1 6125 97 THE EPIGENETIC MECHANISMS OF AMPHETAMINE. AMPHETAMINE (AMPH) IS A PSYCHOSTIMULANT AND THE MOST PRESCRIBED DRUG TO TREAT ATTENTION DEFICIT HYPERACTIVE DISORDER (ADHD). ALTHOUGH THERAPEUTICALLY USED DOSES ARE GENERALLY WELL TOLERATED, NUMEROUS SIDE EFFECTS ARE STILL KNOWN TO OCCUR, SUCH AS JITTERINESS, LOSS OF APPETITE AND PSYCHOSIS. MOREOVER, AMPH IS LIABLE TO BE ABUSED BY USERS LOOKING FOR INCREASED ALERTNESS, WEIGHT LOSS OR ATHLETIC PERFORMANCE. A GROWING BODY OF EVIDENCE INDICATES THAT DRUGS OF ABUSE, INCLUDING AMPH, CONTROL GENE EXPRESSION THROUGH CHROMATIN MODIFICATIONS. HOWEVER, WHILE NUMEROUS STUDIES HAVE INVESTIGATED THE MOLECULAR MECHANISMS OF AMPH ACTION, ONLY A SMALL NUMBER OF STUDIES HAVE EXPLORED CHANGES IN GENE EXPRESSION CAUSED BY AMPH. THIS REVIEW EXAMINES THE EPIGENETIC CHANGES INDUCED BY CHRONIC AND ACUTE TREATMENTS WITH AMPH AND INCLUDES, WHERE RELEVANT, DATA OBTAINED WITH OTHER PSYCHOSTIMULANTS SUCH AS METHAMPHETAMINE AND COCAINE. 2015 2 5819 23 STRESS CHANGES AMPHETAMINE RESPONSE, D2 RECEPTOR EXPRESSION AND EPIGENETIC REGULATION IN LOW-ANXIETY RATS. THE AIM OF THIS STUDY WAS TO ASSESS THE INFLUENCE OF CHRONIC RESTRAINT STRESS ON AMPHETAMINE (AMPH)-RELATED APPETITIVE 50-KHZ ULTRASONIC VOCALISATIONS (USVS) IN RATS DIFFERING IN FREEZING DURATION IN A CONTEXTUAL FEAR TEST (CFT), I.E. HR (HIGH-ANXIETY RESPONSIVE) AND LR (LOW-ANXIETY RESPONSIVE) RATS. THE LR AND THE HR RATS, PREVIOUSLY EXPOSED TO AN AMPH BINGE EXPERIENCE, DIFFERED IN SENSITIVITY TO AMPH'S REWARDING EFFECTS, MEASURED AS APPETITIVE VOCALISATIONS. MOREOVER, CHRONIC RESTRAINT STRESS ATTENUATED AMPH-RELATED APPETITIVE VOCALISATIONS IN THE LR RATS BUT HAD NO INFLUENCE ON THE HR RATS' BEHAVIOUR. TO SPECIFY, THE RESTRAINT LR RATS VOCALISED APPETITIVELY LESS IN THE AMPH-ASSOCIATED CONTEXT AND AFTER AN AMPH CHALLENGE THAN THE CONTROL LR RATS. THIS PHENOMENON WAS ASSOCIATED WITH A DECREASE IN THE MRNA LEVEL FOR D2 DOPAMINE RECEPTOR IN THE AMYGDALA AND ITS PROTEIN EXPRESSION IN THE BASAL AMYGDALA (BA) AND OPPOSITE CHANGES IN THE NUCLEUS ACCUMBENS (NAC) - AN INCREASE IN THE MRNA LEVEL FOR D2 DOPAMINE RECEPTOR AND ITS PROTEIN EXPRESSION IN THE NAC SHELL, COMPARED TO CONTROL CONDITIONS. MOREOVER, WE OBSERVED THAT CHRONIC RESTRAINT STRESS INFLUENCED EPIGENETIC REGULATION IN THE LR AND THE HR RATS DIFFERENTLY. THE CONTRASTING CHANGES WERE OBSERVED IN THE DENTATE GYRUS (DG) OF THE HIPPOCAMPUS - THE LR RATS PRESENTED A DECREASE, BUT THE HR RATS SHOWED AN INCREASE IN H3K9 TRIMETHYLATION. THE RESTRAINT LR RATS ALSO SHOWED HIGHER MIR-494 AND MIR-34C LEVELS IN THE NAC THAN THE CONTROL LR GROUP. OUR STUDY PROVIDES BEHAVIOURAL AND BIOCHEMICAL DATA CONCERNING THE ROLE OF DIFFERENCES IN FEAR-CONDITIONED RESPONSE IN STRESS VULNERABILITY AND AMPH-ASSOCIATED APPETITIVE BEHAVIOUR. THE LR RATS WERE LESS SENSITIVE TO THE REWARDING EFFECTS OF AMPH WHEN PREVIOUSLY EXPOSED TO CHRONIC STRESS THAT WAS ACCOMPANIED BY CHANGES IN D2 DOPAMINE RECEPTOR EXPRESSION AND EPIGENETIC REGULATION IN MESOLIMBIC AREAS. 2019 3 3970 30 LONG-LASTING EPIGENETIC CHANGES IN THE DOPAMINE TRANSPORTER IN ADULT ANIMALS EXPOSED TO AMPHETAMINE DURING EMBRYOGENESIS: INVESTIGATING BEHAVIORAL EFFECTS. THE DOPAMINE TRANSPORTER (DAT) IS AN INTEGRAL MEMBER OF THE DOPAMINERGIC SYSTEM AND IS RESPONSIBLE FOR THE RELEASE AND REUPTAKE OF DOPAMINE FROM THE SYNAPTIC SPACE INTO THE DOPAMINERGIC NEURONS. DAT IS ALSO THE MAJOR TARGET OF AMPHETAMINE (AMPH). THE EFFECTS OF AMPH ON DAT HAVE BEEN INTENSIVELY STUDIED; HOWEVER, THE MECHANISMS UNDERLYING THE LONG-TERM EFFECTS CAUSED BY EMBRYONAL EXPOSURE TO ADDICTIVE DOSES OF AMPH REMAIN LARGELY UNEXPLORED. AS IN MAMMALS, IN THE NEMATODE C. ELEGANS AMPH CAUSES CHANGES IN LOCOMOTION WHICH ARE LARGELY MEDIATED BY THE C. ELEGANS DAT HOMOLOGUE, DAT-1. HERE, WE SHOW THAT CHRONIC EMBRYONIC EXPOSURES TO AMPH ALTER THE EXPRESSION OF DAT-1 IN ADULT C. ELEGANS VIA LONG-LASTING EPIGENETIC MODIFICATIONS. THESE CHANGES ARE CORRELATED WITH AN ENHANCED BEHAVIORAL RESPONSE TO AMPH IN ADULT ANIMALS. IMPORTANTLY, PHARMACOLOGICAL AND GENETIC INTERVENTION DIRECTED AT PREVENTING THE AMPH-INDUCED EPIGENETIC MODIFICATIONS OCCURRING DURING EMBRYOGENESIS INHIBITED THE LONG-LASTING BEHAVIORAL EFFECTS OBSERVED IN ADULT ANIMALS. BECAUSE MANY COMPONENTS OF THE DOPAMINERGIC SYSTEM, AS WELL AS EPIGENETIC MECHANISMS, ARE HIGHLY CONSERVED BETWEEN C. ELEGANS AND MAMMALS, THESE RESULTS COULD BE CRITICAL FOR OUR UNDERSTANDING OF HOW DRUGS OF ABUSE INITIATE PREDISPOSITION TO ADDICTION. 2023 4 1327 29 DEPRESSION AND ANTIDEPRESSANTS: INSIGHTS FROM KNOCKOUT OF DOPAMINE, SEROTONIN OR NORADRENALINE RE-UPTAKE TRANSPORTERS. MAJOR DEPRESSIVE DISORDER (MDD) WHICH IS SUPPOSED TO RESULT FROM A COMPLEX INTERACTION OF GENETIC AND EPIGENETIC, ENVIRONMENTAL AND DEVELOPMENTAL FACTORS IS ONE OF THE MOST COMMON DEBILITATING PUBLIC HEALTH PROBLEMS. THE MOLECULAR MECHANISMS UNDERLYING THIS DISEASE ARE STILL LARGELY UNCLEAR. IDENTIFYING COMMON PATHWAYS FOR DIVERSE ANTIDEPRESSANTS (ADS) AS WELL AS NEW DRUG TARGETS AND THEREBY DEVELOPING MORE EFFECTIVE TREATMENTS ARE PRIMARY GOALS OF RESEARCH IN THIS FIELD. MAJOR TARGETS OF ADS ARE THE SEROTONIN TRANSPORTER (SERT), THE NORADRENALINE TRANSPORTER (NAT) AND ALSO THE DOPAMINE TRANSPORTER (DAT) LOCATED IN THE PLASMA MEMBRANE OF CORRESPONDING NEURONS. THESE MONOAMINE TRANSPORTERS (MATS) ARE IMPORTANT REGULATORS OF THE EXTRACELLULAR NEUROTRANSMITTER CONCENTRATION. AMONG THE CLINICALLY IMPORTANT ADS ARE TRICYCLIC ADS (E.G. IMIPRAMINE), SELECTIVE SEROTONIN RE-UPTAKE INHIBITORS (SSRIS, E.G. FLUOXETINE), SELECTIVE NORADRENALINE (NA) RE-UPTAKE INHIBITORS (SNRIS, E.G. REBOXETINE) AND NAT/DAT INHIBITORS LIKE BUPROPION. THIS REVIEW IS FOCUSSING ON BRAIN CHANGES IN MONOAMINE NEUROTRANSMITTER SYSTEMS, DOWNSTREAM TARGETS OF MONOAMINERGIC NEUROTRANSMISSION AS WELL AS OF BEHAVIOURS OF MICE WITH A CONVENTIONAL KNOCKOUT (KO) OF EITHER THE SERT, DAT OR NAT. MAT KNOCKOUT INDUCES CHANGES IN BEHAVIOUR AND BRAIN NEUROCHEMISTRY. ALTHOUGH AT LEAST NATKO AND SERTKO MICE WERE EXPECTED TO SHOW A PHENOTYPE LIKE AD-TREATED WILD-TYPE MICE, THIS HOLDS TRUE ONLY FOR THE NATKO MICE WHEREAS SERTKO MICE SHOW AN ANXIETY-LIKE PHENOTYPE. CHRONIC SOCIAL OR RESTRAINT STRESS-INDUCED DEPRESSION-LIKE BEHAVIOUR AND CONCOMITANT CHANGES IN BRAIN NEUROTROPHINS ARE PREVENTED BY PHARMACOLOGICALLY DIVERSE ADS AND BY NATKO. THUS, NATKO MICE ARE AN INTERESTING TOOL TO INVESTIGATE THE MECHANISMS BEYOND MONOAMINES RESPONSIBLE FOR DEPRESSION AS WELL AS FOR AD ACTIONS. 2011 5 5152 28 PPM1F IN DENTATE GYRUS MODULATES ANXIETY-RELATED BEHAVIORS BY REGULATING BDNF EXPRESSION VIA AKT/JNK/P-H3S10 PATHWAY. ANXIETY IS A SERIOUS PSYCHIATRIC DISORDER, WITH A HIGHER INCIDENCE RATE IN WOMEN THAN IN MEN. PROTEIN PHOSPHATASE MG(2+)/MN(2+)-DEPENDENT 1F (PPM1F), A SERINE/THREONINE PHOSPHATASE, HAS BEEN SHOWN TO HAVE MULTIPLE BIOLOGICAL AND CELLULAR FUNCTIONS. HOWEVER, THE EFFECTS OF PPM1F AND ITS NEURONAL SUBSTRATES ON ANXIETY REMAIN LARGELY UNCLEAR. IN THIS STUDY, WE SHOWED THAT CHRONIC RESTRAINT STRESS (CRS) INDUCED ANXIETY-RELATED BEHAVIORS ONLY IN FEMALE MICE, WHILE ACUTE RESTRAINT STRESS (ARS) PRODUCED ANXIETY-RELATED BEHAVIORS IN BOTH MALE AND FEMALE MICE IN LIGHT-DARK AND ELEVATED PLUS MAZE TESTS AND INDUCED UPREGULATION OF PPM1F AND DOWNREGULATION OF BRAIN-DERIVED NEUROTROPHIC FACTOR (BDNF) EXPRESSION IN THE HIPPOCAMPUS. ADENO-ASSOCIATED VIRUS-MEDIATED OVEREXPRESSION OF PPM1F OR CONDITIONAL KNOCKOUT OF BDNF IN DENTATE GYRUS (DG) LED TO A MORE PRONOUNCED ANXIETY-RELATED BEHAVIOR IN FEMALE THAN IN MALE MICE AS INDICATED BY THE BEHAVIORAL EVALUATIONS. MEANWHILE, OVEREXPRESSION OF PPM1F IN THE DG DECREASED TOTAL BDNF EXON-SPECIFIC MESSENGER RNA EXPRESSION IN THE HIPPOCAMPUS WITH THE DECREASED BINDING ACTIVITY OF PHOSPHORYLATED H3S10 TO ITS INDIVIDUAL PROMOTERS IN FEMALE MICE. FURTHERMORE, WE IDENTIFIED THAT OVEREXPRESSION OF PPM1F DECREASED THE PHOSPHORYLATION LEVELS OF AKT AND JNK IN THE HIPPOCAMPUS OF FEMALE MICE. THESE RESULTS MAY SUGGEST THAT PPM1F REGULATES ANXIETY-RELATED BEHAVIORS BY MODULATING BDNF EXPRESSION AND H3S10 PHOSPHORYLATION-MEDIATED EPIGENETIC MODIFICATION, WHICH MAY BE SERVED AS POTENTIALLY PATHOLOGICAL GENES ASSOCIATED WITH ANXIETY OR OTHER MENTAL DISEASES. 2021 6 1315 34 DELTA FOSB MEDIATES EPIGENETIC DESENSITIZATION OF THE C-FOS GENE AFTER CHRONIC AMPHETAMINE EXPOSURE. THE MOLECULAR MECHANISMS UNDERLYING THE TRANSITION FROM RECREATIONAL DRUG USE TO CHRONIC ADDICTION REMAIN POORLY UNDERSTOOD. ONE MOLECULE IMPLICATED IN THIS PROCESS IS DELTAFOSB, A TRANSCRIPTION FACTOR THAT ACCUMULATES IN STRIATUM AFTER REPEATED DRUG EXPOSURE AND MEDIATES SENSITIZED BEHAVIORAL RESPONSES TO PSYCHOSTIMULANTS AND OTHER DRUGS OF ABUSE. THE DOWNSTREAM TRANSCRIPTIONAL MECHANISMS BY WHICH DELTAFOSB REGULATES DRUG-INDUCED BEHAVIORS ARE INCOMPLETELY UNDERSTOOD. WE REPORTED PREVIOUSLY THE CHROMATIN REMODELING MECHANISMS BY WHICH DELTAFOSB ACTIVATES THE EXPRESSION OF CERTAIN GENES; HOWEVER, THE MECHANISMS UNDERLYING DELTAFOSB-MEDIATED GENE REPRESSION REMAIN UNKNOWN. HERE, WE IDENTIFY C-FOS, AN IMMEDIATE EARLY GENE RAPIDLY INDUCED IN STRIATUM AFTER ACUTE PSYCHOSTIMULANT EXPOSURE, AS A NOVEL DOWNSTREAM TARGET THAT IS REPRESSED CHRONICALLY BY DELTAFOSB. WE SHOW THAT ACCUMULATION OF DELTAFOSB IN STRIATUM AFTER CHRONIC AMPHETAMINE TREATMENT DESENSITIZES C-FOS MRNA INDUCTION TO A SUBSEQUENT DRUG DOSE. DELTAFOSB DESENSITIZES C-FOS EXPRESSION BY RECRUITING HISTONE DEACETYLASE 1 (HDAC1) TO THE C-FOS GENE PROMOTER, WHICH, IN TURN, DEACETYLATES SURROUNDING HISTONES AND ATTENUATES GENE ACTIVITY. ACCORDINGLY, LOCAL KNOCK-OUT OF HDAC1 IN STRIATUM ABOLISHES AMPHETAMINE-INDUCED DESENSITIZATION OF THE C-FOS GENE. IN CONCERT, CHRONIC AMPHETAMINE INCREASES HISTONE H3 METHYLATION ON THE C-FOS PROMOTER, A CHROMATIN MODIFICATION ALSO KNOWN TO REPRESS GENE ACTIVITY, AS WELL AS EXPRESSION LEVELS OF THE H3 HISTONE METHYLTRANSFERASE, KMT1A (LYSINE METHYLTRANSFERASE 1A, FORMERLY SUV39H1). THIS STUDY REVEALS A NOVEL EPIGENETIC PATHWAY THROUGH WHICH DELTAFOSB MEDIATES DISTINCT TRANSCRIPTIONAL PROGRAMS THAT MAY ULTIMATELY ALTER BEHAVIORAL PLASTICITY TO CHRONIC AMPHETAMINE EXPOSURE. 2008 7 1821 22 EFFECTS OF CHRONIC SOCIAL DEFEAT ON BEHAVIORAL AND NEURAL CORRELATES OF SOCIALITY: VASOPRESSIN, OXYTOCIN AND THE VASOPRESSINERGIC V1B RECEPTOR. CHRONIC SOCIAL STRESS IN RODENTS PRODUCES BEHAVIORAL AND NEUROENDOCRINE PATTERNS ANALOGOUS TO SYMPTOMS ASSOCIATED WITH PSYCHOPATHOLOGIES IN HUMANS. CHRONIC SOCIAL DEFEAT IN MICE HAS BEEN USED TO STUDY THE GENETIC AND EPIGENETIC PRECURSORS OF STRESS-RELATED SOCIAL DISORDERS. THE NEUROPEPTIDES ARGININE VASOPRESSIN (AVP) AND OXYTOCIN (OT) ARE RELEASED IN CENTRAL TARGETS TO MODULATE ANTI- AND PRO-SOCIAL BEHAVIORS, RESPECTIVELY. AVP BINDS TO V1A AND V1B RECEPTORS (V1BRS) IN DISCRETE BRAIN REGIONS RELATED TO ANXIETY, DEPRESSION AND AFFILIATIVE BEHAVIORS. RECENT EVIDENCE SUGGESTS THAT V1BRS ARE INVOLVED IN STRESS AND ANXIETY AND MAY BE AN ATTRACTIVE TARGET FOR THE TREATMENT OF ASSOCIATED DISORDERS. IN THE PRESENT SERIES OF EXPERIMENTS, WE AIMED TO EVALUATE THE EFFECTS OF CHRONIC SOCIAL DEFEAT STRESS ON: 1) ANXIETY-RELATED BEHAVIORS IN A SOCIAL INVESTIGATION PARADIGM AND THEIR POTENTIAL MODULATION BY AN ACUTE DOSE OF SSR149415, A V1BR ANTAGONIST; 2) AVP AND FOS PROTEIN LEVELS IN THE PARAVENTRICULAR NUCLEUS OF THE HYPOTHALAMUS (PVN) AND; 3) AVP- AND OT-RECEPTOR (OTR) MRNA LEVELS IN BRAIN REGIONS ASSOCIATED WITH SOCIALITY. WHEN COMPARED TO UNDEFEATED ANIMALS, SOCIALLY DEFEATED MICE EXHIBITED AN ANXIOGENIC BEHAVIORAL PROFILE TOWARDS A NOVEL MALE CONSPECIFIC, WITH SSR149415 PARTLY ATTENUATING THESE EFFECTS. HISTOCHEMISTRY USING IMMUNOFLUORESCENCE SHOWED DEFEAT PRODUCED SIGNIFICANT ELEVATIONS OF FOS AND DOUBLE LABELING OF AVP AND FOS PROTEINS IN THE PARAVENTRICULAR NUCLEUS OF THE HYPOTHALAMUS (PVN). SSR149415 ATTENUATED THE EFFECTS OF DEFEAT ON FOS AND AVP/FOS DOUBLE LABELING, CONSISTENT WITH AN ANXIOLYTIC EFFECT. DEFEATED MICE SHOWED ELEVATED LEVELS OF OTR MRNA LEVELS IN THE LATERAL SEPTUM (LS) IN ADDITION TO INCREASED V1BR AND OTR MRNA IN THE MEDIAL AMYGDALA (MEA). WE SUGGEST THE INVOLVEMENT OF V1BRS AND OTRS IN A CIRCUIT INVOLVING THE PVN, MEA AND LS IN THE EFFECTS OF DEFEAT ON SOCIALITY. SSR149415 ATTENUATED ANXIOGENESIS IN THE SOCIAL INVESTIGATION MODEL AND BOTH FOS AND AVP/FOS LABELING, SUGGESTING V1BRS ARE AN ATTRACTIVE TARGET FOR THE TREATMENT OF ANXIETY IN GENERAL AND DISORDERS OF SOCIALITY IN PARTICULAR. 2011 8 5201 22 PRENATAL MORPHINE EXPOSURE INCREASES GAMMA OSCILLATION AND THETA COHERENCE IN THE RAT REWARD SYSTEM. PREVIOUS STUDIES HAVE FOUND THAT PRENATAL MORPHINE (PNM) EXPOSURE LEADS TO BOTH INCREASED AND DECREASED RISK OF SUBSTANCE ABUSE IN OFFSPRING. UNDERSTANDING MORE ABOUT THE NEUROBIOLOGICAL CHANGES AFTER THE PNM EXPOSURE WOULD HELP TO UNDERSTAND MORE ABOUT THIS ISSUE. SIGNALING FROM DOPAMINE NEURONS OF THE VENTRAL TEGMENTAL AREA (VTA) IN THE MESOACCUMBAL AND MESOCORTICAL PATHWAYS PLAYS A VITAL ROLE IN DRUG DEPENDENCY. TO PROVIDE FURTHER KNOWLEDGE ABOUT THE EFFECTS OF PNM ON DRUG SEEKING BEHAVIOR AND THE DOPAMINE SYSTEM. WE RECORDED LOCAL FIELD POTENTIALS (LFP) SIMULTANEOUSLY IN THE VTA, NAC (NUCLEUS ACCUMBENS), BLA (BASOLATERAL AMYGDALA) AND MPFC (MEDIAL PREFRONTAL CORTEX) IN MALE ADULT RATS PRENATALLY TREATED WITH SALINE OR MORPHINE. MORPHINE (10 MG/KG) INDUCED CONDITIONED PLACE PREFERENCE (CPP) ESTABLISHMENT, EXTINCTION AND PRIMING WERE TESTED TO INVESTIGATE THE EFFECTS OF PNM ON ADDICTIVE-LIKE BEHAVIOR. IN ADDITION, THE EXPRESSION OF NUCLEAR HISTONE DEACETYLASES (HDAC4, HDAC5), WHICH PLAYS ESSENTIAL EPIGENETIC ROLES IN NEUROPLASTICITY AFTER DRUG USE WERE ALSO TESTED IN VTA AND NAC. THE RESULTS SHOWED THAT PNM DID NOT CHANGE THE ACQUISITION OF MORPHINE CPP IN MALE RATS, BUT IMPAIRED CPP EXTINCTION AND MORPHINE (5 MG/KG) - PRIMED REINSTATEMENT OF CPP AFTER EXTINCTION. PNM INCREASED THE LOW GAMMA (30-60 HZ) AND HIGH (60-90 HZ) GAMMA LFP POWERS IN NAC AND BLA. PNM ALSO LEADS TO INCREASED THETA (4-9 HZ) COHERENCE BETWEEN VTA AND NAC, AND INCREASED HDAC5 EXPRESSION IN VTA. AFTER CHRONIC MORPHINE ADMINISTRATION, COHERENCE BETWEEN VTA-NAC, MPFC-NAC AND MPFC-BLA INCREASED SIGNIFICANTLY IN PNS RATS, BUT NO CHANGES WERE FIND IN PNM RATS, INDICATING IMPAIRED PLASTICITY IN BRAIN CIRCUITS. ALL THESE RESULTS SUGGEST THAT PNM EXPOSURE INCREASED REWARD PROCESSING IN ADULT MALE RATS, BUT IMPAIRED MORPHINE CPP EXTINCTION AND REINSTATEMENT, WHICH RELATE TO DECREASES NETWORK PLASTICITY AND INCREASED HDAC5 EXPRESSION IN THE REWARD SYSTEM. 2022 9 581 32 BEHAVIORAL AND NEUROCHEMICAL CHARACTERIZATION OF TRKB-DEPENDENT MECHANISMS OF AGOMELATINE IN GLUCOCORTICOID RECEPTOR-IMPAIRED MICE. GROWING EVIDENCE INDICATES THAT IMPAIRMENT OF THE STRESS RESPONSE, IN PARTICULAR THE NEGATIVE FEEDBACK REGULATION MECHANISM EXERTED BY THE HYPOTHALAMO-PITUITARY-ADRENAL (HPA) AXIS, MIGHT BE RESPONSIBLE FOR THE HIPPOCAMPAL ATROPHY OBSERVED IN DEPRESSED PATIENTS. ANTIDEPRESSANTS, POSSIBLY THROUGH THE ACTIVATION OF BDNF SIGNALING, MAY ENHANCE NEUROPLASTICITY AND RESTORE NORMAL HIPPOCAMPAL FUNCTIONS. IN THIS CONTEXT, GLUCOCORTICOID RECEPTOR-IMPAIRED (GR-I) MICE-A TRANSGENIC MOUSE MODEL OF REDUCED GR-INDUCED NEGATIVE FEEDBACK REGULATION OF THE HPA AXIS-WERE USED TO INVESTIGATE THE ROLE OF BDNF/TRKB SIGNALING IN THE BEHAVIORAL AND NEUROCHEMICAL EFFECTS OF THE NEW GENERATION ANTIDEPRESSANT DRUG, AGOMELATINE. GR-I MICE EXHIBITED MARKED ALTERATIONS IN DEPRESSIVE-LIKE AND ANXIETY-LIKE BEHAVIORS, TOGETHER WITH A DECREASED CELL PROLIFERATION AND ALTERED LEVELS OF NEUROPLASTIC AND EPIGENETIC MARKERS IN THE HIPPOCAMPUS. GR-I MICE AND THEIR WILD-TYPE LITTERMATES WERE TREATED FOR 21 DAYS WITH VEHICLE, AGOMELATINE (50MG/KG/DAY; I.P) OR THE TRKB INHIBITOR ANA-12 (0.5MG/KG/DAY, I.P) ALONE, OR IN COMBINATION WITH AGOMELATINE. CHRONIC TREATMENT WITH AGOMELATINE RESULTED IN ANTIDEPRESSANT-LIKE EFFECTS IN GR-I MICE AND REVERSED THE DEFICIT IN HIPPOCAMPAL CELL PROLIFERATION AND SOME OF THE ALTERATIONS OF MRNA PLASTICITY MARKERS IN GR-I MICE. ANA-12 BLOCKED THE EFFECT OF AGOMELATINE ON MOTOR ACTIVITY AS WELL AS ITS ABILITY TO RESTORE A NORMAL HIPPOCAMPAL CELL PROLIFERATION AND EXPRESSION OF NEUROTROPHIC FACTORS. ALTOGETHER, OUR FINDINGS INDICATE THAT AGOMELATINE REQUIRES TRKB SIGNALING TO REVERSE SOME OF THE MOLECULAR AND BEHAVIORAL ALTERATIONS CAUSED BY HPA AXIS IMPAIRMENT. 2016 10 1005 21 CHRONIC VARIABLE PHYSICAL STRESS DURING THE PERIPUBERTAL-JUVENILE PERIOD CAUSES DIFFERENTIAL DEPRESSIVE AND ANXIOGENIC EFFECTS IN THE NOVELTY-SEEKING PHENOTYPE: FUNCTIONAL IMPLICATIONS FOR HIPPOCAMPAL AND AMYGDALAR BRAIN-DERIVED NEUROTROPHIC FACTOR AND THE MOSSY FIBRE PLASTICITY. EXPERIMENTALLY NAIVE RATS SHOW VARIANCE IN THEIR LOCOMOTOR REACTIVITY TO NOVELTY, SOME DISPLAYING HIGHER (HR) WHILE OTHERS DISPLAYING LOWER (LR) REACTIVITY, ASSOCIATED WITH VULNERABILITY TO STRESS. WE EMPLOYED A CHRONIC VARIABLE PHYSICAL STRESS REGIMEN INCORPORATING INTERMITTENT AND RANDOM EXPOSURES OF PHYSICAL STRESSORS OR CONTROL HANDLING DURING THE PERIPUBERTAL-JUVENILE PERIOD TO ASSESS INTERACTIONS BETWEEN STRESS AND THE LRHR PHENOTYPE IN DEPRESSIVE- AND ANXIETY-LIKE BEHAVIORS ON THE FORCED SWIM AND SOCIAL INTERACTION TESTS, RESPECTIVELY. A DECREASE IN IMMOBILITY IN THE FORCED SWIM TEST ALONG WITH A DECREASE IN SOCIAL CONTACT IN THE SOCIAL INTERACTION TEST WERE OBSERVED IN THE JUVENILE HRS, COUPLED WITH INCREASES IN BRAIN-DERIVED NEUROTROPHIC FACTOR (BDNF) MRNA IN THE HIPPOCAMPUS AND IN THE BASOLATERAL AMYGDALA WITH CHRONIC VARIABLE PHYSICAL STRESS. IN CONTRAST, AN INCREASE IN IMMOBILITY IN THE FORCED SWIM TEST AND A DECREASE IN SOCIAL CONTACT WAS OBSERVED IN THE LR COUNTERPARTS COUPLED WITH AN INCREASE IN THE BDNF MRNA IN THE BASOLATERAL AMYGDALA FOLLOWING CHRONIC VARIABLE PHYSICAL STRESS. FURTHERMORE, CHRONIC PHYSICAL STRESS LED TO INCREASED H3 AND H4 ACETYLATION AT THE P2 AND P4 PROMOTERS OF THE HIPPOCAMPAL BDNF GENE IN THE HR RATS THAT IS ASSOCIATED WITH INCREASED SUPRAPYRAMIDAL MOSSY FIBRE (SP-MF) TERMINAL FIELD VOLUME. IN CONTRAST, CHRONIC VARIABLE PHYSICAL STRESS LED TO DECREASED H4 ACETYLATION AT THE P4 PROMOTER, ASSOCIATED WITH DECREASED SP-MF VOLUME IN THE LR RATS. THESE FINDINGS SHOW DISSOCIATION IN DEPRESSIVE- AND ANXIETY-LIKE BEHAVIORS FOLLOWING CHRONIC VARIABLE PHYSICAL STRESS IN THE JUVENILE HR ANIMALS THAT MAY BE MEDIATED BY INCREASED LEVELS OF BDNF IN THE HIPPOCAMPUS AND IN THE AMYGDALA, RESPECTIVELY. MOREOVER, CHRONIC VARIABLE PHYSICAL STRESS DURING THE PERIPUBERTAL-JUVENILE PERIOD RESULTS IN OPPOSITE EFFECTS IN DEPRESSIVE-LIKE BEHAVIOR IN THE LRHR RATS BY WAY OF INDUCING DIFFERENTIAL EPIGENETIC REGULATION OF THE HIPPOCAMPAL BDNF GENE THAT, IN TURN, MAY MEDIATE MOSSY FIBRE SPROUTING. 2011 11 4418 28 MOLECULAR AND EPIGENETIC ASPECTS OF OPIOID RECEPTORS IN DRUG ADDICTION AND PAIN MANAGEMENT IN SPORT. OPIOIDS ARE SUBSTANCES DERIVED FROM OPIUM (NATURAL OPIOIDS). IN ITS RAW STATE, OPIUM IS A GUMMY LATEX EXTRACTED FROM PAPAVER SOMNIFERUM. THE USE OF OPIOIDS AND THEIR NEGATIVE HEALTH CONSEQUENCES AMONG PEOPLE WHO USE DRUGS HAVE BEEN STUDIED. TODAY, OPIOIDS ARE STILL THE MOST COMMONLY USED AND EFFECTIVE ANALGESIC TREATMENTS FOR SEVERE PAIN, BUT THEIR USE AND ABUSE CAUSES DETRIMENTAL SIDE EFFECTS FOR HEALTH, INCLUDING ADDICTION, THUS IMPACTING THE USER'S QUALITY OF LIFE AND CAUSING OVERDOSE. THE MESOCORTICOLIMBIC DOPAMINERGIC CIRCUITRY REPRESENTS THE BRAIN CIRCUIT MEDIATING BOTH NATURAL REWARDS AND THE REWARDING ASPECTS OF NEARLY ALL DRUGS OF ABUSE, INCLUDING OPIOIDS. HENCE, UNDERSTANDING HOW OPIOIDS AFFECT THE FUNCTION OF DOPAMINERGIC CIRCUITRY MAY BE USEFUL FOR BETTER KNOWLEDGE OF THE PROCESS AND TO DEVELOP EFFECTIVE THERAPEUTIC STRATEGIES IN ADDICTION. THE AIM OF THIS REVIEW WAS TO SUMMARIZE THE MAIN FEATURES OF OPIOIDS AND OPIOID RECEPTORS AND FOCUS ON THE MOLECULAR AND UPCOMING EPIGENETIC MECHANISMS LEADING TO OPIOID ADDICTION. SINCE SYNTHETIC OPIOIDS CAN BE EFFECTIVE FOR PAIN MANAGEMENT, THEIR ABILITY TO INDUCE ADDICTION IN ATHLETES, WITH THE RISK OF INCURRING DOPING, IS ALSO DISCUSSED. 2023 12 1783 31 EFFECT OF AGOMELATINE ON MEMORY DEFICITS AND HIPPOCAMPAL GENE EXPRESSION INDUCED BY CHRONIC SOCIAL DEFEAT STRESS IN MICE. CHRONIC STRESS IS KNOWN TO INDUCE NOT ONLY ANXIETY AND DEPRESSIVE-LIKE PHENOTYPES IN MICE BUT ALSO COGNITIVE IMPAIRMENTS, FOR WHICH THE ACTION OF CLASSICAL ANTIDEPRESSANT COMPOUNDS REMAINS UNSATISFACTORY. IN THIS CONTEXT, WE INVESTIGATED THE EFFECTS OF CHRONIC SOCIAL DEFEAT STRESS (CSDS) ON ANXIETY-, SOCIAL- AND COGNITIVE-RELATED BEHAVIORS, AS WELL AS HIPPOCAMPAL BDNF, SYNAPTIC PLASTICITY MARKERS (PSD-95, SYNAPTOPHYSIN, SPINOPHILIN, SYNAPSIN I AND MAP-2), AND EPIGENETIC MODIFYING ENZYMES (MYST2, HDAC2, HDAC6, MLL3, KDM5B, DNMT3B, GADD45B) GENE EXPRESSION IN C57BL/6J MICE. CSDS FOR 10 DAYS PROVOKED LONG-LASTING ANXIOUS-LIKE PHENOTYPE IN THE OPEN FIELD AND EPISODIC MEMORY DEFICITS IN THE NOVEL OBJECT RECOGNITION TEST. WHILE TOTAL BDNF MRNA LEVEL WAS UNCHANGED, BDNF EXON IV, MAP-2, HDAC2, HDAC6 AND MLL3 GENE EXPRESSION WAS SIGNIFICANTLY DECREASED IN THE CSDS MOUSE HIPPOCAMPUS. IN CSDS MICE TREATED 3 WEEKS WITH 50 MG/KG/D AGOMELATINE, AN ANTIDEPRESSANT WITH MELATONERGIC RECEPTOR AGONIST AND 5-HT(2C) RECEPTOR ANTAGONIST PROPERTIES, THE ANXIOUS-LIKE PHENOTYPE WAS NOT REVERSED, BUT THE TREATMENT SUCCESSFULLY PREVENTED THE COGNITIVE IMPAIRMENTS AND HIPPOCAMPAL GENE EXPRESSION MODIFICATIONS. ALTOGETHER, THESE DATA EVIDENCED THAT, IN MICE, AGOMELATINE WAS EFFECTIVE IN ALLEVIATING STRESS-INDUCED ALTERED COGNITIVE FUNCTIONS, POSSIBLY THROUGH A MECHANISM INVOLVING BDNF SIGNALING, SYNAPTIC PLASTICITY AND EPIGENETIC REMODELING. 2017 13 4402 24 MODULATION OF NOCICEPTION BY SOCIAL FACTORS IN RODENTS: CONTRIBUTION OF THE OPIOID SYSTEM. RATIONALE: THE OPIOID SYSTEM IS INVOLVED IN THE REGULATION OF SEVERAL BEHAVIORAL AND PHYSIOLOGICAL RESPONSES, CONTROLLING PAIN, REWARD, AND ADDICTIVE BEHAVIORS. OPIOID ADMINISTRATION, DEPENDING ON DRUGS AND DOSES, USUALLY AFFECTS SOCIABILITY REDUCING INTERACTIONS BETWEEN CONSPECIFICS, WHEREAS SOME AFFILIATIVE BEHAVIORS SUCH AS SEXUAL ACTIVITY, SOCIAL GROOMING, AND PLAY BEHAVIOR INCREASE THE ENDOGENOUS OPIOID ACTIVITY. OBJECTIVES: THE POSSIBLE INTERACTION BETWEEN ENDOGENOUS OPIOIDS RELEASED DURING SOCIO/SEXUAL BEHAVIOR AND THEIR ANALGESIC EFFECT ON PAIN RESPONSE IS REVIEWED IN THE RODENT LITERATURE. RESULTS: DIRECT EVIDENCE FOR SOCIALLY MEDIATED OPIOID CHANGES RESULTING IN INCREASE IN NOCICEPTIVE THRESHOLD DERIVES FROM STUDIES EXPLORING THE EFFECTS OF DEFEAT EXPERIENCES, SOCIAL ISOLATION, MATERNAL, SEXUAL BEHAVIOR, AND SOCIAL REUNION AMONG KIN OR FAMILIAR ANIMALS IN LABORATORY RODENTS. INDIRECT EVIDENCE FOR ENDOGENOUS ACTIVATION OF THE OPIOID SYSTEM, POSSIBLY AFFECTING PAIN SENSITIVITY, DERIVES FROM STUDIES INVESTIGATING THE RELEVANCE OF NATURAL SOCIAL REWARD USING THE CONDITIONED PLACE PREFERENCE PROTOCOLS OR ANALYZING ULTRASONIC VOCALIZATIONS ASSOCIATED TO POSITIVE AFFECTIVE CONTEXTS. FINALLY, GENETIC AND EPIGENETIC FACTORS THAT AFFECT THE OPIOID SYSTEM DURING DEVELOPMENT ARE REPORTED TO BE INVOLVED IN MODULATING THE RESPONSE TO SOCIAL STIMULI AS WELL AS NOCICEPTION. CONCLUSIONS: ALL STUDIES HIGHLIGHT THE RELEVANCE OF AFFILIATIVE CONTACT BEHAVIOR BETWEEN CONSPECIFICS THAT IS RESPONSIBLE FOR THE ACTIVATION OF THE ENDOGENOUS MU-OPIOID SYSTEM, INDUCING NOCICEPTIVE THRESHOLD INCREASE. 2012 14 3650 25 INCREASED TRANSCRIPTION OF TSPO, HDAC2, AND HDAC6 IN THE AMYGDALA OF MALES WITH ALCOHOL USE DISORDER. INTRODUCTION: REPEATED EXPOSURE TO HIGH DOSES OF ALCOHOL TRIGGERS NEUROINFLAMMATORY PROCESSES THAT CONTRIBUTE TO CRAVING AND MOOD DYSFUNCTION IN ALCOHOL USE DISORDER (AUD). THE UPREGULATION OF THE TRANSLOCATOR PROTEIN (TSPO) IS CONSIDERED A BIOMARKER OF NEUROINFLAMMATION, AND TSPO LIGANDS HAVE BEEN USED AS NEUROIMAGING BIOMARKERS OF NEUROINFLAMMATION. EPIGENETIC MECHANISMS ARE ALSO IMPLICATED IN NEUROINFLAMMATORY RESPONSES TO ALCOHOL, AND ELEVATED EXPRESSION OF HDAC2 AND HDAC6 HAS BEEN REPORTED IN THE BRAIN OF ANIMALS EXPOSED TO CHRONIC ALCOHOL. METHODS: THE PRESENT STUDY EXAMINED THE TRANSCRIPTIONAL REGULATION OF TSPO, HDAC2, AND HDAC6 IN HUMAN POSTMORTEM BRAIN TISSUE FROM MALES PREVIOUSLY DIAGNOSED WITH AUD (N = 11) COMPARED TO AGE-MATCHED NONDEPENDENT MALES (N = 13) IN FOUR BRAIN REGIONS RELEVANT TO AUD: PREFRONTAL CORTEX (PFC), NUCLEUS ACCUMBENS (NAC), HIPPOCAMPUS (HPP), AND AMYGDALA (AMY). RESULTS: TRANSLOCATOR PROTEIN MRNA LEVELS IN AMY AND PFC AND HDAC2 AND HDAC6 MRNA LEVELS IN AMY WERE UPREGULATED IN AUD COMPARED TO CONTROLS. IN AMY, TSPO MRNA LEVELS WERE POSITIVELY ASSOCIATED WITH HDAC2 AND HDAC6 MRNA LEVELS, SUGGESTING A POSSIBLE REGULATION OF TSPO BY HDAC2 AND HDAC6 IN THIS BRAIN REGION. IN CONTRAST, THERE WERE NO GROUP DIFFERENCES FOR TSPO, HDAC2, AND HDAC6 IN NAC AND HPP. CONCLUSION: OUR STUDY IS THE FIRST TO FIND UPREGULATED TSPO MRNA LEVELS IN AMY AND PFC IN POSTMORTEM BRAINS FROM AUD CONSISTENT WITH NEUROINFLAMMATION, AND IN THE AMYGDALA, THEY IMPLICATE EPIGENETIC REGULATION OF TSPO BY HDAC2 AND HDAC6. 2021 15 1706 26 DYNORPHIN/KOP AND NOCICEPTIN/NOP GENE EXPRESSION AND EPIGENETIC CHANGES BY COCAINE IN RAT STRIATUM AND NUCLEUS ACCUMBENS. COCAINE INDUCES NEUROCHEMICAL CHANGES OF ENDOGENOUS PRODYNORPHIN-KAPPA OPIOID RECEPTOR (PDYN-KOP) AND PRONOCICEPTIN/ORPHANINFQ-NOCICEPTIN RECEPTOR (PN/OFQ-NOP) SYSTEMS. BOTH SYSTEMS PLAY AN IMPORTANT ROLE IN REWARDING MECHANISMS AND ADDICTIVE STIMULUS PROCESSING BY MODULATING DRUG-INDUCED DOPAMINERGIC ACTIVATION IN THE MESOCORTICO-LIMBIC BRAIN AREAS. THEY ARE ALSO INVOLVED IN REGULATING STRESS MECHANISMS RELATED TO ADDICTION. THE AIM OF THIS STUDY WAS TO INVESTIGATE POSSIBLE CHANGES OF GENE EXPRESSION OF THE DYNORPHINERGIC AND NOCICEPTINERGIC SYSTEM COMPONENTS IN THE NUCLEUS ACCUMBENS (NA) AND IN MEDIAL AND LATERAL CAUDATE PUTAMEN (MCPU AND LCPU, RESPECTIVELY) OF RATS, FOLLOWING CHRONIC SUBCUTANEOUS INFUSION OF COCAINE. IN ADDITION, THE EPIGENETIC HISTONE MODIFICATIONS H3K4ME3 AND H3K27ME3 (AN ACTIVATING AND A REPRESSIVE MARKER, RESPECTIVELY) AT THE PROMOTER LEVEL OF THE PDYN, KOP, PN/OFQ AND NOP GENES WERE INVESTIGATED. RESULTS SHOWED THAT COCAINE INDUCED PDYN GENE EXPRESSION UP-REGULATION IN THE NA AND LCPU, AND ITS DOWN-REGULATION IN THE MCPU, WHEREAS KOP MRNA LEVELS WERE UNCHANGED. MOREOVER, COCAINE EXPOSURE DECREASED PN/OFQ GENE EXPRESSION IN THE NA AND LCPU, WHILE NOP MRNA LEVELS APPEARED SIGNIFICANTLY INCREASED IN THE NA AND DECREASED IN THE LCPU. SPECIFIC CHANGES OF THE H3K4ME3 AND H3K27ME3 LEVELS WERE FOUND AT PDYN, PN/OFQ, AND NOP GENE PROMOTER, CONSISTENT WITH THE OBSERVED GENE EXPRESSION ALTERATIONS. THE PRESENT FINDINGS CONTRIBUTE TO BETTER DEFINE THE ROLE OF ENDOGENOUS PDYN-KOP AND PN/OFQ-NOP SYSTEMS IN NEUROPLASTICITY MECHANISMS FOLLOWING CHRONIC COCAINE TREATMENT. THE EPIGENETIC HISTONE MODIFICATIONS UNDERLYING THE GENE EXPRESSION CHANGES LIKELY MEDIATE THE EFFECTS OF COCAINE ON TRANSCRIPTIONAL REGULATION OF SPECIFIC GENE PROMOTERS THAT RESULT IN LONG-LASTING DRUG-INDUCED PLASTICITY. 2014 16 998 20 CHRONIC SUBCONVULSIVE ACTIVITY DURING EARLY POSTNATAL LIFE PRODUCES AUTISTIC BEHAVIOR IN THE ABSENCE OF NEUROTOXICITY IN THE JUVENILE WEANLING PERIOD. THE DIAGNOSIS OF AUTISM SPECTRUM DISORDER (ASD) VARIES FROM VERY MILD TO SEVERE SOCIAL AND COGNITIVE IMPAIRMENTS. WE HYPOTHESIZED THAT EPIGENETIC SUBCONVULSIVE ACTIVITY IN EARLY POSTNATAL LIFE MAY CONTRIBUTE TO THE DEVELOPMENT OF AUTISTIC BEHAVIOR IN A SEX-RELATED MANNER. LOW DOSES OF KAINIC ACID (KA) (25-100 MUG) WERE ADMINISTERED TO RAT PUPS FOR 15 DAYS BEGINNING ON POSTNATAL (P) DAY 6 TO CHRONICALLY ELEVATE NEURONAL ACTIVITY. A BATTERY OF CLASSICAL AND NOVEL BEHAVIORAL TESTS WAS USED, AND SEX DIFFERENCES WERE OBSERVED. OUR NOVEL OPEN HANDLING TEST REVEALED THAT ASD MALES NOSE POKED MORE OFTEN AND ASD FEMALES CLIMBED AND ESCAPED MORE FREQUENTLY WITH AGE. IN THE SOCIAL INTERACTION TEST, ASD MALES WERE LESS SOCIAL THAN ASD FEMALES WHO WERE MORE ANXIOUS IN HANDLING AND ELEVATED PLUS MAZE (EPM) TASKS. TO EVALUATE GROUP DYNAMICS, SIBLING AND NON-SIBLING CONTROL AND EXPERIMENTAL ANIMALS EXPLORED 3 DIFFERENT SHAPED NOVEL SOCIAL ENVIRONMENTS. CONTROL PUPS HUDDLED QUICKLY AND MORE FREQUENTLY IN ALL ENVIRONMENTS WHETHER THEY SOCIALIZED WITH LITTERMATES OR NON-SIBLINGS COMPARED TO ASD GROUPS. NON-SIBLING ASD PUPS WERE ERRATIC AND HUDDLED IN SMALLER GROUPS. IN THE OBJECT RECOGNITION TEST, ONLY ASD MALES SPENT LESS TIME WITH THE NOVEL OBJECT COMPARED TO CONTROL PUPS. DATA SUGGEST THAT CHRONIC SUBCONVULSIVE ACTIVITY IN EARLY POSTNATAL LIFE LEADS TO AN ASD PHENOTYPE IN THE ABSENCE OF CELL DEATH. MALES WERE MORE SUSCEPTIBLE TO DEVELOPING ASOCIAL BEHAVIORS AND COGNITIVE PATHOLOGIES, WHEREAS FEMALES WERE PRONE TO HIGHER LEVELS OF HYPERACTIVITY AND ANXIETY, VALIDATING OUR POSTNATAL ASD MODEL APPARENT IN THE PRE-JUVENILE PERIOD. 2019 17 4857 22 OPTOGENETIC STIMULATION OF THE ANTERIOR CINGULATE CORTEX AMELIORATES AUTISTIC-LIKE BEHAVIORS IN RATS INDUCED BY NEONATAL ISOLATION, CAUDATE PUTAMEN AS A SITE FOR ALTERATION. EPIGENETIC AGENTS, SUCH AS NEONATAL ISOLATION DURING NEURODEVELOPMENTAL PERIOD OF LIFE, CAN CHANGE VARIOUS REGIONS OF THE BRAIN. IT MAY FURTHER INDUCE PSYCHOLOGICAL DISORDERS SUCH AS AUTISTIC-LIKE PHENOMENA. THIS STUDY INDICATED THE ROLE OF CHRONIC INCREASED ANTERIOR CINGULATE CORTEX (ACC) OUTPUT ON ALTERATION OF CAUDATE PUTAMEN (CPU) AS A MAIN BEHAVIOR REGULATOR REGION OF THE BRAIN IN ADULT MATERNAL DEPRIVED (MD) RATS. FOR MAKING AN ANIMAL MODEL, NEONATES WERE ISOLATED FROM THEIR MOTHERS IN POSTNATAL DAYS (PND 1-10, 3 H/DAY). SUBSEQUENTLY, THEY BILATERALLY RECEIVED PLENTI-CAMKIIA-HCHR2 (H134R)-MCHERRY-WPRE VIRUS IN ACC AREA VIA STEREOTAXIC SURGERY IN PND50. AFTER 22 DAYS, THESE REGIONS WERE EXPOSED TO BLUE LASER (473 NM) FOR SIX CONSECUTIVE DAYS (15 MIN/DAY). THEN, BEHAVIORAL DEFICITS WERE TESTED AND WERE COMPARED WITH CONTROL GROUP IN THE FOLLOWING DAY. ANIMALS WERE IMMEDIATELY KILLED AND THEIR BRAINS WERE PREPARED FOR TISSUE PROCESSING. RESULTS SHOWED THAT NEONATAL ISOLATION INDUCES AUTISTIC-LIKE BEHAVIORS AND LEADS TO OVEREXPRESSION OF NMDAR1 AND NOX2-GP91(PHOX) PROTEINS AND ELEVATION OF CATALASE ACTIVITY IN THE CPU REGIONS OF THE ADULT OFFSPRING COMPARED WITH CONTROL GROUP. CHRONIC OPTOGENETIC STIMULATION OF ACC NEURONS CONTAINING (CHR2+) LED TO SIGNIFICANT REDUCTION IN THE APPEARANCE OF STEREOTYPICAL BEHAVIOR AND ALIEN-PHOBIA IN MD RATS. THE AMOUNT OF NMDAR1 AND NOX2-GP91(PHOX) EXPRESSION AND THE CATALASE ACTIVITY IN CPU WERE REDUCED AFTER THIS TREATMENT. THEREFORE, AUTISTIC-LIKE BEHAVIOR SEEMS TO BE RELATED WITH ELEVATION OF NMDAR1 AND NOX2-GP91(PHOX) PROTEIN LEVELS THAT ENHANCE THE EFFECT OF GLUTAMATERGIC PROJECTION ON CPU REGIONS. OPTOGENETIC TREATMENT ALSO COULD AMELIORATE BEHAVIORAL DEFICITS BY MODULATING THESE PROTEIN DENSITIES. 2019 18 294 18 AGING INCREASES VULNERABILITY TO STRESS-INDUCED DEPRESSION VIA UPREGULATION OF NADPH OXIDASE IN MICE. BRAIN AGING PROCEEDS WITH CELLULAR AND MOLECULAR CHANGES IN THE LIMBIC SYSTEM. AGING-DEPENDENT CHANGES MIGHT AFFECT EMOTION AND STRESS COPING, YET THE UNDERLYING MECHANISMS REMAIN UNCLEAR. HERE, WE SHOW AGED (18-MONTH-OLD) MICE EXHIBIT UPREGULATION OF NADPH OXIDASE AND OXIDATIVE STRESS IN THE HIPPOCAMPUS, WHICH MIRRORS THE CHANGES IN YOUNG (2-MONTH-OLD) MICE SUBJECTED TO CHRONIC STRESS. AGED MICE THAT LACK P47PHOX, A KEY SUBUNIT OF NADPH OXIDASE, DO NOT SHOW INCREASED OXIDATIVE STRESS. AGED MICE EXHIBIT DEPRESSION-LIKE BEHAVIOR FOLLOWING WEAK STRESS THAT DOES NOT PRODUCE DEPRESSIVE BEHAVIOR IN YOUNG MICE. AGED MICE HAVE REDUCED EXPRESSION OF THE EPIGENETIC FACTOR SUV39H1 AND ITS UPSTREAM REGULATOR P-AMPK, AND INCREASED EXPRESSION OF PPP2CA IN THE HIPPOCAMPUS-CHANGES THAT OCCUR IN YOUNG MICE EXPOSED TO CHRONIC STRESS. SUV39H1 MEDIATES STRESS- AND AGING-INDUCED SUSTAINED UPREGULATION OF P47PHOX AND OXIDATIVE STRESS. THESE RESULTS SUGGEST THAT AGING INCREASES SUSCEPTIBILITY TO STRESS BY UPREGULATING NADPH OXIDASE IN THE HIPPOCAMPUS. 2020 19 1197 29 CORTICOSTERONE INDUCES DISCRETE EPIGENETIC SIGNATURES IN THE DORSAL AND VENTRAL HIPPOCAMPUS THAT DEPEND UPON SEX AND GENOTYPE: FOCUS ON METHYLATED NR3C1 GENE. THE GENOMIC EFFECTS OF CIRCULATING GLUCOCORTICOIDS ARE PARTICULARLY RELEVANT IN CORTICO-LIMBIC STRUCTURES, WHICH EXPRESS A HIGH CONCENTRATION OF STEROID HORMONE RECEPTORS. TO DATE, NO STUDIES HAVE INVESTIGATED GENOMIC DIFFERENCES IN HIPPOCAMPAL SUBREGIONS, NAMELY THE DORSAL (DHPC) AND VENTRAL (VHPC) HIPPOCAMPUS, IN PRECLINICAL MODELS TREATED WITH EXOGENOUS GLUCOCORTICOIDS. CHRONIC ORAL CORTICOSTERONE (CORT) IN MOUSE IS A PHARMACOLOGICAL APPROACH THAT DISRUPTS THE ACTIVITY OF THE HYPOTHALAMIC-PITUITARY-ADRENAL AXIS, INCREASES AFFECTIVE BEHAVIOR, AND INDUCES GENOMIC CHANGES AFTER STRESS IN THE HPC OF WILDTYPE (WT) MICE AND MICE HETEROZYGOUS FOR THE GENE CODING FOR BRAIN-DERIVED NEUROTROPHIC FACTOR VAL66MET (HMET), A VARIANT ASSOCIATED WITH GENETIC SUSCEPTIBILITY TO STRESS. USING RNA-SEQUENCING, WE INVESTIGATED THE GENOMIC SIGNATURES OF ORAL CORT IN THE DHPC AND VHPC OF WT AND HMET MALE AND FEMALE MICE, AND EXAMINED SEX AND GENOTYPE DIFFERENCES IN RESPONSE TO ORAL CORT. MALES UNDER CORT SHOWED LOWER GLYCEMIA AND INCREASED ANXIETY- AND DEPRESSION-LIKE BEHAVIOR COMPARED TO FEMALES THAT SHOWED INSTEAD OPPOSITE AFFECTIVE BEHAVIOR IN RESPONSE TO CORT. RANK-RANK-HYPERGEOMETRIC OVERLAP (RRHO) WAS USED TO IDENTIFY GENES FROM A CONTINUOUS GRADIENT OF SIGNIFICANCY THAT WERE CONCORDANT ACROSS GROUPS. RRHO SHOWED THAT CORT-INDUCED DIFFERENTIALLY EXPRESSED GENES (DEGS) IN WT MICE AND HMET MICE CONVERGED IN THE DHPC OF MALES AND FEMALES, WHILE IN THE VHPC, DEGS CONVERGED IN MALES AND DIVERGED IN FEMALES. THE VHPC SHOWED A HIGHER NUMBER OF DEGS COMPARED TO THE DHPC AND EXHIBITED SEX DIFFERENCES RELATED TO GLUCOCORTICOID RECEPTOR (GR)-BINDING GENES AND EPIGENETIC MODIFIERS. METHYL-DNA-IMMUNOPRECIPITATION IN THE VHPC REVEALED DIFFERENTIAL METHYLATION OF THE EXONS 1(C) AND 1(F) OF THE GR GENE (NR3C1) IN HMET FEMALES. TOGETHER, WE REPORT BEHAVIORAL AND ENDOCRINOLOGICAL SEX DIFFERENCES IN RESPONSE TO CORT, AS WELL AS EPIGENETIC SIGNATURES THAT I) DIFFER IN THE DHPC AND VHPC,II) ARE DISTINCT IN MALES AND FEMALES, AND III) IMPLICATE DIFFERENTIAL METHYLATION OF NR3C1 SELECTIVELY IN HMET FEMALES. 2022 20 2666 28 ESTABLISHMENT OF AN INTERMITTENT COLD STRESS MODEL USING TUPAIA BELANGERI AND EVALUATION OF COMPOUND C737 TARGETING NEURON-RESTRICTIVE SILENCER FACTOR. PREVIOUS STUDIES HAVE SHOWN THAT INTERMITTENT COLD STRESS (ICS) INDUCES DEPRESSION-LIKE BEHAVIORS IN MAMMALS. TUPAIA BELANGERI (THE TREE SHREW) IS THE ONLY EXPERIMENTAL ANIMAL OTHER THAN THE CHIMPANZEE THAT HAS BEEN SHOWN TO BE SUSCEPTIBLE TO INFECTION BY HEPATITIS B AND C VIRUSES. MOREOVER, FULL GENOME SEQUENCE ANALYSIS HAS REVEALED STRONG HOMOLOGY BETWEEN HOST PROTEINS IN TUPAIA AND IN HUMANS AND OTHER PRIMATES. TUPAIA NEUROMODULATOR RECEPTOR PROTEINS ARE ALSO KNOWN TO HAVE A HIGH DEGREE OF HOMOLOGY WITH THEIR CORRESPONDING PRIMATE PROTEINS. BASED ON THESE SIMILARITIES, WE HYPOTHESIZED THAT INDUCTION OF ICS IN TUPAIA WOULD PROVIDE A USEFUL ANIMAL MODEL OF STRESS RESPONSES. WE EXPOSED YOUNG ADULT TUPAIA TO ICS AND OBSERVED DECREASES IN BODY TEMPERATURE AND BODY WEIGHT IN BOTH FEMALE AND MALE TUPAIA, SUGGESTING THAT TUPAIA ARE AN APPROPRIATE ANIMAL MODEL FOR ICS STUDIES. WE FURTHER EXAMINED THE EFFICACY OF A NEW SMALL-MOLECULE COMPOUND, C737, AGAINST THE EFFECTS OF ICS. C737 MIMICS THE HELICAL STRUCTURE OF NEURON-RESTRICTIVE SILENCER FACTOR (NRSF/REST), WHICH REGULATES A WIDE RANGE OF TARGET GENES INVOLVED IN NEURONAL FUNCTION AND PAIN MODULATION. TREATMENT WITH C737 SIGNIFICANTLY REDUCED STRESS-INDUCED WEIGHT LOSS IN FEMALE TUPAIA; THESE EFFECTS WERE STRONGER THAN THOSE ELICITED BY THE ANTIDEPRESSANT AGOMELATINE. THESE RESULTS SUGGEST THAT TUPAIA REPRESENTS A USEFUL NON-RODENT ICS MODEL. OUR DATA ALSO PROVIDE NEW INSIGHTS INTO THE FUNCTION OF NRSF/REST IN STRESS-INDUCED DEPRESSION AND OTHER DISORDERS WITH EPIGENETIC INFLUENCES OR THOSE WITH HIGH PREVALENCE IN WOMEN. 2016