Bockstaele et al., 1993) and noradrenergic projections from the locus coeruleus (LC) (Runnels et al., 2009; Figure 1A). These afferences follow a precise topological organization. For instance, inputs from the LC concentrate mainly in layers I and II/III, dopaminergic nerve terminals from the VTA populate preferentially layers V and VI (Vander Weele et al., 2018; Quessy et al., 2021), the amygdala innervates mainly layers II and V (Aggleton et al., 2015; McGarry and Carter, 2016), serotonergic inputs arrive mainly in layers I and V/VI and sparser proportions in layer II/III (Linley et al., 2013), and projections from the hippocampus are located in layers II/III and V (Liu and Carter, 2018; Figure 2).

Medial prefrontal cortex inputs and outputs. Schematic representation of the (A) afferent and (B) efferent projections in the medial prefrontal cortex with their respective neurotransmitter systems. AMY, amygdala; DRN, dorsal raphe nucleus; LC, locus coeruleus; LHb, lateral habenula; mPFC, medial prefrontal cortex; NAc, nucleus accumbens; Th, thalamus; vHIPP, ventral hippocampus; VTA, ventral tegmental area.

Cellular organization of the medial prefrontal cortex. The medial prefrontal cortex is organized in layers, numbered I (medial, close to the midline) to VI (lateral). Pyramidal glutamate neurons are lying in layers II/III (red), V (green), and VI (not represented), while GABAergic interneurons (somatostatin in purple, parvalbumin in blue, and vasoactive intestinal peptide in brown) are spread in layers I, II/III and V. The mPFC receives layer-specific inputs (dark blue and yellow) from locus coeruleus (LC), basolateral and basomedial amygdala (BLA and BMA), ventral hippocampus (vHIPP), dorsal raphe (DRN) and ventral tegmental area (VTA) while mPFC pyramidal neurons send projections (red and green) to the nucleus accumbens (NAc), dorsal striatum (DSt), BLA, contralateral PFC, thalamus, VTA and brainstem nuclei.

In return, mPFC neurons send glutamatergic projections to nucleus accumbens (NAc), hippocampus, amygdala, lateral habenula, thalamus and hypothalamus, DRN, VTA, periaqueducal gray (PAG), and LC (Porrino and Goldman-Rakic, 1982; Arnsten and Goldman-Rakic, 1984; Takagishi and Chiba, 1991; Gabbott et al., 2005; Gonçalves et al., 2009; Vander Weele et al., 2018) and also GABAergic projections to the NAc (Lee et al., 2014; Figure 1B). Interestingly, a clear dichotomy in the laminar organization of these projections can be observed between cortico-cortical and cortico-fugal projecting pyramidal neurons (Marín and Müller, 2014). Cortico-cortical neurons from layers II/III project to ipsilateral and contralateral cortical areas, while cortico-fugal neurons spread across layers II/III, V, and VI project mainly to subcortical regions. Subsequent differences can be made between cortico-fugal neurons (Figure 2) with NAc-projecting mPFC pyramidal neurons being mainly located in layers II/III and VTA-projecting mPFC neurons being mainly enriched in sublayers V (Gabbott et al., 2005; Kim et al., 2017; Bittar et al., 2021).

Together, the cellular diversity of the mPFC following a complex laminar and anatomical distribution is ideally organized to integrate the diverse sensory and emotional information coming from other brain regions and redirect it to other structures to drive behavioral responses to environmental challenges. In the next section of this review, we will elaborate on the morphological and functional consequences of chronic stress that have been described in the mPFC of males and females.

 The Impact of Chronic Stress on mPFC Neuronal Network’s Integrity Morphological Alterations

Previous studies performed on post-mortem tissue from MDD patients reported several neuroanatomical alterations in the mPFC. For instance, gray matter is reduced in the mPFC of patients suffering from MDD across its different sub-structures (Zhao et al., 2014; Kandilarova et al., 2019). Accordingly, morphological studies in human MDD post-mortem tissue revealed a consistent decrease in the number and length of dendrites and lower spine density in mPFC pyramidal neurons of depressed patients (Drevets et al., 2008; Kang et al., 2012). Although these alterations have been reported mainly in the male brain, most of the studies did not differentiate men from women (Rajkowska et al., 1999) and it is, therefore, difficult to conclude if these variations are sex-specific or not.

These findings in humans have been supported by studies in animal models of chronic stress. For instance, male rats exposed to chronic restraint stress exhibit a 20% reduction of the apical dendritic length and branch number (Cook and Wellman, 2004; Radley et al., 2004; Brown et al., 2005; Hains et al., 2009) with a significant reduction in spine density, volume and surface area in pyramidal neurons from layer II/III of the PLC and ACC (Radley et al., 2008; Hains et al., 2009; Duman and Duman, 2015). Interestingly, a similar decrease in spine density has been observed in susceptible but not resilient male mice following chronic social defeat stress (CSDS) (Qu et al., 2018) and in both males and females following prolonged social isolation (Sarkar and Kabbaj, 2016) in PLC pyramidal neurons but not in ILC. Noticeably, the acute administration of ketamine was shown to rescue spine density deficits in isolated males, but not females, and to reverse anhedonic behaviors and behavioral despair in both sexes (Sarkar and Kabbaj, 2016). These results suggest that the therapeutic action of this fast-acting antidepressant may be mediated through different molecular and functional mechanisms in males and females. Additionally, as it was shown in the human brain, these morphological changes have been associated with a decrease of cytoarchitectural gene expression and protein levels such as TUBB4 (Kang et al., 2012) in men and women.

More recently, exposure to 21 days of chronic variable stress (CVS) has been shown to induce sex-specific modifications in the dendritic complexity of two distinct pyramidal populations in the mPFC, namely NAc- or VTA-projecting mPFC neurons (Bittar et al., 2021). Indeed, in females, CVS was shown to decrease dendritic arborization much more importantly in NAc-projecting mPFC while VTA-projecting neurons showed a greater dendritic retraction in stressed males than females (Bittar et al., 2021). Together, this supports the idea that stress interferes with the morpho-functional properties of specific neuronal pathways in the mPFC, potentially through pathways-specific molecular changes affecting males and females differently, as suggested before in human MDD and animal models of depressive-like behaviors (Labonté et al., 2017; Seney et al., 2018; Scarpa et al., 2020; Bittar et al., 2021).

In addition to the effects mentioned above on pyramidal neurons, alterations in GABAergic interneurons have also been consistently reported in the mPFC of MDD patients. Density and size reduction of GABA interneurons, along with decreased expression of the 67kDa glutamic acid decarboxylase (GAD67) gene expression, have been reported in post-mortem mPFC tissue from MDD patients (Karolewicz et al., 2010). In contrast, more recent studies found no change in the number of SST-expressing GABAergic neurons in men and women mPFC although a reduction in SST mRNA expression levels was reported in the dorsolateral PFC and ACC with females exhibiting a much stronger decrease than men (Tripp et al., 2011; Seney et al., 2015). Here again, these findings have been supported in animal models of chronic stress. Indeed, dendritic hypertrophy was also reported in SST interneurons following chronic restraint stress in males (Gilabert-Juan et al., 2013) although, SST and neuropeptide Y protein levels were reduced in males after chronic unpredictable stress in the mPFC (Banasr et al., 2017). However, in contrast with data in humans, increases in the number of parvalbumin (PV) positive cells and PV mRNA in the PLC and ILC was reported in female mice after chronic unpredictable mild stress while in males, the number of PV positive cells was significantly increased only in the PLC with no change in PV mRNA expression (Shepard et al., 2016).

 E/I Balance Integrity in Stressed Males and Females

Overall, the sum of evidence reported here suggests that chronic stress induces a global reorganization of neuronal spine and arborization in the mPFC, disrupting the frontotemporal neuronal network’s integrity differently in males and females (Sarkar and Kabbaj, 2016; Bittar et al., 2021). Importantly, these sex-specific changes, affecting excitatory and inhibitory neuronal populations are likely to interfere with the balance between excitatory and inhibitory (E/I) tones required to maintain proper function of the mPFC (Fee et al., 2017).

At this point, whether chronic stress increases or decreases the E/I balance in the mPFC is still a matter of debate with functional studies that aim at modulating the activity of the mPFC, and report conflicting results. On one hand, studies increasing the excitability of mPFC pyramidal neurons or decreasing the inhibitory tone of GABAergic interneurons suggest that pyramidal hyperactivity in the mPFC associates with the expression of depressive-like behaviors. For instance, asynchronous optogenetic activation of pyramidal neurons in the mPFC was shown to induce the expression of depressive-like behaviors in male rats (Ferenczi et al., 2016). Previous studies showed that the optogenetic stimulation of the Stabilized Step-Function Opsin (SSFO) (Yizhar et al., 2011) in pyramidal neurons induces stable subthreshold neuronal depolarization, priming the neurons to natural endogenous stimuli (Berndt et al., 2009) and providing a more physiologically relevant increase in neuronal excitability. The activation of mPFC pyramidal neurons with this approach was shown to increase blood-oxygen-level dependent activity in the mPFC and trigger the expression of anhedonia and social avoidance with no motor or cognitive impairments in naive male rats (Ferenczi et al., 2016). Interestingly, this pattern of activity recapitulates some of the findings reported before in treatment-resistant MDD patients (Lozano et al., 2011; Li et al., 2013; Holtzheimer et al., 2017) and suggests that pyramidal neurons’ hyperactivity in the mPFC drives specific aspects of depressive-like phenotypes. This imbalance in the E/I ratio was also reported in mice following CVS. Indeed, the E/I frequency ratio was significantly shifted toward excitation in NAc-projecting mPFC neurons, with lower inhibitory inputs onto these neurons in both males and females, combined with stronger excitatory inputs, but only in stressed females (Bittar et al., 2021). In contrast, E/I imbalance in VTA-projecting mPFC neurons was only trending toward excitation with higher excitatory inputs in both sexes but no change in the inhibitory tones imposed over these neurons in both stressed males and females (Bittar et al., 2021). Interestingly, this was corroborated by pathway-specific variations in the expression of GABA and glutamate NMDA receptor subunits (Bittar et al., 2021) as a potential mechanistic explanation for these stress-induced functional changes.

Consistently, the inactivation of GABAergic inhibitory tones in the mPFC has also been shown to promote the expression of depressive-like behaviors. For instance, the acute chemogenetic inhibition of SST-expressing GABAergic interneurons in the PLC triggers anxiety-like behaviors in male and female mice (Soumier and Sibille, 2014). Chemogenetic inactivation of PV-expressing GABAergic interneurons during learned helplessness increases the escape latency and failure to escape as measures of behavioral despair (Perova et al., 2015). Furthermore, SST-KO mice exhibit depressive- and anxiety-like behaviors along with reductions of BDNF and GAD67 expression in GABA interneurons and elevated corticosterone blood levels (Lin and Sibille, 2015). By compiling human cellular, synaptic, and gene expression data from recent studies, Yao et al. (2021) generated computational models of human layer II/III local circuit. Among these models, they created a depression microcircuit model by reducing SST inhibition according to previous gene expression data from MDD patients (Seney et al., 2015). In this model, a reduction in SST inhibition leads to an increase in the pyramidal firing rate, increasing baseline activity, disrupting signal-to-noise ratio, and the increasing probabilities of both false signal detection and failed signal detection over background noise (Yao et al., 2021).

On the other hand, contrasting findings have been reported where the stimulation of pyramidal neurons in the mPFC has been associated with antidepressant responses. For instance, social withdrawal and anhedonia induced in males after 10 days of social defeat stress were shown to be reversed by optogenetic stimulations of the mPFC (Covington et al., 2010) while similar stimulation of pyramidal neurons in the infralimbic portion of the mPFC in naïve animals decreases helplessness, anhedonia, and anxiety (Fuchikami et al., 2015). Furthermore, although the acute chemogenetic inactivation of SST GABAergic interneurons in the mPFC induces anxiety-like behaviors, their prolonged inhibition over 21 days promoted antidepressant-like responses in males, increasing time spent in the open arms of the elevated plus-maze test (Soumier and Sibille, 2014).

Together, by interfering with the morphological and functional organization of pyramidal and GABAergic neurons in the mPFC, chronic stress interferes with the E/I balance controlling the function of the mPFC. The morphological adaptations observed in pyramidal and interneurons of the mPFC after chronic stress suggest that their ability to integrate and transmit correctly neuronal signals is compromised. This is leading to functional modifications that interfere with the E/I balance. A proper E/I balance assures proper responses to various stimuli received by these neurons. This being said, given the complex integrative role of the mPFC at the circuit level, it is likely that the morphological changes reported above may affect precise neuronal subpopulations that could be defined based on their inputs or outputs (Shansky et al., 2009) and by doing so, change the activity of neuronal pathways controlling emotional stress responses (Lin and Sibille, 2015; Knowland and Lim, 2018; Biselli et al., 2019; Bittar et al., 2021). In the following section, we will review the literature dissecting the functional and behavioral contributions of distinct neuronal circuits targeting or originating from the mPFC in the establishment of stress responses in males and females.

 Functional Contributions of the mPFC Circuitry in Mediating Behavioral Stress Responses Alterations in mPFC Afferences

The mPFC receives various afferences from cortical, subcortical and brainstem areas (Zhang et al., 2010; Gabbott et al., 2012; Linley et al., 2013; Vander Weele et al., 2018; Quessy et al., 2021) which have been shown to control several fundamental behavioral features such as memory formation, emotional processing, decision-making, attention and behavioral flexibility (Beversdorf et al., 1999; Gunaydin et al., 2014; Mitchell, 2015; Sharp, 2017; Phillips et al., 2019). With this in mind, recent studies investigating the contributions of these afferences in the elaboration and consolidation of stress responses address more specifically their roles in modulating anxiety, behavioral despair, social avoidance, and anhedonia-like behavioral features in males and females (Table 1).

Overview of preclinical studies involving mPFC afferences in anxiety-like and depressive-like behaviors.

Afferences Species Sex studied Stress Neuromodulatory approach Effects observed Tests performed References
Ventral Mouse Not specified Naive Chemogenetic activation Anxiogenic EPM, OFT Parfitt et al., 2017
hippocampus Mouse Not specified Naive Chemogenetic inhibition Anxiolytic
(vHIPP) Mouse Male Naive Optogenetic inhibition Anxiolytic, antidepressant EPM, OFT, NSF Padilla-Coreano et al., 2016
Basolateral amygdala (BLA) Mouse Male Naive Optogenetic stimulation Anxiogenic EPM Lowery-Gionta et al., 2018
Mouse Male Naive Optogenetic stimulation Anxiogenic, pro-depressive EPM, OFT, Social exploration Felix-Ortiz et al., 2016
Mouse Male Naive Optogenetic inhibition Anxiolytic, antidepressant OFT, Social exploration
Mouse Both Naive Chemogenetic activation Anxiogenic EPM Marcus et al., 2020
Locus coeruleus (LC) Rat Male Naive Chemogenetic activation Anxiogenic, aversive OFT, Place preference Hirschberg et al., 2017
Mediodorsal thalamus (MDT) Mouse Not specified Naive Chemogenetic activation Antidepressant FST, TST Miller et al., 2017
Rat Male Naive Optogenetic inhibition No effect FST Carreno et al., 2016
Mouse Male Naive Optogenetic inhibition No effect EPM Padilla-Coreano et al., 2016
Ventral tegmental area (VTA) Mouse Female Naive Optogenetic stimulation Anxiogenic EPM Gunaydin et al., 2014
Mouse Male Acute SDS Optogenetic inhibition Pro-depressive, anhedonia Social interaction, SPT Chaudhury et al., 2013
Mouse Male Acute SDS Optogenetic stimulation No effect
Mouse Male CSDS Optogenetic stimulation Antidepressant Social interaction Friedman et al., 2014

Neurons from the VTA projecting to the mPFC constitute the mesocortical pathway. The VTA itself, and more importantly, via its projections to the mPFC has been extensively studied for its contribution to aversive stimuli processing (Gunaydin et al., 2014; Lammel et al., 2014). Functional studies have also revealed the crucial impact of this dopaminergic pathway on the regulation of anxiety and social behaviors involved in emotional stress responses (Friedman et al., 2014; Liu D. et al., 2020). For instance, the optogenetic stimulation of the VTA-mPFC pathway in stress naïve female mice had an anxiogenic effect and triggered aversion in a conditioned place preference test (Gunaydin et al., 2014). Interestingly, this was not associated with any change in the social interaction test, suggesting that the mesocortical pathway is regulating aversion but not sociability. Additionally, the acute stimulation of this pathway had no noticeable effect on sociability and anhedonic behaviors in males after sub-threshold social defeat stress while the optogenetic inhibition of the VTA-mPFC pathway following sub-threshold CSDS was shown to induce social withdrawal in males (Chaudhury et al., 2013). Interestingly, the VTA-mPFC firing rate was significantly reduced in susceptible animals but not in resilient and control, suggesting that decreased activity of this pathway causes social avoidance in susceptible males (Chaudhury et al., 2013). Moreover, the density of dopamine axon terminals in the layers V and VI of the mPFC is reduced in male and female mice after CSDS (Quessy et al., 2021). Additionally, repeated optogenetic stimulation of mPFC-projecting VTA neurons in mice that underwent CSDS reversed social avoidance (Friedman et al., 2014). Another study also reported an increased c-Fos expression in the mPFC after optogenetic stimulation of the VTA dopamine neurons (Gunaydin et al., 2014).

The ventral hippocampus (vHIPP) sends dense glutamatergic projections to the mPFC with denser inputs in the vmPFC (Goldman-Rakic et al., 1984). This pathway was previously shown to be particularly relevant to social memory, emotional and motivational behaviors (Bannerman et al., 2004; Sigurdsson and Duvarci, 2016; Phillips et al., 2019). Interestingly, functional studies revealed the bidirectional control of this projection over the expression of anxiety-like behaviors (Padilla-Coreano et al., 2016; Parfitt et al., 2017). For instance, acute chemogenetic stimulation of mPFC-projecting vHIPP neurons in stress naïve mice induced anxiety-like behaviors with a decreased time spent in the open arms of the elevated plus-maze, an increased latency to feed in the novelty-suppressed feeding test, and a decreased time in the center in the open field test (Parfitt et al., 2017). On the contrary, inhibition of this pathway, either with chemogenetic or optogenetic approaches, alleviates anxiety-like behaviors in males as shown by the increased time spent in the open arms of the elevated plus-maze test (Padilla-Coreano et al., 2016). More work will be required to investigate whether this circuit contributes to the same behavior in females.

Projections from the basolateral amygdala (BLA) to the mPFC are also directly involved in the control of anxiety-like behaviors in mice. The mPFC receives excitatory glutamatergic inputs from the BLA targeting dmPFC and vmPFC in layers II/III and V (Gabbott et al., 2012). Traditionally, the BLA has been associated with the control of fear, anxiety, and reward learning (Wassum and Izquierdo, 2015; Sharp, 2017) and its projections to the mPFC have been implicated in anxiety-related behaviors (Liu et al., 2015; Liu W.-Z. et al., 2020; Felix-Ortiz et al., 2016). For instance, lesioning the BLA in stress naïve rats induced a reduction of spine density on the basal dendritic tree of pyramidal neurons without dendritic attrition in the mPFC (Liu et al., 2015). Furthermore, the optogenetic activation of this pathway in stress naïve male mice increased anxiety (Felix-Ortiz et al., 2016; Lowery-Gionta et al., 2018), and social avoidance (Felix-Ortiz et al., 2016) while the optogenetic inhibition of these pathways induced opposite behavioral effects (Felix-Ortiz et al., 2016). Moreover, a recent study highlighted the anxiogenic effect of the BLA-mPFC pathway in stress-naive males and females with acute chemogenetic stimulation, decreasing the time spent in the open arms during the elevated plus-maze test (Marcus et al., 2020). The anxiogenic effect of the BLA-mPFC pathway was exacerbated by the viral deletion of cannabinoid receptor CB1 in the mPFC-projecting BLA neurons, suggesting the role of endocannabinoid negative feedback in anxiety regulation in the BLA-mPFC circuit. This manipulation impairs the electrophysiological regulation of mPFC neurons receiving BLA inputs (Marcus et al., 2020).

The LC sends dense noradrenergic projections distributed across the mPFC superficial layers I and II/III (Nestler et al., 2008). The LC has been involved in arousal, attention, cognitive flexibility, decision making, and emotions (Beversdorf et al., 1999; Nestler et al., 2008; Benarroch, 2009) and more recently, its projections to the mPFC have been involved in the control of anxiety-like behaviors in mice (Hirschberg et al., 2017). Indeed, chemogenetic activation of the LC to mPFC neuronal pathway was shown to trigger anxiety-like behaviors in the open field test and aversion in the place preference test in naïve male rats (Hirschberg et al., 2017). Similarly, chemogenetic activation of this pathway was shown to improve set-shifting behaviors in conditioning chamber tests (Cope et al., 2019), highlighting the importance of this pathway in adaptive behaviors during learning and its relevance to stress-copying strategies.

Finally, the mediodorsal thalamus (MDT) integrates inputs from various brain regions such as the amygdala, VTA, and DRN and transmits this information to the mPFC (Aggleton and Mishkin, 1984; Groenewegen, 1988; García-Cabezas et al., 2009). The MDT has been shown to control the integration of emotional information from these limbic structures and is involved in learning, decision-making process (Mitchell, 2015), and behavioral flexibility (Floresco et al., 1999; Parnaudeau et al., 2015). MDT-mPFC connectivity has been shown to be impaired in treatment-resistant MDD patients (Li et al., 2013). Previous studies showed that the chemogenetic activation of the MDT to mPFC neuronal pathway decreases behavioral despair with reduced immobility in the tail suspension test and forced swim test in naive mice (Miller et al., 2017). On the contrary, optogenetic inhibition of MDT-mPFC neurons was shown to have no effect on depressive-like behaviors in the forced swim test and elevated plus maze in males (Carreno et al., 2016; Padilla-Coreano et al., 2016). Interestingly, the mPFC neurons receiving MDT inputs express GluN2B receptor subunit, accounting for approximately 35% of NMDAR-mediated currents (Miller et al., 2017). Viral deletion of GluN2B significantly enhanced MDT-mPFC but not vHIPP-mPFC EPSC amplitude in the mPFC layer III pyramidal neurons (Miller et al., 2017). GluN2B receptors are critical for ketamine’s antidepressant effect (Miller et al., 2014) supporting a mechanism of action for ketamine to engage preferentially MDT-mPFC inputs rather than the vHIPP-mPFC pathway.

 Alterations in mPFC Outputs

As detailed above, the mPFC projects to several brain regions involved in the control of emotions and reward processing (Gunaydin et al., 2014; Floresco, 2015; Wassum and Izquierdo, 2015). As for the contribution of its afferences, functional studies have also dissected the roles of specific neuronal pathways in the expression of stress susceptibility and resilience (Table 2).

Overview of preclinical studies involving mPFC efferences in anxiety-like and depressive-like behaviors.

Efferences Species Sex studied Stress Neuromodulatory approach Effects observed Tests performed References
Basomedial amygdala (BMA) Mouse Both Naive Optogenetic stimulation Anxiolytic OFT, EPM Adhikari et al., 2015
Mouse Both Naive Optogenetic inhibition Anxiogenic
Basolateral amygdala (BLA) Mouse Male Acute SDS Optogenetic stimulation Anxiolytic EPM Vialou et al., 2014
Mouse Male Chronic restraint stress Optogenetic stimulation Anxiolytic OFT, EPM Liu W.-Z. et al., 2020
Amygdala Mouse Male CSDS Chemogenetic activation Antidepressant Social interaction Hultman et al., 2016
Nucleus accumbens (NAc) Mouse Male CSDS Optogenetic stimulation Antidepressant Social interaction Bagot et al., 2015
Mouse Male Acute SDS Optogenetic stimulation Pro-depressive, anhedonia Social interaction, SPT Vialou et al., 2014
Mouse Both Naive Optogenetic stimulation Pro-depressive Linear 3-chamber assay Murugan et al., 2017
Mouse Both sCVS Chemogenetic activation Anxogenic, pro-depressive NSF, EPM, FST, Splash test Bittar et al., 2021
Mouse Both sCVS Chemogenetic inhibition Anxiolytic, antidepressant
Dorsal raphe nucleus (DRN) Mouse Male CSDS Optogenetic inhibition Pro-depressive Social interaction Challis et al., 2014
Mouse Male CSDS Optogenetic stimulation Antidepressant
Rat Female Inescapable tailshock Optogenetic inhibition Pro-depressive Social interaction Dolzani et al., 2018
Rat Male Naive Optogenetic stimulation Antidepressant FST Warden et al., 2012

Amongst the distinct neuronal circuits emerging from the mPFC, the corticoaccumbal pathway has received considerable interest regarding its involvement in the expression of stress susceptibility or resilience. For instance, the optogenetic acute stimulation of pyramidal mPFC neurons projecting to the NAc was shown to promote anxiety in the open field test in naïve males but did not change the immobility in the forced swim test or the interaction time in the social interaction test (Bagot et al., 2015). On the contrary, acute stimulation of the same neurons after CSDS did not trigger any change in anxiety and behavioral despair in the open field and the forced swim tests. However, it promoted resilience to social stress by increasing social interaction after CSDS in males (Bagot et al., 2015). Elevated activity in the NAc-projecting mPFC neurons was also reported during pro-hedonic reward-seeking in mice (Otis et al., 2017). On the contrary, stimulation of the same pathway after acute social defeat increased social avoidance and elicited anhedonia in males (Vialou et al., 2014). Consistently, continuous optogenetic stimulation of mPFC nerve terminals in the NAc reduced social interaction (Murugan et al., 2017). Interestingly, the acute chemogenetic activation of the corticoaccumbal pathway was shown to induce no behavioral impact in both stress naive males or females (Bittar et al., 2021). However, when combined with subthreshold CVS, the same stimulation paradigm was sufficient to induce anxiety and behavioral despair in both sexes (Bittar et al., 2021). Interestingly, inhibition of the same population after CVS was shown to rescue anxiety and despair phenotypes in females but not in males, suggesting that the corticoaccumbal pathway may be necessary to induce anxiety and despair in females but not in males (Bittar et al., 2021). Therefore, these contrasting results suggest that activity patterns of the cortico-accumbal pathway, which can be modulated differently by acute and chronic stress (Vialou et al., 2014; Bagot et al., 2015; Bittar et al., 2021), is particularly relevant in the determination of the proper behavioral response to stress, especially regarding anxious, hedonic, and social behaviors.

The contribution of the mPFC projections to the amygdala, and more specifically to its different nuclei, has also been extensively studied in the context of stress responses. Indeed, optogenetic stimulation of the vmPFC neurons projecting to the basomedial nucleus of the amygdala (BMA) was shown to decrease anxiety-like behaviors with increased time spent in the open arms of the elevated plus-maze in both male and female mice chronically exposed to corticosterone (Adhikari et al., 2015). On the contrary, the inhibition of this pathway decreased the time spent in open arms in both sexes (Adhikari et al., 2015). In comparison, optogenetic stimulation of the mPFC neurons projecting to the BLA decreased anxiety behaviors in the elevated plus-maze but had no effect on social avoidance and anhedonia after acute social defeat (Vialou et al., 2014) and chronic restraint stress (Liu W.-Z. et al., 2020) in male mice. Finally, chemogenetic activation of mPFC afferences to the amygdala during social interaction test reduced CSDS-induced social avoidance in susceptible male mice (Hultman et al., 2016).

Additionally, mPFC neurons projecting to the dorsal raphe nucleus (DRN) were shown to control specific aspects of social behaviors. Optogenetic inhibition of this pathway decreases social avoidance after CSDS in male mice (Challis et al., 2014). Another study using chemogenetic approaches showed that the inhibition of this pathway in female rats exposed to inescapable tail shocks increases exploration in the juvenile social exploration test (Dolzani et al., 2018). Similarly, the optogenetic stimulation of mPFC-DRN neurons in naïve male rats decreased helplessness and behavioral despair by increasing the kicking and decreasing immobility in the forced swim test (Warden et al., 2012). Interestingly, high-frequency deep brain stimulation of the mPFC ILC in naive male rats triggered a decreased firing rate in the DRN (Srejic et al., 2015). This decrease is due to the activation of GABAergic interneurons in the DRN, inhibiting the principal neurons. Altogether, these studies suggest that mPFC neurons projecting to the DRN target the GABA interneurons and trigger their activation, leading to a decrease in DRN principal neuron activity (Warden et al., 2012; Challis et al., 2014; Srejic et al., 2015).

In consequence, the activation of the mPFC neurons that project to the LC, vHIPP, BLA, and VTA elicits anxiety, while the inhibition of vHIPP-mPFC and BLA-mPFC have anxiolytic effects in rodents (Figure 3). Activation of the BLA-mPFC neurons also has a pro-depressive impact, as well as inhibiting the VTA-mPFC pathway (Figure 4). Globally, the functional changes reported here argue in favor of the increased activity in the mPFC associated with anxiety and depressive-like behaviors. These findings also inform us on the probable direction of the E/I imbalance after stress exposure, the balance shifting toward excitation in this case. While we have a better understanding of these pathways’ contributions in males, studies investigating their contributions in females are still lacking. Despite this limitation, the little evidence we have from studies comparing males and females suggests that specific pathways such as the corticoaccumbal pathway may contribute differently to the expression of emotional stress responses in both sexes.

Medial prefrontal circuitry involved in anxiety-like behaviors. (A) Schematic representation of the mPFC circuits involved in the expression of either (A) anxiogenic or (B) anxiolytic behavioral responses. mPFC, medial prefrontal cortex; NAc, nucleus accumbens; Th, thalamus; vHIPP, ventral hippocampus; VTA, ventral tegmental area.

Medial prefrontal circuitry involved in depressive-like behaviors. (A) Schematic representation of the mPFC circuits involved in the expression of either (A) depressive- or (B) antidepressant-like behavioral responses. mPFC, medial prefrontal cortex; NAc, nucleus accumbens; Th, thalamus; vHIPP, ventral hippocampus; VTA, ventral tegmental area. CSDS, chronic social defeat stress; EPM, elevated plus-maze test; FST, forced swim test; NSF, novelty-suppressed feeding test; OFT, open field test; sCVS, subthreshold chronic variable stress; SDS, social defeat stress; SPT, sucrose preference test.

 Conclusion and Future Perspectives

The sum of evidence described in this review strongly supports the role of the mPFC as a hub region in the integration and consolidation of emotional responses to chronic stress in males and females (Murrough et al., 2011; Soumier and Sibille, 2014; Ferenczi et al., 2016). This complex process appears to involve a series of morphological and anatomical alterations (Radley et al., 2004; Gilabert-Juan et al., 2013; Sarkar and Kabbaj, 2016; Bittar et al., 2021) combined with changes in the strength of mPFC inputs from several brain structures (Marcus et al., 2020; Bittar et al., 2021). Ultimately, these modifications induced by stress interfere with the E/I balance in the mPFC in a sex-specific fashion and finally with the top-down processing of sensory and emotional information. As of now, several studies investigated the contribution of neuronal pathways projecting to the mPFC (Gunaydin et al., 2014; Parfitt et al., 2017; Cope et al., 2019; Marcus et al., 2020) and, while others investigated the contribution of this structure in mediating stress responses (Challis et al., 2014; Vialou et al., 2014; Adhikari et al., 2015; Bittar et al., 2021), more work is required to dissect the contribution of distinct neuronal populations within the mPFC projecting to other brain structures. Indeed, with the development of more sophisticated functional and behavioral approaches, it is becoming increasingly clear that distinct neuronal pathways emerging from the mPFC control specific behavioral features within complex stress responses differently in males and females. Additionally, it will be important in future studies to consider the contribution of the different sub-structures of the PFC such as the ACC, the PLC and ILC, and the orbitofrontal cortex in the expression of complex stress responses in males and females.

Now, another crucial aspect to consider in future studies is the type of stress used to induce anxiety- and depressive-like behaviors in animals, which based on the literature reviewed above, appear to impose distinct changes on the activity of mPFC neurons and circuits. Indeed, stress paradigms involving mainly physical stressors are likely to impact the mPFC circuitry differently than those involving psychosocial stressors (Nestler and Hyman, 2010). Such distinctions have been shown to be of particular importance in recent studies of stress-induced transcriptional alterations in the brain from different mouse models of depressive-like behaviors (Labonté et al., 2017; Scarpa et al., 2020). Understanding how these different types of stress impact the activity of neuronal circuits in males and females to ultimately induce the expression of a complex stress response will be of the upmost importance to identify the cellular substrate to target with therapeutic interventions. Indeed, by combining molecular and pharmacological approaches with the strategies elaborated here, one will start to delineate the foundations for new therapeutic interventions that target the neuronal substrate responsible for precise behavioral manifestations rather than a complex and heterogenous stress phenotype.

 Author Contributions

TPB and BL contributed to the literature review and the redaction of the manuscript. Both authors contributed to the article and approved the submitted version.

 Conflict of Interest

The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Funding. This work was supported by a Brain & Behavior Research Foundation NARSAD Young Investigator Award (to BL), the Canadian Institutes of Health Research (Grant No. SVB397205 to BL), the Natural Science and Engineering Research Council of Canada (Grant No. RGPIN-2019-06496 to BL), and Fonds de Recherche en Santé du Québec (FRQS) Junior-1 salary support (to BL). BL holds a Sentinelle Nord Research Chair.

 References aan het Rot M. Mathew S. J. Charney D. S. (2009). Neurobiological mechanisms in major depressive disorder. CMAJ 180 305313. 10.1503/cmaj.080697 19188629 Adhikari A. Lerner T. N. Finkelstein J. Pak S. Jennings J. H. Davidson T. J. (2015). Basomedial amygdala mediates top-down control of anxiety and fear. Nature 527 179185. 10.1038/nature15698 26536109 Aggleton J. P. Mishkin M. (1984). Projections of the amygdala to the thalamus in the cynomolgus monkey. J. Comp. Neurol. 222 5668. 10.1002/cne.902220106 6321564 Aggleton J. P. Wright N. F. Rosene D. L. Saunders R. C. (2015). Complementary Patterns of Direct Amygdala and Hippocampal Projections to the Macaque Prefrontal Cortex. Cereb. Cortex 25 43514373. 10.1093/cercor/bhv019 25715284 American Psychiatric Association (2013). Diagnostic and Statistical Manual of Mental Disorders (DSM-5). Virginia: American Psychiatric Association. Arnsten A. F. Goldman-Rakic P. S. (1984). Selective prefrontal cortical projections to the region of the locus coeruleus and raphe nuclei in the rhesus monkey. Brain Res. 306 918. Athanasiadis C. Gough B. Robertson S. (2018). What do counsellors need to know about male depression? Br. J. Guidance Counsel. 46 596604. 10.1080/03069885.2017.1346232 Bagot R. C. Parise E. M. Peña C. J. Zhang H.-X. Maze I. Chaudhury D. (2015). Ventral hippocampal afferents to the nucleus accumbens regulate susceptibility to depression. Nat. Commun. 6:7062. 10.1038/ncomms8062 25952660 Banasr M. Lepack A. Fee C. Duric V. Maldonado-Aviles J. DiLeone R. (2017). Characterization of GABAergic marker expression in the chronic unpredictable stress model of depression. Chronic Stress 1:2470547017720459. Bandelow B. Michaelis S. (2015). Epidemiology of anxiety disorders in the 21st century. Dialogues Clin. Neurosci. 17 327335. Bannerman D. M. Rawlins J. N. P. McHugh S. B. Deacon R. M. J. Yee B. K. Bast T. (2004). Regional dissociations within the hippocampus—memory and anxiety. Neurosci. Biobehav. Rev. 28 273283. 10.1016/j.neubiorev.2004.03.004 15225971 Barbas H. Olmos J. (1990). Projections from the amygdala to basoventral and mediodorsal prefrontal regions in the rhesus monkey. J. Comparat. Neurol. 300 549571. 10.1002/cne.903000409 2273093 Bechara A. Tranel D. Damasio H. (2000). Characterization of the decision-making deficit of patients with ventromedial prefrontal cortex lesions. Brain 123 21892202. 10.1093/brain/123.11.2189 11050020 Benarroch E. E. (2009). The locus ceruleus norepinephrine system: Functional organization and potential clinical significance. Neurology 73 16991704. 10.1212/WNL.0b013e3181c2937c 19917994 Berndt A. Yizhar O. Gunaydin L. A. Hegemann P. Deisseroth K. (2009). Bi-stable neural state switches. Nat. Neurosci. 12 229234. 10.1038/nn.2247 19079251 Beversdorf D. Q. Hughes J. D. Steinberg B. A. Lewis L. D. Heilman K. M. (1999). Noradrenergic modulation of cognitive flexibility in problem solving. NeuroRep. 10 27632767. Bicks L. K. Koike H. Akbarian S. Morishita H. (2015). Prefrontal Cortex and Social Cognition in Mouse and Man. Front. Psychol. 6:1805. 10.3389/fpsyg.2015.01805 26635701 Biselli T. Lange S. S. Sablottny L. Steffen J. Walther A. (2019). Optogenetic and chemogenetic insights into the neurocircuitry of depression-like behaviour: A systematic review. Eur. J. Neurosci. 53 938. 10.1111/ejn.14603 31633833 Bittar T. P. Pelaez M. C. Silva J. C. H. Quessy F. Lavigne A.-A. Morency D. (2021). Chronic stress induces sex-specific functional and morphological alterations in cortico-accumbal and cortico-tegmental pathways. Biol. Psychiatry 2021:014. 10.1016/j.biopsych.2021.02.014 33867113 Breslau J. Gilman S. E. Stein B. D. Ruder T. Gmelin T. Miller E. (2017). Sex differences in recent first-onset depression in an epidemiological sample of adolescents. Transl. Psychiatry 7:e1139. 10.1038/tp.2017.105 28556831 Brown S. M. Henning S. Wellman C. L. (2005). Mild, short-term stress alters dendritic morphology in rat medial prefrontal cortex. Cereb. Cortex 15 17141722. 10.1093/cercor/bhi048 15703248 Burgin K. E. Waxham M. N. Rickling S. Westgate S. A. Mobley W. C. Kelly P. T. (1990). In situ hybridization histochemistry of Ca2+/calmodulin-dependent protein kinase in developing rat brain. J. Neurosci. 10 17881798. Caballero A. Flores-Barrera E. Cass D. K. Tseng K. Y. (2014). Differential regulation of parvalbumin and calretinin interneurons in the prefrontal cortex during adolescence. Brain Struct. Funct. 219 395406. 10.1007/s00429-013-0508-8 23400698 Carreno F. R. Donegan J. J. Boley A. M. Shah A. DeGuzman M. Frazer A. (2016). Activation of a ventral hippocampus–medial prefrontal cortex pathway is both necessary and sufficient for an antidepressant response to ketamine. Mol. Psychiatry 21 12981308. 10.1038/mp.2015.176 26619811 Cavanagh A. Wilson C. J. Kavanagh D. J. Caputi P. (2017). Differences in the Expression of Symptoms in Men Versus Women with Depression: A Systematic Review and Meta-analysis. Harvard Rev. Psychiatry 25 2938. 10.1097/HRP.0000000000000128 28059934 Challis C. Beck S. G. Berton O. (2014). Optogenetic modulation of descending prefrontocortical inputs to the dorsal raphe bidirectionally bias socioaffective choices after social defeat. Front. Behav. Neurosci. 8:43. 10.3389/fnbeh.2014.00043 24596546 Chaudhury D. Walsh J. J. Friedman A. K. Juarez B. Ku S. M. Koo J. W. (2013). Rapid regulation of depression-related behaviors by control of midbrain dopamine neurons. Nature 493 532536. 10.1038/nature11713 23235832 Christie M. J. Bridge S. James L. B. Beart P. M. (1985). Excitotoxin lesions suggest an aspartatergic projection from rat medial prefrontal cortex to ventral tegmental area. Brain Res. 333 169172. 10.1016/0006-8993(85)90140-4 Cook S. C. Wellman C. L. (2004). Chronic stress alters dendritic morphology in rat medial prefrontal cortex. J. Neurobiol. 60 236248. 10.1002/neu.20025 15266654 Cope Z. A. Vazey E. M. Floresco S. B. Aston Jones G. S. (2019). DREADD-mediated modulation of locus coeruleus inputs to mPFC improves strategy set-shifting. Neurobiol. Learning Memory 161 111. 10.1016/j.nlm.2019.02.009 30802603 Covington H. E. Lobo M. K. Maze I. Vialou V. Hyman J. M. Zaman S. (2010). Antidepressant Effect of Optogenetic Stimulation of the Medial Prefrontal Cortex. J. Neurosci. 30 1608216090. 10.1523/JNEUROSCI.1731-10.2010 21123555 Dalla C. Pitychoutis P. M. Kokras N. Papadopoulou-Daifoti Z. (2010). Sex differences in animal models of depression and antidepressant response. Basic Clin. Pharmacol. Toxicol. 106 226233. 10.1111/j.1742-7843.2009.00516.x 20050844 Dolzani S. D. Baratta M. V. Moss J. M. Leslie N. L. Tilden S. G. Sørensen A. T. (2018). Inhibition of a Descending Prefrontal Circuit Prevents Ketamine-Induced Stress Resilience in Females. eNeuro 5:2018. 10.1523/ENEURO.0025-18.2018 29516036 Douglas R. J. Martin K. A. C. (2004). Neuronal circuits of the neocortex. Annu. Rev. Neurosci. 27 419451. 10.1146/annurev.neuro.27.070203.144152 15217339 Drevets W. C. Price J. L. Furey M. L. (2008). Brain structural and functional abnormalities in mood disorders: implications for neurocircuitry models of depression. Brain Struct. Funct. 213 93118. 10.1007/s00429-008-0189-x 18704495 Duman C. H. Duman R. S. (2015). Spine synapse remodeling in the pathophysiology and treatment of depression. Neurosci. Lett. 601 2029. 10.1016/j.neulet.2015.01.022 25582786 Erondu N. E. Kennedy M. B. (1985). Regional distribution of type II Ca2+/calmodulin-dependent protein kinase in rat brain. J. Neurosci. 5 32703277. Euston D. R. Gruber A. J. McNaughton B. L. (2012). The role of medial prefrontal cortex in memory and decision making. Neuron 76 10571070. 10.1016/j.neuron.2012.12.002 23259943 Fava M. Kendler K. S. (2000). Major Depressive Disorder. Neuron 28 335341. 10.1016/S0896-6273(00)00112-4 Fee C. Banasr M. Sibille E. (2017). Somatostatin-Positive Gamma-Aminobutyric Acid Interneuron Deficits in Depression: Cortical Microcircuit and Therapeutic Perspectives. Biol. Psychiatry 82 549559. 10.1016/j.biopsych.2017.05.024 28697889 Felix-Ortiz A. C. Burgos-Robles A. Bhagat N. D. Leppla C. A. Tye K. M. (2016). Bidirectional modulation of anxiety-related and social behaviors by amygdala projections to the medial prefrontal cortex. Neuroscience 321 197209. 10.1016/j.neuroscience.2015.07.041 26204817 Ferenczi E. A. Zalocusky K. A. Liston C. Grosenick L. Warden M. R. Amatya D. (2016). Prefrontal cortical regulation of brainwide circuit dynamics and reward-related behavior. Science 351:aac9698. 10.1126/science.aac9698 26722001 Flint J. Kendler K. S. (2014). The Genetics of Major Depression. Neuron 81 484503. 10.1016/j.neuron.2014.01.027 24507187 Floresco S. B. (2015). The nucleus accumbens: an interface between cognition, emotion, and action. Annu. Rev. Psychol. 66 2552. 10.1146/annurev-psych-010213-115159 25251489 Floresco S. B. Braaksma D. N. Phillips A. G. (1999). Thalamic-cortical-striatal circuitry subserves working memory during delayed responding on a radial arm maze. J. Neurosci. 19 1106111071. Fried E. I. Nesse R. M. (2015). Depression is not a consistent syndrome: An investigation of unique symptom patterns in the STARD study. J. Affect. Disord. 172 96102. 10.1016/j.jad.2014.10.010 25451401 Friedman A. K. Walsh J. J. Juarez B. Ku S. M. Chaudhury D. Wang J. (2014). Enhancing Depression Mechanisms in Midbrain Dopamine Neurons Achieves Homeostatic Resilience. Science 344 313319. 10.1126/science.1249240 24744379 Fuchikami M. Thomas A. Liu R. Wohleb E. S. Land B. B. DiLeone R. J. (2015). Optogenetic stimulation of infralimbic PFC reproduces ketamine’s rapid and sustained antidepressant actions. Proc. Natl. Acad. Sci. U S A. 112 81068111. 10.1073/pnas.1414728112 26056286 Gabbott P. L. A. Warner T. A. Jays P. R. L. Salway P. Busby S. J. (2005). Prefrontal cortex in the rat: projections to subcortical autonomic, motor, and limbic centers. J. Comp. Neurol. 492 145177. 10.1002/cne.20738 16196030 Gabbott P. Warner T.-A. Brown J. Salway P. Gabbott T. Busby S. (2012). Amygdala afferents monosynaptically innervate corticospinal neurons in rat medial prefrontal cortex. J. Comparat. Neurol. 520 24402458. 10.1002/cne.23047 22247040 García-Cabezas M. A. Martínez-Sánchez P. Sánchez-González M. A. Garzón M. Cavada C. (2009). Dopamine innervation in the thalamus: monkey versus rat. Cereb. Cortex 19 424434. 10.1093/cercor/bhn093 18550594 Gilabert-Juan J. Castillo-Gomez E. Guirado R. Moltó M. D. Nacher J. (2013). Chronic stress alters inhibitory networks in the medial prefrontal cortex of adult mice. Brain Struct. Funct. 218 15911605. 10.1007/s00429-012-0479-1 23179864 Goldman-Rakic P. S. Selemon L. D. Schwartz M. L. (1984). Dual pathways connecting the dorsolateral prefrontal cortex with the hippocampal formation and parahippocampal cortex in the rhesus monkey. Neuroscience 12 719743. 10.1016/0306-4522(84)90166-0 Gonçalves L. Nogueira M. I. Shammah-Lagnado S. J. Metzger M. (2009). Prefrontal afferents to the dorsal raphe nucleus in the rat. Brain Res. Bull. 78 240247. 10.1016/j.brainresbull.2008.11.012 19103268 Grant B. F. Saha T. D. Ruan W. J. Goldstein R. B. Chou S. P. Jung J. (2016). Epidemiology of DSM-5 Drug Use Disorder: Results From the National Epidemiologic Survey on Alcohol and Related Conditions-III. JAMA Psychiatry 73 3947. 10.1001/jamapsychiatry.2015.2132 26580136 Gray A. L. Hyde T. M. Deep-Soboslay A. Kleinman J. E. Sodhi M. S. (2015). Sex differences in glutamate receptor gene expression in major depression and suicide. Mol. Psychiatry 20 10571068. 10.1038/mp.2015.91 26169973 Groenewegen H. J. (1988). Organization of the afferent connections of the mediodorsal thalamic nucleus in the rat, related to the mediodorsal-prefrontal topography. Neuroscience 24 379431. 10.1016/0306-4522(88)90339-9 Gunaydin L. A. Grosenick L. Finkelstein J. C. Kauvar I. V. Fenno L. E. Adhikari A. (2014). Natural neural projection dynamics underlying social behavior. Cell 157 15351551. 10.1016/j.cell.2014.05.017 24949967 Hadas I. Sun Y. Lioumis P. Zomorrodi R. Jones B. Voineskos D. (2019). Association of Repetitive Transcranial Magnetic Stimulation Treatment With Subgenual Cingulate Hyperactivity in Patients With Major Depressive Disorder: A Secondary Analysis of a Randomized Clinical Trial. JAMA Netw. Open 2:e195578. 10.1001/jamanetworkopen.2019.5578 31167023 Hains A. B. Vu M. A. T. Maciejewski P. K. van Dyck C. H. Gottron M. Arnsten A. F. T. (2009). Inhibition of protein kinase C signaling protects prefrontal cortex dendritic spines and cognition from the effects of chronic stress. Proc. Natl. Acad. Sci. U S A. 106 1795717962. 10.1073/pnas.0908563106 19805148 Heidbreder C. A. Groenewegen H. J. (2003). The medial prefrontal cortex in the rat: evidence for a dorso-ventral distinction based upon functional and anatomical characteristics. Neurosci. Biobehav. Rev. 27 555579. Hirschberg S. Li Y. Randall A. Kremer E. J. Pickering A. E. (2017). Functional dichotomy in spinal- vs prefrontal-projecting locus coeruleus modules splits descending noradrenergic analgesia from ascending aversion and anxiety in rats. eLife 6:e29808. 10.7554/eLife.29808 29027903 Holtzheimer P. E. Husain M. M. Lisanby S. H. Taylor S. F. Whitworth L. A. McClintock S. (2017). Subcallosal cingulate deep brain stimulation for treatment-resistant depression: a multisite, randomised, sham-controlled trial. Lancet Psychiatry 4 839849. 10.1016/S2215-0366(17)30371-1 Hoover W. B. Vertes R. P. (2007). Anatomical analysis of afferent projections to the medial prefrontal cortex in the rat. Brain Struct. Funct. 212 149179. 10.1007/s00429-007-0150-4 17717690 Hultman R. Mague S. D. Li Q. Katz B. M. Michel N. Lin L. (2016). Dysregulation of prefrontal cortex-mediated slow evolving limbic dynamics drives stress-induced emotional pathology. Neuron 91 439452. 10.1016/j.neuron.2016.05.038 27346529 Jones E. G. Huntley G. W. Benson D. L. (1994). Alpha calcium/calmodulin-dependent protein kinase II selectively expressed in a subpopulation of excitatory neurons in monkey sensory-motor cortex: comparison with GAD-67 expression. J. Neurosci. 14 611629. Kandilarova S. Stoyanov D. Sirakov N. Maes M. Specht K. (2019). Reduced grey matter volume in frontal and temporal areas in depression: contributions from voxel-based morphometry study. Acta Neuropsychiatrica 31 252257. 10.1017/neu.2019.20 31234950 Kang H. J. Voleti B. Hajszan T. Rajkowska G. Stockmeier C. A. Licznerski P. (2012). Decreased expression of synapse-related genes and loss of synapses in major depressive disorder. Nat. Med. 18 14131417. 10.1038/nm.2886 22885997 Karolewicz B. Maciag D. O’Dwyer G. Stockmeier C. A. Feyissa A. M. Rajkowska G. (2010). Reduced level of glutamic acid decarboxylase-67 kDa in the prefrontal cortex in major depression. Int. J. Neuropsychopharmacol. 13 411420. 10.1017/S1461145709990587 20236554 Karpyak V. M. Biernacka J. M. Geske J. R. Abulseoud O. A. Brunner M. D. Chauhan M. (2016). Gender-specific effects of comorbid depression and anxiety on the propensity to drink in negative emotional states. Addiction 111 13661375. 10.1111/add.13386 27009547 Keedwell P. A. Andrew C. Williams S. C. R. Brammer M. J. Phillips M. L. (2005). The neural correlates of anhedonia in major depressive disorder. Biol. Psychiatry 58 843853. 10.1016/j.biopsych.2005.05.019 16043128 Kendler K. S. Gatz M. Gardner C. O. Pedersen N. L. (2006). A Swedish national twin study of lifetime major depression. Am. J. Psychiatry 163 109114. 10.1176/appi.ajp.163.1.109 16390897 Kerney M. Smaers J. B. Schoenemann P. T. Dunn J. C. (2017). The coevolution of play and the cortico-cerebellar system in primates. Primates 58 485491. 10.1007/s10329-017-0615-x 28620843 Kessler R. C. Chiu W. T. Demler O. Merikangas K. R. Walters E. E. (2005). Prevalence, severity, and comorbidity of 12-month DSM-IV disorders in the National Comorbidity Survey Replication. Arch. Gen. Psychiatry 62 617627. 10.1001/archpsyc.62.6.617 15939839 Kessler R. C. McGonagle K. A. Swartz M. Blazer D. G. Nelson C. B. (1993). Sex and depression in the National Comorbidity Survey. I: Lifetime prevalence, chronicity and recurrence. J. Affect. Disord. 29 8596. Khan A. Brodhead A. E. Schwartz K. A. Kolts R. L. Brown W. A. (2005). Sex differences in antidepressant response in recent antidepressant clinical trials. J. Clin. Psychopharmacol. 25 318324. Kim C. K. Ye L. Jennings J. H. Pichamoorthy N. Tang D. D. Yoo A.-C. W. (2017). Molecular and Circuit-Dynamical Identification of Top-Down Neural Mechanisms for Restraint of Reward Seeking. Cell 170 1013.e1027.e. 10.1016/j.cell.2017.07.020 28823561 Kim J.-H. Cho M. J. Hong J. P. Bae J. N. Cho S.-J. Hahm B.-J. (2015). Gender Differences in Depressive Symptom Profile: Results from Nationwide General Population Surveys in Korea. J. Korean Med. Sci. 30 16591666. 10.3346/jkms.2015.30.11.1659 26539012 Knowland D. Lim B. K. (2018). Circuit-based frameworks of depressive behaviors: The role of reward circuitry and beyond. Pharmacol. Biochem. Behav. 174 4252. 10.1016/j.pbb.2017.12.010 29309799 Ko J. (2017). Neuroanatomical Substrates of Rodent Social Behavior: The Medial Prefrontal Cortex and Its Projection Patterns. Front. Neural Circuits 11:41. 10.3389/fncir.2017.00041 28659766 Kornstein S. G. Schatzberg A. F. Thase M. E. Yonkers K. A. McCullough J. P. Keitner G. I. (2000a). Gender differences in chronic major and double depression. J. Affect. Disord. 60 111. Kornstein S. G. Schatzberg A. F. Thase M. E. Yonkers K. A. McCullough J. P. Keitner G. I. (2000b). Gender differences in treatment response to sertraline versus imipramine in chronic depression. Am. J. Psychiatry 157 14451452. 10.1176/appi.ajp.157.9.1445 10964861 Kumar S. Black S. J. Hultman R. Szabo S. T. DeMaio K. D. Du J. (2013). Cortical control of affective networks. J. Neurosci. 33 11161129. 10.1523/JNEUROSCI.0092-12.2013 23325249 Labonté B. Engmann O. Purushothaman I. Menard C. Wang J. Tan C. (2017). Sex-specific transcriptional signatures in human depression. Nat. Med. 23 11021111. 10.1038/nm.4386 28825715 Lai C.-H. (2011). Major depressive disorder: gender differences in symptoms, life quality, and sexual function. J. Clin. Psychopharmacol. 31 3944. 10.1097/JCP.0b013e318205a670 21192141 Lammel S. Lim B. K. Malenka R. C. (2014). Reward and aversion in a heterogeneous midbrain dopamine system. Neuropharmacology 76(Pt B), 351359. 10.1016/j.neuropharm.2013.03.019 23578393 Larkum M. (2013). A cellular mechanism for cortical associations: an organizing principle for the cerebral cortex. Trends Neurosci. 36 141151. 10.1016/j.tins.2012.11.006 23273272 Laubach M. Amarante L. M. Swanson K. White S. R. (2018). What, If Anything, Is Rodent Prefrontal Cortex? eNeuro 5:2018. 10.1523/ENEURO.0315-18.2018 30406193 Laubach M. Caetano M. S. Narayanan N. S. (2015). Mistakes were made: Neural mechanisms for the adaptive control of action initiation by the medial prefrontal cortex. J. Physiol. Paris 109 104117. 10.1016/j.jphysparis.2014.12.001 25636373 Lee A. T. Vogt D. Rubenstein J. L. Sohal V. S. (2014). A Class of GABAergic Neurons in the Prefrontal Cortex Sends Long-Range Projections to the Nucleus Accumbens and Elicits Acute Avoidance Behavior. J. Neurosci. 34 1151911525. 10.1523/JNEUROSCI.1157-14.2014 25164650 Li C.-T. Chen L.-F. Tu P.-C. Wang S.-J. Chen M.-H. Su T.-P. (2013). Impaired prefronto-thalamic functional connectivity as a key feature of treatment-resistant depression: a combined MEG, PET and rTMS study. PLoS One 8:e70089. 10.1371/journal.pone.0070089 23936378 Lin L. C. Sibille E. (2015). Somatostatin, neuronal vulnerability and behavioral emotionality. Mol. Psychiatry 20 377387. 10.1038/mp.2014.184 25600109 Linley S. B. Hoover W. B. Vertes R. P. (2013). Pattern of distribution of serotonergic fibers to the orbitomedial and insular cortex in the rat. J. Chem. Neuroanat. 48–49 2945. 10.1016/j.jchemneu.2012.12.006 23337940 Liu D. Tang Q.-Q. Wang D. Song S.-P. Yang X.-N. Hu S.-W. (2020). Mesocortical BDNF signaling mediates antidepressive-like effects of lithium. Neuropsychopharmacology 45 15571566. 10.1038/s41386-020-0713-0 32428928 Liu R.-J. Ota K. T. Dutheil S. Duman R. S. Aghajanian G. K. (2015). Ketamine Strengthens CRF-Activated Amygdala Inputs to Basal Dendrites in mPFC Layer V Pyramidal Cells in the Prelimbic but not Infralimbic Subregion, A Key Suppressor of Stress Responses. Neuropsychopharmacology 40 20662075. 10.1038/npp.2015.70 25759300 Liu W.-Z. Zhang W.-H. Zheng Z.-H. Zou J.-X. Liu X.-X. Huang S.-H. (2020). Identification of a prefrontal cortex-to-amygdala pathway for chronic stress-induced anxiety. Nat. Commun. 11:2221. 10.1038/s41467-020-15920-7 32376858 Liu X. Carter A. G. (2018). Ventral Hippocampal Inputs Preferentially Drive Corticocortical Neurons in the Infralimbic Prefrontal Cortex. J. Neurosci. 38 73517363. 10.1523/JNEUROSCI.0378-18.2018 29959235 Lowery-Gionta E. G. Crowley N. A. Bukalo O. Silverstein S. Holmes A. Kash T. L. (2018). Chronic stress dysregulates amygdalar output to the prefrontal cortex. Neuropharmacology 139 6875. 10.1016/j.neuropharm.2018.06.032 29959957 Lozano A. M. Giacobbe P. Hamani C. Rizvi S. J. Kennedy S. H. Kolivakis T. T. (2011). A multicenter pilot study of subcallosal cingulate area deep brain stimulation for treatment-resistant depression. J. Neurosurg. 116 315322. 10.3171/2011.10.JNS102122 22098195 Marcus D. J. Bedse G. Gaulden A. D. Ryan J. D. Kondev V. Winters N. D. (2020). Endocannabinoid Signaling Collapse Mediates Stress-Induced Amygdalo-Cortical Strengthening. Neuron 105 1062.e1076.e. 10.1016/j.neuron.2019.12.024 31948734 Marín O. Müller U. (2014). Lineage origins of GABAergic versus glutamatergic neurons in the neocortex. Curr. Opin. Neurobiol. 26 132141. 10.1016/j.conb.2014.01.015 24549207 Markram H. Toledo-Rodriguez M. Wang Y. Gupta A. Silberberg G. Wu C. (2004). Interneurons of the neocortical inhibitory system. Nat. Rev. Neurosci. 5 793807. 10.1038/nrn1519 15378039 Maroun M. (2013). Medial prefrontal cortex: multiple roles in fear and extinction. Neuroscientist 19 370383. 10.1177/1073858412464527 23090707 McGarry L. M. Carter A. G. (2016). Inhibitory Gating of Basolateral Amygdala Inputs to the Prefrontal Cortex. J. Neurosci. 36 93919406. 10.1523/JNEUROSCI.0874-16.2016 27605614 Menon V. Uddin L. Q. (2010). Saliency, switching, attention and control: a network model of insula function. Brain Struct. Funct. 214 655667. 10.1007/s00429-010-0262-0 20512370 Meyer G. Schaaps J. P. Moreau L. Goffinet A. M. (2000). Embryonic and early fetal development of the human neocortex. J. Neurosci. 20 18581868. Miller O. H. Bruns A. Ben Ammar I. Mueggler T. Hall B. J. (2017). Synaptic Regulation of a Thalamocortical Circuit Controls Depression-Related Behavior. Cell Rep. 20 18671880. 10.1016/j.celrep.2017.08.002 28834750 Miller O. H. Yang L. Wang C.-C. Hargroder E. A. Zhang Y. Delpire E. (2014). GluN2B-containing NMDA receptors regulate depression-like behavior and are critical for the rapid antidepressant actions of ketamine. Elife 3:e03581. 10.7554/eLife.03581 25340958 Mitchell A. S. (2015). The mediodorsal thalamus as a higher order thalamic relay nucleus important for learning and decision-making. Neurosci. Biobehav. Rev. 54 7688. 10.1016/j.neubiorev.2015.03.001 25757689 Moorman D. E. James M. H. McGlinchey E. M. Aston-Jones G. (2015). Differential roles of medial prefrontal subregions in the regulation of drug seeking. Brain Res. 1628 130146. 10.1016/j.brainres.2014.12.024 25529632 Morris L. S. Costi S. Tan A. Stern E. R. Charney D. S. Murrough J. W. (2020). Ketamine normalizes subgenual cingulate cortex hyper-activity in depression. Neuropsychopharmacology 45 975981. 10.1038/s41386-019-0591-5 31896116 Murayama M. Pérez-Garci E. Nevian T. Bock T. Senn W. Larkum M. E. (2009). Dendritic encoding of sensory stimuli controlled by deep cortical interneurons. Nature 457 11371141. 10.1038/nature07663 19151696 Murrough J. W. Iacoviello B. Neumeister A. Charney D. S. Iosifescu D. V. (2011). Cognitive dysfunction in depression: neurocircuitry and new therapeutic strategies. Neurobiol. Learn. Mem. 96 553563. 10.1016/j.nlm.2011.06.006 21704176 Murugan M. Jang H. J. Park M. Miller E. M. Cox J. Taliaferro J. P. (2017). Combined Social and Spatial Coding in a Descending Projection from the Prefrontal Cortex. Cell 171 1663.e1677.e. 10.1016/j.cell.2017.11.002 29224779 Narayanan N. S. Laubach M. (2017). Inhibitory Control: Mapping Medial Frontal Cortex. Curr. Biol. 27 R148R150. 10.1016/j.cub.2017.01.010 28222293 Nazroo J. Y. Edwards A. C. Brown G. W. (1997). Gender differences in the onset of depression following a shared life event: a study of couples. Psychol. Med. 27 919. Nestler E. Hyman S. Malenka R. (2008). “Chapter 6: Widely Projecting Systems: Monoamines, Acetylcholine, and Orexin,” in Molecular Neuropharmacology: A Foundation for Clinical Neuroscience, 2nd Edn, ed. Malenka R. (New York: McGraw-Hill Professional), 516. Nestler E. J. (1998). Antidepressant treatments in the 21st century. Biol. Psychiatry 44 526533. Nestler E. J. Hyman S. E. (2010). Animal models of neuropsychiatric disorders. Nat. Neurosci. 13 11611169. 10.1038/nn.2647 20877280 Nieuwenhuys R. (1994). The neocortex. An overview of its evolutionary development, structural organization and synaptology. Anat. Embryol. 190 307337. 10.1007/BF00187291 7840420 Noonan M. P. Mars R. B. Sallet J. Dunbar R. I. M. Fellows L. K. (2018). The structural and functional brain networks that support human social networks. Behav. Brain Res. 355 1223. 10.1016/j.bbr.2018.02.019 29471028 Otis J. M. Namboodiri V. M. K. Matan A. M. Voets E. S. Mohorn E. P. Kosyk O. (2017). Prefrontal cortex output circuits guide reward seeking through divergent cue encoding. Nature 543 103107. 10.1038/nature21376 28225752 Padilla-Coreano N. Bolkan S. S. Pierce G. M. Blackman D. R. Hardin W. D. Garcia-Garcia A. L. (2016). Direct ventral hippocampal-prefrontal input is required for anxiety-related neural activity and behavior. Neuron 89 857866. 10.1016/j.neuron.2016.01.011 26853301 Palomero-Gallagher N. Hoffstaedter F. Mohlberg H. Eickhoff S. B. Amunts K. Zilles K. (2019). Human Pregenual Anterior Cingulate Cortex: Structural, Functional, and Connectional Heterogeneity. Cereb. Cortex 29 25522574. 10.1093/cercor/bhy124 29850806 Parfitt G. M. Nguyen R. Bang J. Y. Aqrabawi A. J. Tran M. M. Seo D. K. (2017). Bidirectional Control of Anxiety-Related Behaviors in Mice: Role of Inputs Arising from the Ventral Hippocampus to the Lateral Septum and Medial Prefrontal Cortex. Neuropsychopharmacology 42 17151728. 10.1038/npp.2017.56 28294135 Parker G. Fletcher K. Paterson A. Anderson J. Hong M. (2014). Gender differences in depression severity and symptoms across depressive sub-types. J. Affect. Disord. 167 351357. 10.1016/j.jad.2014.06.018 25020270 Parnaudeau S. Taylor K. Bolkan S. S. Ward R. D. Balsam P. D. Kellendonk C. (2015). Mediodorsal thalamus hypofunction impairs flexible goal-directed behavior. Biol. Psychiatry 77 445453. 10.1016/j.biopsych.2014.03.020 24813335 Perova Z. Delevich K. Li B. (2015). Depression of Excitatory Synapses onto Parvalbumin Interneurons in the Medial Prefrontal Cortex in Susceptibility to Stress. J. Neurosci. 35 32013206. 10.1523/JNEUROSCI.2670-14.2015 25698754 Petilla Interneuron Nomenclature Group (2008). Petilla terminology: nomenclature of features of GABAergic interneurons of the cerebral cortex. Nat. Rev. Neurosci. 9 557568. 10.1038/nrn2402 18568015 Phillips M. L. Chase H. W. Sheline Y. I. Etkin A. Almeida J. R. C. Deckersbach T. (2015). Identifying predictors, moderators, and mediators of antidepressant response in major depressive disorder: neuroimaging approaches. Am. J. Psychiatry 172 124138. 10.1176/appi.ajp.2014.14010076 25640931 Phillips M. L. Robinson H. A. Pozzo-Miller L. (2019). Ventral hippocampal projections to the medial prefrontal cortex regulate social memory. eLife 8:e44182. 10.7554/eLife.44182 31112129 Porrino L. J. Goldman-Rakic P. S. (1982). Brainstem innervation of prefrontal and anterior cingulate cortex in the rhesus monkey revealed by retrograde transport of HRP. J. Comp. Neurol. 205 6376. 10.1002/cne.902050107 6121826 Price J. L. Drevets W. C. (2012). Neural circuits underlying the pathophysiology of mood disorders. Trends Cognit. Sci. 16 6171. 10.1016/j.tics.2011.12.011 22197477 Qu Y. Yang C. Ren Q. Ma M. Dong C. Hashimoto K. (2018). Regional differences in dendritic spine density confer resilience to chronic social defeat stress. Acta Neuropsychiatr. 30 117122. 10.1017/neu.2017.16 28566105 Quessy F. Bittar T. Blanchette L. J. Lévesque M. Labonté B. (2021). Stress-induced alterations of mesocortical and mesolimbic dopaminergic pathways. Sci. Rep. 11:11000. 10.1038/s41598-021-90521-y 34040100 Radley J. J. Rocher A. B. Rodriguez A. Ehlenberger D. B. Dammann M. McEwen B. S. (2008). Repeated stress alters dendritic spine morphology in the rat medial prefrontal cortex. J. Comp. Neurol. 507 11411150. 10.1002/cne.21588 18157834 Radley J. J. Sisti H. M. Hao J. Rocher A. B. McCall T. Hof P. R. (2004). Chronic behavioral stress induces apical dendritic reorganization in pyramidal neurons of the medial prefrontal cortex. Neuroscience 125 16. 10.1016/j.neuroscience.2004.01.006 15051139 Rajkowska G. Miguel-Hidalgo J. J. Wei J. Dilley G. Pittman S. D. Meltzer H. Y. (1999). Morphometric evidence for neuronal and glial prefrontal cell pathology in major depression. Biol. Psychiatry 45 10851098. 10.1016/s0006-3223(99)00041-4 Rice S. M. Fallon B. J. Aucote H. M. Möller-Leimkühler A. M. (2013). Development and preliminary validation of the male depression risk scale: furthering the assessment of depression in men. J. Affect. Disord. 151 950958. 10.1016/j.jad.2013.08.013 24051100 Ridderinkhof K. R. van den Wildenberg W. P. M. Segalowitz S. J. Carter C. S. (2004). Neurocognitive mechanisms of cognitive control: The role of prefrontal cortex in action selection, response inhibition, performance monitoring, and reward-based learning. Brain Cognit. 56 129140. 10.1016/j.bandc.2004.09.016 15518930 Riga D. Matos M. R. Glas A. Smit A. B. Spijker S. Oever V. (2014). Optogenetic dissection of medial prefrontal cortex circuitry. Front. Syst. Neurosci. 8:00230. 10.3389/fnsys.2014.00230 25538574 Rudy B. Fishell G. Lee S. Hjerling-Leffler J. (2011). Three Groups of Interneurons Account for Nearly 100% of Neocortical GABAergic Neurons. Dev. Neurobiol. 71 4561. 10.1002/dneu.20853 21154909 Runnels P. New A. S. Charney D. S. (2009). “Posttraumatic Stress Disorder: Neurobiology,” in Encyclopedia of Neuroscience, ed. Squire L. R. (Oxford: Academic Press), 847852. 10.1016/B978-008045046-9.00523-4 Sarkar A. Kabbaj M. (2016). Sex Differences in Effects of Ketamine on Behavior, Spine Density, and Synaptic Proteins in Socially Isolated Rats. Biol. Psychiatry 80 448456. 10.1016/j.biopsych.2015.12.025 26957131 Scarpa J. R. Fatma M. Loh Y.-H. E. Traore S. R. Stefan T. Chen T. H. (2020). Shared Transcriptional Signatures in Major Depressive Disorder and Mouse Chronic Stress Models. Biol. Psychiatry 88 159168. 10.1016/j.biopsych.2019.12.029 32169281 Seney M. L. Huo Z. Cahill K. French L. Puralewski R. Zhang J. (2018). Opposite Molecular Signatures of Depression in Men and Women. Biol. Psychiatry 84 1827. 10.1016/j.biopsych.2018.01.017 29548746 Seney M. L. Tripp A. McCune S. A. Lewis D. Sibille E. (2015). Laminar and cellular analyses of reduced somatostatin gene expression in the subgenual anterior cingulate cortex in major depression. Neurobiol. Dis. 73 213219. 10.1016/j.nbd.2014.10.005 25315685 Shah A. J. Ghasemzadeh N. Zaragoza-Macias E. Patel R. Eapen D. J. Neeland I. J. (2014). Sex and age differences in the association of depression with obstructive coronary artery disease and adverse cardiovascular events. J. Am. Heart Assoc. 3:e000741. 10.1161/JAHA.113.000741 24943475 Shansky R. M. Hamo C. Hof P. R. McEwen B. S. Morrison J. H. (2009). Stress-induced dendritic remodeling in the prefrontal cortex is circuit specific. Cereb. Cortex 19 24792484. 10.1093/cercor/bhp003 19193712 Sharp B. M. (2017). Basolateral amygdala and stress-induced hyperexcitability affect motivated behaviors and addiction. Translat. Psychiatry 7 e1194e1194. 10.1038/tp.2017.161 28786979 Shepard R. Page C. E. Coutellier L. (2016). Sensitivity of the prefrontal GABAergic system to chronic stress in male and female mice: Relevance for sex differences in stress-related disorders. Neuroscience 332 112. 10.1016/j.neuroscience.2016.06.038 27365172 Sigurdsson T. Duvarci S. (2016). Hippocampal-Prefrontal Interactions in Cognition, Behavior and Psychiatric Disease. Front. Syst. Neurosci. 9:00190. 10.3389/fnsys.2015.00190 26858612 Soumier A. Sibille E. (2014). Opposing effects of acute versus chronic blockade of frontal cortex somatostatin-positive inhibitory neurons on behavioral emotionality in mice. Neuropsychopharmacology 39 22522262. 10.1038/npp.2014.76 24690741 Sramek J. J. Murphy M. F. Cutler N. R. (2016). Sex differences in the psychopharmacological treatment of depression. Dialog. Clin. Neurosci. 18 447457. Srejic L. R. Hamani C. Hutchison W. D. (2015). High-frequency stimulation of the medial prefrontal cortex decreases cellular firing in the dorsal raphe. Eur. J. Neurosci. 41 12191226. 10.1111/ejn.12856 25712703 Swedish Council on Health Technology Assessment (2004). Treatment of Depression: A Systematic Review. Stockholm: Swedish Council on Health Technology Assessment. Takagishi M. Chiba T. (1991). Efferent projections of the infralimbic (area 25) region of the medial prefrontal cortex in the rat: an anterograde tracer PHA-L study. Brain Res. 566 2639. Thase M. E. Entsuah R. Cantillon M. Kornstein S. G. (2005). Relative antidepressant efficacy of venlafaxine and SSRIs: sex-age interactions. J. Womens Health 14 609616. 10.1089/jwh.2005.14.609 16181017 Tripp A. Kota R. S. Lewis D. A. Sibille E. (2011). Reduced somatostatin in subgenual anterior cingulate cortex in major depression. Neurobiol. Dis. 42 116124. 10.1016/j.nbd.2011.01.014 21232602 Uylings H. B. M. Groenewegen H. J. Kolb B. (2003). Do rats have a prefrontal cortex? Behav. Brain Res. 146 317. Van Bockstaele E. J. Biswas A. Pickel V. M. (1993). Topography of serotonin neurons in the dorsal raphe nucleus that send axon collaterals to the rat prefrontal cortex and nucleus accumbens. Brain Res. 624 188198. Vander Weele C. M. Siciliano C. A. Matthews G. A. Namburi P. Izadmehr E. M. Espinel I. C. (2018). Dopamine enhances signal-to-noise ratio in cortical-brainstem encoding of aversive stimuli. Nature 563 397401. 10.1038/s41586-018-0682-1 30405240 Vialou V. Bagot R. C. Cahill M. E. Ferguson D. Robison A. J. Dietz D. M. (2014). Prefrontal cortical circuit for depression- and anxiety-related behaviors mediated by cholecystokinin: role of ΔFosB. J. Neurosci. 34 38783887. 10.1523/JNEUROSCI.1787-13.2014 24623766 Wang X. Zhang C. Szábo G. Sun Q.-Q. (2013). Distribution of CaMKIIα expression in the brain in vivo, studied by CaMKIIα-GFP mice. Brain Res. 1518 925. 10.1016/j.brainres.2013.04.042 23632380 Warden M. R. Selimbeyoglu A. Mirzabekov J. J. Lo M. Thompson K. R. Kim S.-Y. (2012). A prefrontal cortex–brainstem neuronal projection that controls response to behavioural challenge. Nature 492 428432. 10.1038/nature11617 23160494 Wassum K. M. Izquierdo A. (2015). The basolateral amygdala in reward learning and addiction. Neurosci. Biobehavi. Rev. 57 271283. 10.1016/j.neubiorev.2015.08.017 26341938 Weissman M. M. Bland R. C. Canino G. J. Faravelli C. Greenwald S. Hwu H. G. (1996). Cross-national epidemiology of major depression and bipolar disorder. JAMA 276 293299. Weissman M. M. Bland R. Joyce P. R. Newman S. Wells J. E. Wittchen H. U. (1993). Sex differences in rates of depression: cross-national perspectives. J. Affect. Disord. 29 7784. Wellman C. L. Moench K. M. (2019). Preclinical studies of stress, extinction, and prefrontal cortex: intriguing leads and pressing questions. Psychopharmacology 236 5972. 10.1007/s00213-018-5023-4 30225660 Williams L. M. (2016). Precision psychiatry: a neural circuit taxonomy for depression and anxiety. Lancet Psychiatry 3 472480. 10.1016/S2215-0366(15)00579-9 Wonders C. P. Anderson S. A. (2006). The origin and specification of cortical interneurons. Nat. Rev. Neurosci. 7 687696. 10.1038/nrn1954 16883309 World Health Organization (2018). Depression. Geneva: World Health Organization. Yao H. K. Guet-McCreight A. Mazza F. Chameh H. M. Prevot T. D. Griffiths J. (2021). Reduced inhibition in depression impairs stimulus processing in human cortical microcircuits. bioRxiv 431698. [preprint]. 10.1101/2021.02.17.431698 Yizhar O. Fenno L. E. Prigge M. Schneider F. Davidson T. J. O’Shea D. J. (2011). Neocortical excitation/inhibition balance in information processing and social dysfunction. Nature 477 171178. 10.1038/nature10360 21796121 Young E. A. Kornstein S. G. Marcus S. M. Harvey A. T. Warden D. Wisniewski S. R. (2009). Sex differences in response to citalopram: a STARD report. J. Psychiatr Res. 43 503511. 10.1016/j.jpsychires.2008.07.002 18752809 Zhang Z.-W. Burke M. W. Calakos N. Beaulieu J.-M. Vaucher E. (2010). Confocal analysis of cholinergic and dopaminergic inputs onto pyramidal cells in the prefrontal cortex of rodents. Front. Neuroanat. 4:00021. 10.3389/fnana.2010.00021 20589096 Zhao Y.-J. Du M.-Y. Huang X.-Q. Lui S. Chen Z.-Q. Liu J. (2014). Brain grey matter abnormalities in medication-free patients with major depressive disorder: a meta-analysis. Psychol. Med. 44 29272937. 10.1017/S0033291714000518 25065859 Zhu Y. Li H. Zhou L. Wu J. Y. Rao Y. (1999). Cellular and molecular guidance of GABAergic neuronal migration from an extracortical origin to the neocortex. Neuron 23 473485.