1 6528 142 TRANSCRIPTIONAL CORRELATES OF CHRONIC ALCOHOL NEUROADAPTATION IN DROSOPHILA LARVAE. WHEN PRESENTED WITH THE CHOICE, DROSOPHILA MELANOGASTER FEMALES WILL OFTEN PREFER TO LAY EGGS ON FOOD CONTAINING A SIGNIFICANT AMOUNT OF ALCOHOL. WHILE, IN SOME CASES, THIS BEHAVIORAL DECISION CAN PROVIDE A SURVIVAL ADVANTAGE TO THE DEVELOPING LARVAE, IT CAN ALSO LEAD TO DEVELOPMENTAL AND COGNITIVE PROBLEMS. ALCOHOL CONSUMPTION CAN AFFECT EXECUTIVE FUNCTIONS, EPISODIC MEMORY, AND OTHER BRAIN FUNCTION CAPACITIES. HOWEVER, IN THE FRUIT FLY, THE INITIAL COGNITIVE EFFECTS OF ALCOHOL CONSUMPTION HAVE BEEN SHOWN TO REVERSE UPON PERSISTENT EXPOSURE TO ALCOHOL. USING AN OLFACTORY CONDITIONING ASSAY WHERE AN ODORANT IS IMPLEMENTED AS A CONDITIONED STIMULUS AND PAIRED WITH A HEAT SHOCK AS AN UNCONDITIONED STIMULUS, A PREVIOUS STUDY HAS SHOWN THAT WHEN EXPOSED TO A SHORT ACUTE DOSE OF ALCOHOL, DROSOPHILA LARVAE CAN NO LONGER LEARN THIS ASSOCIATION. INTERESTINGLY, UPON PROLONGED CHRONIC ALCOHOL EXPOSURE, LARVAE SEEM TO SUCCESSFULLY AVOID THE CONDITIONED STIMULUS JUST AS WELL AS CONTROL ALCOHOL-NAIVE LARVAE, SUGGESTIVE OF ALCOHOL-INDUCED NEUROADAPTATIONS. HOWEVER, THE MECHANISMS BY WHICH DROSOPHILA ADAPT TO THE PRESENCE OF ALCOHOL REMAINS UNKNOWN. IN THIS STUDY, WE EXPLORE THE TRANSCRIPTIONAL CORRELATES OF NEUROADAPTATION IN DROSOPHILA LARVAE EXPOSED TO CHRONIC ALCOHOL TO UNDERSTAND THE GENETIC AND CELLULAR COMPONENTS RESPONSIBLE FOR THIS ADAPTATION. FOR THIS, WE EMPLOYED RNA SEQUENCING TECHNOLOGY TO EVALUATE DIFFERENCES IN GENE EXPRESSION IN THE BRAIN OF LARVAE CHRONICALLY EXPOSED TO ALCOHOL. OUR RESULTS SUGGEST THAT ALCOHOL-INDUCED NEUROADAPTATIONS ARE MODULATED BY A DIVERSE ARRAY OF SYNAPTIC GENES WITHIN THE LARVAL BRAIN THROUGH A SERIES OF EPIGENETIC MODULATORS. 2021 2 5165 29 PRECLINICAL RESERPINE MODELS RECAPITULATING MOTOR AND NON-MOTOR FEATURES OF PARKINSON'S DISEASE: ROLES OF EPIGENETIC UPREGULATION OF ALPHA-SYNUCLEIN AND AUTOPHAGY IMPAIRMENT. RESERPINE IS AN EFFECTIVE DRUG FOR THE CLINICAL TREATMENT OF HYPERTENSION. IT ALSO INDUCES PARKINSON'S DISEASE (PD)-LIKE SYMPTOMS IN HUMANS AND ANIMALS POSSIBLE THROUGH THE INHIBITION OF MONOAMINE VESICULAR TRANSPORTERS, THUS DECREASING THE LEVELS OF MONOAMINE NEUROTRANSMITTERS IN THE BRAIN. HOWEVER, THE PRECISE MECHANISMS REMAIN UNCLEAR. HEREIN, WE AIMED TO DEVELOP A PRECLINICAL RESERPINE MODEL RECAPITULATING THE NON-MOTOR AND MOTOR SYMPTOMS OF PD AND INVESTIGATE THE UNDERLYING POTENTIAL CELLULAR MECHANISMS. INCUBATION OF RESERPINE INDUCED APOPTOSIS, LED TO THE ACCUMULATION OF INTRACELLULAR REACTIVE OXYGEN SPECIES (ROS), LOWERED DNA METHYLATION OF ALPHA-SYNUCLEIN GENE, RESULTED IN ALPHA-SYNUCLEIN PROTEIN DEPOSITION, AND ELEVATED THE RATIO OF LC3-II/LC3-I AND P62 IN CULTURED SH-SY5Y CELLS. FEEDING RESERPINE DOSE-DEPENDENTLY SHORTENED THE LIFESPAN AND CAUSED IMPAIRMENT OF MOTOR FUNCTIONS IN MALE AND FEMALE DROSOPHILA. MOREOVER, LONG-TERM ORAL ADMINISTRATION OF RESERPINE LED TO MULTIPLE MOTOR AND NON-MOTOR SYMPTOMS, INCLUDING CONSTIPATION, PAIN HYPERSENSITIVITY, OLFACTORY IMPAIRMENT, AND DEPRESSION-LIKE BEHAVIORS IN MICE. THE MECHANISTIC STUDIES SHOWED THAT CHRONIC RESERPINE EXPOSURE CAUSED HYPOMETHYLATION OF THE ALPHA-SYNUCLEIN GENE AND UP-REGULATED ITS EXPRESSION AND ELEVATED THE RATIO OF LC3-II/LC3-I AND EXPRESSION OF P62 IN THE SUBSTANTIA NIGRA OF MICE. THUS, WE ESTABLISHED PRECLINICAL ANIMAL MODELS USING RESERPINE TO RECAPITULATE THE MOTOR AND NON-MOTOR SYMPTOMS OF PD. CHRONIC RESERPINE EXPOSURE EPIGENETICALLY ELEVATED THE LEVELS OF ALPHA-SYNUCLEIN EXPRESSION POSSIBLE BY LOWERING THE DNA METHYLATION STATUS AND INDUCING AUTOPHAGIC IMPAIRMENT IN VITRO AND IN VIVO. 2022 3 843 45 CHEMOSENSORY ABILITY AND SENSITIVITY IN HEALTH AND DISEASE: EPIGENETIC REGULATION AND COVID-19. THROUGHOUT THE ANIMAL KINGDOM, OUR TWO CHEMICAL SENSES, OLFACTION AND GUSTATION, ARE DEFINED BY TWO PRIMARY FACTORS: GENOMIC ARCHITECTURE OF THE ORGANISMS AND THEIR LIVING ENVIRONMENT. DURING THE PAST THREE YEARS OF THE GLOBAL COVID-19 PANDEMIC, THESE TWO SENSORY MODALITIES HAVE DRAWN MUCH ATTENTION AT THE BASIC SCIENCE AND CLINICAL LEVELS BECAUSE OF THE STRONG ASSOCIATION OF OLFACTORY AND GUSTATORY DYSFUNCTION WITH VIRAL INFECTION. LOSS OF OUR SENSE OF SMELL ALONE, OR TOGETHER WITH A LOSS OF TASTE, HAS EMERGED AS A RELIABLE INDICATOR OF COVID-19 INFECTION. PREVIOUSLY, SIMILAR DYSFUNCTIONS HAVE BEEN DETECTED IN A LARGE COHORT OF PATIENTS WITH CHRONIC CONDITIONS. THE RESEARCH FOCUS REMAINS ON UNDERSTANDING THE PERSISTENCE OF OLFACTORY AND GUSTATORY DISTURBANCES IN THE POST-INFECTION PHASE, ESPECIALLY IN CASES WITH LONG-TERM EFFECT OF INFECTION (LONG COVID). ALSO, BOTH SENSORY MODALITIES SHOW CONSISTENT AGE-RELATED DECLINE IN STUDIES AIMED TO UNDERSTAND THE PATHOLOGY OF NEURODEGENERATIVE CONDITIONS. SOME STUDIES USING CLASSICAL MODEL ORGANISMS SHOW AN IMPACT ON NEURAL STRUCTURE AND BEHAVIOR IN OFFSPRING AS AN OUTCOME OF PARENTAL OLFACTORY EXPERIENCE. THE METHYLATION STATUS OF SPECIFIC ODORANT RECEPTORS, ACTIVATED IN PARENTS, IS PASSED ON TO THE OFFSPRING. FURTHERMORE, EXPERIMENTAL EVIDENCE INDICATES AN INVERSE CORRELATION OF GUSTATORY AND OLFACTORY ABILITIES WITH OBESITY. SUCH DIVERSE LINES OF EVIDENCE EMERGING FROM BASIC AND CLINICAL RESEARCH STUDIES INDICATE A COMPLEX INTERPLAY OF GENETIC FACTORS, EVOLUTIONARY FORCES, AND EPIGENETIC ALTERATIONS. ENVIRONMENTAL FACTORS THAT REGULATE GUSTATION AND OLFACTION COULD INDUCE EPIGENETIC MODULATION. HOWEVER, IN TURN, SUCH MODULATION LEADS TO VARIABLE EFFECTS DEPENDING ON GENETIC MAKEUP AND PHYSIOLOGICAL STATUS. THEREFORE, A LAYERED REGULATORY HIERARCHY REMAINS ACTIVE AND IS PASSED ON TO MULTIPLE GENERATIONS. IN THE PRESENT REVIEW, WE ATTEMPT TO UNDERSTAND THE EXPERIMENTAL EVIDENCE THAT INDICATES VARIABLE REGULATORY MECHANISMS THROUGH MULTILAYERED AND CROSS-REACTING PATHWAYS. OUR ANALYTICAL APPROACH WILL ADD TO ENHANCEMENT OF PREVAILING THERAPEUTIC INTERVENTIONS AND BRING TO THE FOREFRONT THE SIGNIFICANCE OF CHEMOSENSORY MODALITIES FOR THE EVALUATION AND MAINTENANCE OF LONG-TERM HEALTH. 2023 4 1135 25 COMPREHENSIVE MULTI-OMICS ANALYSIS REVEALS MITOCHONDRIAL STRESS AS A CENTRAL BIOLOGICAL HUB FOR SPACEFLIGHT IMPACT. SPACEFLIGHT IS KNOWN TO IMPOSE CHANGES ON HUMAN PHYSIOLOGY WITH UNKNOWN MOLECULAR ETIOLOGIES. TO REVEAL THESE CAUSES, WE USED A MULTI-OMICS, SYSTEMS BIOLOGY ANALYTICAL APPROACH USING BIOMEDICAL PROFILES FROM FIFTY-NINE ASTRONAUTS AND DATA FROM NASA'S GENELAB DERIVED FROM HUNDREDS OF SAMPLES FLOWN IN SPACE TO DETERMINE TRANSCRIPTOMIC, PROTEOMIC, METABOLOMIC, AND EPIGENETIC RESPONSES TO SPACEFLIGHT. OVERALL PATHWAY ANALYSES ON THE MULTI-OMICS DATASETS SHOWED SIGNIFICANT ENRICHMENT FOR MITOCHONDRIAL PROCESSES, AS WELL AS INNATE IMMUNITY, CHRONIC INFLAMMATION, CELL CYCLE, CIRCADIAN RHYTHM, AND OLFACTORY FUNCTIONS. IMPORTANTLY, NASA'S TWIN STUDY PROVIDED A PLATFORM TO CONFIRM SEVERAL OF OUR PRINCIPAL FINDINGS. EVIDENCE OF ALTERED MITOCHONDRIAL FUNCTION AND DNA DAMAGE WAS ALSO FOUND IN THE URINE AND BLOOD METABOLIC DATA COMPILED FROM THE ASTRONAUT COHORT AND NASA TWIN STUDY DATA, INDICATING MITOCHONDRIAL STRESS AS A CONSISTENT PHENOTYPE OF SPACEFLIGHT. 2020 5 683 32 BRAIN PLASTICITY AND COGNITIVE FUNCTIONS AFTER ETHANOL CONSUMPTION IN C57BL/6J MICE. ACUTE OR CHRONIC ADMINISTRATIONS OF HIGH DOSES OF ETHANOL IN MICE ARE KNOWN TO PRODUCE SEVERE COGNITIVE DEFICITS LINKED TO HIPPOCAMPAL DAMAGE. HOWEVER, WE RECENTLY REPORTED THAT CHRONIC AND MODERATE ETHANOL INTAKE IN C57BL/6J MICE INDUCED CHROMATIN REMODELING WITHIN THE BDNF PROMOTERS, LEADING TO BOTH ENHANCED BRAIN-DERIVED NEUROTROPHIC FACTOR (BDNF) EXPRESSION AND HIPPOCAMPAL NEUROGENESIS UNDER FREE-CHOICE PROTOCOL. WE PERFORMED HERE A SERIES OF CELLULAR AND BEHAVIORAL STUDIES TO ANALYZE THE CONSEQUENCES OF THESE MODIFICATIONS. WE SHOWED THAT A 3-WEEK CHRONIC FREE-CHOICE ETHANOL CONSUMPTION IN C57BL/6J MICE LED TO A DECREASE IN DNA METHYLATION OF THE BDNF GENE WITHIN THE CA1 AND CA3 SUBFIELDS OF THE HIPPOCAMPUS, AND UPREGULATED HIPPOCAMPAL BDNF SIGNALING PATHWAYS MEDIATED BY ERK, AKT AND CREB. HOWEVER, THIS ACTIVATION DID NOT AFFECT LONG-TERM POTENTIATION IN THE CA1. CONVERSELY, ETHANOL INTAKE IMPAIRED LEARNING AND MEMORY CAPACITIES ANALYZED IN THE CONTEXTUAL FEAR CONDITIONING TEST AND THE NOVEL OBJECT RECOGNITION TASK. IN ADDITION, ETHANOL INCREASED BEHAVIORAL PERSEVERATION IN THE BARNES MAZE TEST BUT DID NOT ALTER THE MOUSE OVERALL SPATIAL CAPACITIES. THESE DATA SUGGESTED THAT IN CONDITIONS OF CHRONIC AND MODERATE ETHANOL INTAKE, THE CHROMATIN REMODELING LEADING TO BDNF SIGNALING UPREGULATION IS PROBABLY AN ADAPTIVE PROCESS, ENGAGED VIA EPIGENETIC REGULATIONS, TO COUNTERACT THE COGNITIVE DEFICITS INDUCED BY ETHANOL. 2015 6 910 34 CHRONIC EXPOSURE TO ETHANOL OF MALE MICE BEFORE MATING PRODUCES ATTENTION DEFICIT HYPERACTIVITY DISORDER-LIKE PHENOTYPE ALONG WITH EPIGENETIC DYSREGULATION OF DOPAMINE TRANSPORTER EXPRESSION IN MOUSE OFFSPRING. PRECONCEPTION EXPOSURE TO ETOH THROUGH THE PATERNAL ROUTE MAY AFFECT NEUROBEHAVIORAL AND DEVELOPMENTAL FEATURES OF OFFSPRING. THIS STUDY INVESTIGATES THE EFFECTS OF PATERNAL EXPOSURE TO ETOH BEFORE CONCEPTION ON THE HYPERACTIVITY, INATTENTION, AND IMPULSIVITY BEHAVIOR OF MALE OFFSPRING IN MICE. SIRE MICE WERE TREATED WITH ETOH IN A CONCENTRATION RANGE APPROXIMATING HUMAN BINGE DRINKING (0-4 G/KG/DAY ETOH) FOR 7 WEEKS AND MATED WITH UNTREATED FEMALES MICE TO PRODUCE OFFSPRING. ETOH EXPOSURE TO SIRE MICE INDUCED ATTENTION DEFICIT HYPERACTIVITY DISORDER (ADHD)-LIKE HYPERACTIVE, INATTENTIVE, AND IMPULSIVE BEHAVIORS IN OFFSPRING. AS A MECHANISTIC LINK, BOTH PROTEIN AND MRNA EXPRESSION OF DOPAMINE TRANSPORTER (DAT), A KEY DETERMINANT OF ADHD-LIKE PHENOTYPES IN EXPERIMENTAL ANIMALS AND HUMANS, WERE SIGNIFICANTLY DECREASED BY PATERNAL ETOH EXPOSURE IN CEREBRAL CORTEX AND STRIATUM OF OFFSPRING MICE ALONG WITH INCREASED METHYLATION OF A CPG REGION OF THE DAT GENE PROMOTER. THE INCREASE IN METHYLATION OF DAT GENE PROMOTER WAS ALSO OBSERVED IN THE SPERM OF SIRE MICE, SUGGESTING GERMLINE CHANGES IN THE EPIGENETIC METHYLATION SIGNATURE OF DAT GENE BY ETOH EXPOSURE. IN ADDITION, THE EXPRESSION OF TWO KEY REGULATORS OF METHYLATION-DEPENDENT EPIGENETIC REGULATION OF FUNCTIONAL GENE EXPRESSION, NAMELY, MECP2 AND DNMT1, WAS MARKEDLY DECREASED IN OFFSPRING CORTEX AND STRIATUM SIRED BY ETOH-EXPOSED MICE. THESE RESULTS SUGGEST THAT PRECONCEPTIONAL EXPOSURE TO ETOH THROUGH THE PATERNAL ROUTE INDUCES BEHAVIORAL CHANGES IN OFFSPRING, POSSIBLY VIA EPIGENETIC CHANGES IN GENE EXPRESSION, WHICH IS ESSENTIAL FOR THE REGULATION OF ADHD-LIKE BEHAVIORS. 2014 7 5812 43 STRESS AND ANXIETY: STRUCTURAL PLASTICITY AND EPIGENETIC REGULATION AS A CONSEQUENCE OF STRESS. THE BRAIN IS THE CENTRAL ORGAN OF STRESS AND ADAPTATION TO STRESS BECAUSE IT PERCEIVES AND DETERMINES WHAT IS THREATENING, AS WELL AS THE BEHAVIORAL AND PHYSIOLOGICAL RESPONSES TO THE STRESSOR. THE ADULT, AS WELL AS DEVELOPING BRAIN, POSSESS A REMARKABLE ABILITY TO SHOW REVERSIBLE STRUCTURAL AND FUNCTIONAL PLASTICITY IN RESPONSE TO STRESSFUL AND OTHER EXPERIENCES, INCLUDING NEURONAL REPLACEMENT, DENDRITIC REMODELING, AND SYNAPSE TURNOVER. THIS IS PARTICULARLY EVIDENT IN THE HIPPOCAMPUS, WHERE ALL THREE TYPES OF STRUCTURAL PLASTICITY HAVE BEEN RECOGNIZED AND INVESTIGATED, USING A COMBINATION OF MORPHOLOGICAL, MOLECULAR, PHARMACOLOGICAL, ELECTROPHYSIOLOGICAL AND BEHAVIORAL APPROACHES. THE AMYGDALA AND THE PREFRONTAL CORTEX, BRAIN REGIONS INVOLVED IN ANXIETY AND FEAR, MOOD, COGNITIVE FUNCTION AND BEHAVIORAL CONTROL, ALSO SHOW STRUCTURAL PLASTICITY. ACUTE AND CHRONIC STRESS CAUSE AN IMBALANCE OF NEURAL CIRCUITRY SUBSERVING COGNITION, DECISION MAKING, ANXIETY AND MOOD THAT CAN INCREASE OR DECREASE EXPRESSION OF THOSE BEHAVIORS AND BEHAVIORAL STATES. IN THE SHORT TERM, SUCH AS FOR INCREASED FEARFUL VIGILANCE AND ANXIETY IN A THREATENING ENVIRONMENT, THESE CHANGES MAY BE ADAPTIVE; BUT, IF THE DANGER PASSES AND THE BEHAVIORAL STATE PERSISTS ALONG WITH THE CHANGES IN NEURAL CIRCUITRY, SUCH MALADAPTATION MAY NEED INTERVENTION WITH A COMBINATION OF PHARMACOLOGICAL AND BEHAVIORAL THERAPIES, AS IS THE CASE FOR CHRONIC OR MOOD ANXIETY DISORDERS. WE SHALL REVIEW CELLULAR AND MOLECULAR MECHANISMS, AS WELL AS RECENT WORK ON INDIVIDUAL DIFFERENCES IN ANXIETY-LIKE BEHAVIOR AND ALSO DEVELOPMENTAL INFLUENCES THAT BIAS HOW THE BRAIN RESPONDS TO STRESSORS. FINALLY, WE SUGGEST THAT SUCH AN APPROACH NEEDS TO BE EXTENDED TO OTHER BRAIN AREAS THAT ARE ALSO INVOLVED IN ANXIETY AND MOOD. THIS ARTICLE IS PART OF A SPECIAL ISSUE ENTITLED 'ANXIETY AND DEPRESSION'. 2012 8 4848 32 OPIOID-INDUCED STRUCTURAL AND FUNCTIONAL PLASTICITY OF MEDIUM-SPINY NEURONS IN THE NUCLEUS ACCUMBENS. OPIOID USE DISORDER (OUD) IS A CHRONIC RELAPSING CLINICAL CONDITION WITH TREMENDOUS MORBIDITY AND MORTALITY THAT FREQUENTLY PERSISTS, DESPITE TREATMENT, DUE TO AN INDIVIDUAL'S UNDERLYING PSYCHOLOGICAL, NEUROBIOLOGICAL, AND GENETIC VULNERABILITIES. EVIDENCE SUGGESTS THAT THESE VULNERABILITIES MAY HAVE NEUROCHEMICAL, CELLULAR, AND MOLECULAR BASES. KEY NEUROPLASTIC EVENTS WITHIN THE MESOCORTICOLIMBIC SYSTEM THAT EMERGE THROUGH CHRONIC EXPOSURE TO OPIOIDS MAY HAVE A DETERMINATIVE INFLUENCE ON BEHAVIORAL SYMPTOMS ASSOCIATED WITH OUD. IN PARTICULAR, STRUCTURAL AND FUNCTIONAL ALTERATIONS IN THE DENDRITIC SPINES OF MEDIUM SPINY NEURONS (MSNS) WITHIN THE NUCLEUS ACCUMBENS (NAC) AND ITS DOPAMINERGIC PROJECTIONS FROM THE VENTRAL TEGMENTAL AREA (VTA) ARE BELIEVED TO FACILITATE THESE BEHAVIORAL SEQUELAE. ADDITIONALLY, GLUTAMATERGIC NEURONS FROM THE PREFRONTAL CORTEX, THE BASOLATERAL AMYGDALA, THE HIPPOCAMPUS, AND THE THALAMUS PROJECT TO THESE SAME MSNS, PROVIDING AN ENRICHED TARGET FOR SYNAPTIC PLASTICITY. HERE, WE REVIEW LITERATURE RELATED TO NEUROADAPTATIONS IN NAC MSNS FROM DOPAMINERGIC AND GLUTAMATERGIC PATHWAYS IN OUD. WE ALSO DESCRIBE NEW FINDINGS RELATED TO TRANSCRIPTIONAL, EPIGENETIC, AND MOLECULAR MECHANISMS IN MSN PLASTICITY IN THE DIFFERENT STAGES OF OUD. 2021 9 3587 37 IMPACT OF TLR4 ON BEHAVIORAL AND COGNITIVE DYSFUNCTIONS ASSOCIATED WITH ALCOHOL-INDUCED NEUROINFLAMMATORY DAMAGE. TOLL-LIKE RECEPTORS (TLRS) PLAY AN IMPORTANT ROLE IN THE INNATE IMMUNE RESPONSE, AND EMERGING EVIDENCE INDICATES THEIR ROLE IN BRAIN INJURY AND NEURODEGENERATION. OUR RECENT RESULTS HAVE DEMONSTRATED THAT ETHANOL IS CAPABLE OF ACTIVATING GLIAL TLR4 RECEPTORS AND THAT THE ELIMINATION OF THESE RECEPTORS IN MICE PROTECTS AGAINST ETHANOL-INDUCED GLIAL ACTIVATION, INDUCTION OF INFLAMMATORY MEDIATORS AND APOPTOSIS. THIS STUDY WAS DESIGNED TO ASSESS WHETHER ETHANOL-INDUCED INFLAMMATORY DAMAGE CAUSES BEHAVIORAL AND COGNITIVE CONSEQUENCES, AND IF BEHAVIORAL ALTERATIONS ARE DEPENDENT OF TLR4 FUNCTIONS. HERE WE SHOW IN MICE DRINKING ALCOHOL FOR 5MONTHS, FOLLOWED BY A 15-DAY WITHDRAWAL PERIOD, THAT ACTIVATION OF THE ASTROGLIAL AND MICROGLIAL CELLS IN FRONTAL CORTEX AND STRIATUM IS MAINTAINED AND THAT THESE EVENTS ARE ASSOCIATED WITH COGNITIVE AND ANXIETY-RELATED BEHAVIORAL IMPAIRMENTS IN WILD-TYPE (WT) MICE, AS DEMONSTRATED BY TESTING THE ANIMALS WITH OBJECT MEMORY RECOGNITION, CONDITIONED TASTE AVERSION AND DARK AND LIGHT BOX ANXIETY TASKS. MICE LACKING TLR4 RECEPTORS ARE PROTECTED AGAINST ETHANOL-INDUCED INFLAMMATORY DAMAGE, AND BEHAVIORAL ASSOCIATED EFFECTS. WE FURTHER ASSESS THE POSSIBILITY OF THE EPIGENETIC MODIFICATIONS PARTICIPATING IN SHORT- OR LONG-TERM BEHAVIORAL EFFECTS ASSOCIATED WITH NEUROINFLAMMATORY DAMAGE. WE SHOW THAT CHRONIC ALCOHOL TREATMENT DECREASES H4 HISTONE ACETYLATION AND HISTONE ACETYLTRANSFERASES ACTIVITY IN FRONTAL CORTEX, STRIATUM AND HIPPOCAMPUS OF WT MICE. ALTERATIONS IN CHROMATIN STRUCTURE WERE NOT OBSERVED IN TLR4(-/-) MICE. THESE RESULTS PROVIDE THE FIRST EVIDENCE OF THE ROLE THAT TLR4 FUNCTIONS PLAY IN THE BEHAVIORAL CONSEQUENCES OF ALCOHOL-INDUCED INFLAMMATORY DAMAGE AND SUGGEST THAT THE EPIGENETIC MODIFICATIONS MEDIATED BY TLR4 COULD CONTRIBUTE TO SHORT- OR LONG-TERM ALCOHOL-INDUCED BEHAVIORAL OR COGNITIVE DYSFUNCTIONS. 2011 10 3970 37 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 11 4213 35 METHIONINE MEDIATES RESILIENCE TO CHRONIC SOCIAL DEFEAT STRESS BY EPIGENETIC REGULATION OF NMDA RECEPTOR SUBUNIT EXPRESSION. RATIONALE: PREVIOUS STUDIES SUGGESTED THAT METHIONINE (MET) LEVELS ARE DECREASED IN DEPRESSED PATIENTS. HOWEVER, WHETHER THE DECREASE IN THIS AMINO ACID IS IMPORTANT FOR PHENOTYPIC BEHAVIORS ASSOCIATED WITH DEPRESSION HAS NOT BEEN DECIPHERED. OBJECTIVE: THE RESPONSE OF INDIVIDUALS TO CHRONIC STRESS IS VARIABLE, WITH SOME INDIVIDUALS DEVELOPING DEPRESSION AND OTHERS BECOMING RESILIENT TO STRESS. IN THIS STUDY, OUR OBJECTIVE WAS TO EXAMINE THE EFFECT OF MET ON SUSCEPTIBILITY TO STRESS. METHODS: MALE C57BL/6J MICE WERE SUBJECTED TO DAILY DEFEAT SESSIONS BY A CD1 AGGRESSOR, FOR 10 DAYS. ON DAY 11, THE BEHAVIOR OF MICE WAS ASSESSED USING SOCIAL INTERACTION AND OPEN-FIELD TESTS. MICE RECEIVED MET 4 H BEFORE EACH DEFEAT SESSION. EPIGENETIC TARGETS WERE ASSESSED EITHER THROUGH REAL-RIME RTPCR OR THROUGH WESTERN BLOTS. RESULTS: MET DID NOT MODULATE ANXIETY-LIKE BEHAVIORS, BUT RATHER PROMOTED RESILIENCE TO CHRONIC STRESS, RESCUED SOCIAL AVOIDANCE BEHAVIORS AND REVERSED THE INCREASE IN THE CORTICAL EXPRESSION LEVELS OF N-METHYL-D-ASPARTATE RECEPTOR (NMDAR) SUBUNITS. ACTIVATING NMDAR ACTIVITY ABOLISHED THE ABILITY OF MET TO PROMOTE RESILIENCE TO STRESS AND TO RESCUE SOCIAL AVOIDANCE BEHAVIOR, WHEREAS INHIBITING NMDAR DID NOT SHOW ANY SYNERGISTIC OR ADDITIVE PROTECTIVE EFFECTS. INDEED, MET INCREASED THE CORTICAL LEVELS OF THE HISTONE METHYLTRANSFERASE SETDB1, AND IN TURN, THE LEVELS OF THE REPRESSIVE HISTONE H3 LYSINE (K9) TRIMETHYLATION (ME3). CONCLUSIONS: OUR DATA INDICATE THAT MET RESCUES SUSCEPTIBILITY TO STRESS BY INACTIVATING CORTICAL NMDAR ACTIVITY THROUGH AN EPIGENETIC MECHANISM INVOLVING HISTONE METHYLATION. 2020 12 4943 42 PATERNAL PRECONCEPTION ALCOHOL EXPOSURE IMPARTS INTERGENERATIONAL ALCOHOL-RELATED BEHAVIORS TO MALE OFFSPRING ON A PURE C57BL/6J BACKGROUND. WHILE ALCOHOL USE DISORDER (AUD) IS A HIGHLY HERITABLE CONDITION, THE BASIS OF AUD IN FAMILIES WITH A HISTORY OF ALCOHOLISM IS DIFFICULT TO EXPLAIN BY GENETIC VARIATION ALONE. EMERGING EVIDENCE SUGGESTS THAT PARENTAL EXPERIENCE PRIOR TO CONCEPTION CAN AFFECT INHERITANCE OF COMPLEX BEHAVIORS IN OFFSPRING VIA NON-GENOMIC (EPIGENETIC) MECHANISMS. FOR INSTANCE, MALE C57BL/6J (B6) MICE EXPOSED TO CHRONIC INTERMITTENT VAPOR ETHANOL (CIE) PRIOR TO MATING WITH STRAIN 129S1/SVIMJ ETHANOL-NAIVE FEMALES PRODUCE MALE OFFSPRING WITH REDUCED ETHANOL-DRINKING PREFERENCE, INCREASED ETHANOL SENSITIVITY, AND INCREASED BRAIN-DERIVED NEUROTROPHIC FACTOR (BDNF) EXPRESSION IN THE VENTRAL TEGMENTAL AREA (VTA). IN THE PRESENT STUDY, WE TESTED THE HYPOTHESIS THAT THESE INTERGENERATIONAL EFFECTS OF PATERNAL CIE ARE REPRODUCIBLE IN MALE OFFSPRING ON AN INBRED B6 BACKGROUND. TO THIS END, B6 MALES WERE EXPOSED TO 6 WEEKS OF CIE (OR ROOM AIR AS A CONTROL) BEFORE MATING WITH ETHANOL-NAIVE B6 FEMALES TO PRODUCE ETHANOL (E)-SIRED AND CONTROL (C)-SIRED MALE AND FEMALE OFFSPRING. WE OBSERVED A SEX-SPECIFIC EFFECT, AS E-SIRED MALES EXHIBITED DECREASED TWO-BOTTLE FREE-CHOICE ETHANOL-DRINKING PREFERENCE, INCREASED SENSITIVITY TO THE ANXIOLYTIC EFFECTS OF ETHANOL, AND INCREASED VTA BDNF EXPRESSION; NO DIFFERENCES WERE OBSERVED IN FEMALE OFFSPRING. THESE FINDINGS CONFIRM AND EXTEND OUR PREVIOUS RESULTS BY DEMONSTRATING THAT THE EFFECTS OF PATERNAL PRECONCEPTION ETHANOL ARE REPRODUCIBLE USING GENETICALLY IDENTICAL, INBRED B6 ANIMALS. 2017 13 5310 25 PSYCHOBIOLOGY AND MOLECULAR GENETICS OF RESILIENCE. EVERY INDIVIDUAL EXPERIENCES STRESSFUL LIFE EVENTS. IN SOME CASES ACUTE OR CHRONIC STRESS LEADS TO DEPRESSION AND OTHER PSYCHIATRIC DISORDERS, BUT MOST PEOPLE ARE RESILIENT TO SUCH EFFECTS. RECENT RESEARCH HAS BEGUN TO IDENTIFY THE ENVIRONMENTAL, GENETIC, EPIGENETIC AND NEURAL MECHANISMS THAT UNDERLIE RESILIENCE, AND HAS SHOWN THAT RESILIENCE IS MEDIATED BY ADAPTIVE CHANGES IN SEVERAL NEURAL CIRCUITS INVOLVING NUMEROUS NEUROTRANSMITTER AND MOLECULAR PATHWAYS. THESE CHANGES SHAPE THE FUNCTIONING OF THE NEURAL CIRCUITS THAT REGULATE REWARD, FEAR, EMOTION REACTIVITY AND SOCIAL BEHAVIOUR, WHICH TOGETHER ARE THOUGHT TO MEDIATE SUCCESSFUL COPING WITH STRESS. 2009 14 3977 36 LONG-TERM EFFECT OF POST-TRAUMATIC STRESS IN ADOLESCENCE ON DENDRITE DEVELOPMENT AND H3K9ME2/BDNF EXPRESSION IN MALE RAT HIPPOCAMPUS AND PREFRONTAL CORTEX. EXPOSURE TO A HARSH ENVIRONMENT IN EARLY LIFE INCREASES IN THE RISK OF POST-TRAUMATIC STRESS DISORDER (PTSD) OF AN INDIVIDUAL. BRAIN DERIVED NEUROTROPHIC FACTOR (BDNF) PLAYS AN IMPORTANT ROLE IN NEURODEVELOPMENT IN DEVELOPMENTAL STAGES. BOTH CHRONIC AND TRAUMATIC STRESSES INDUCE A DECREASE IN THE LEVEL OF BDNF AND REDUCE NEURAL PLASTICITY, WHICH IS LINKED TO THE PATHOGENESIS OF PTSD. ALSO, STUDIES HAVE SHOWN THAT STRESS ALTERS THE EPIGENETIC MARKER H3K9ME2, WHICH CAN BIND TO THE PROMOTER REGION OF THE BDNF GENE AND REDUCE BDNF PROTEIN LEVEL. HOWEVER, THE LONG-TERM EFFECTS OF TRAUMATIC STRESS DURING ADOLESCENCE ON H3K9ME2, BDNF EXPRESSION AND DENDRITE DEVELOPMENT ARE NOT WELL-KNOWN. THE PRESENT STUDY ESTABLISHED A MODEL OF PTSD IN ADOLESCENT RATS USING AN INESCAPABLE FOOT SHOCK (IFS) PROCEDURE. ANXIETY-LIKE BEHAVIORS, SOCIAL INTERACTION BEHAVIOR AND MEMORY FUNCTION WERE ASSESSED BY THE OPEN FIELD TEST, ELEVATED PLUS MAZE TEST, THREE-CHAMBER SOCIABILITY TEST AND MORRIS WATER MAZE TEST. IN ADDITION, NEURONAL DEVELOPMENT AND H3K9ME2/BDNF EXPRESSION IN HIPPOCAMPUS (HIP) AND PREFRONTAL CORTEX (PFC) WERE EVALUATED BY GOLGI STAINING, WESTERN BLOTTING, QRT-PCR ANALYSIS AND CHIP-QPCR ANALYSIS. ADDITIONALLY, THE UNC0642, A SMALL MOLECULE INHIBITOR OF HISTONE METHYLTRANSFERASE (EHMT2) WAS USED FOR INTERVENTION. THE RESULTS SHOWED THAT THE IFS PROCEDURE INDUCED THE PTSD-LIKE BEHAVIORS IN RATS, RESULTED IN FEWER DENDRITE BRANCHES AND SHORTER DENDRITE LENGTH IN CA1 OF HIP AND PFC, INCREASED H3K9ME2 LEVEL AND DECREASED BDNF EXPRESSION IN HIP AND PFC. ALSO, ALTHOUGH ALL THE CHANGES CAN PERSIST TO ADULTHOOD, UNC0642 ADMINISTRATION RELIEVED MOST OF ALTERATIONS. OUR STUDY SUGGESTS THAT TRAUMATIC STRESS IN ADOLESCENCE LEADS TO IMMEDIATE AND LONG-TERM MENTAL DISORDERS, NEURONAL MORPHOLOGICAL CHANGES, LOWER BDNF LEVEL AND INCREASED H3K9ME2 LEVEL IN THE HIP AND PFC, INDICATING THAT H3K9ME2/BDNF DYSFUNCTION PLAYS A KEY ROLE IN PATHOGENESIS OF PTSD. 2020 15 4944 33 PATERNAL PRECONCEPTION ETHANOL EXPOSURE BLUNTS HYPOTHALAMIC-PITUITARY-ADRENAL AXIS RESPONSIVITY AND STRESS-INDUCED EXCESSIVE FLUID INTAKE IN MALE MICE. A GROWING NUMBER OF ENVIRONMENTAL INSULTS HAVE BEEN SHOWN TO INDUCE EPIGENETIC EFFECTS THAT PERSIST ACROSS GENERATIONS. FOR INSTANCE, PATERNAL PRECONCEPTION EXPOSURES TO ETHANOL OR STRESS HAVE INDEPENDENTLY BEEN SHOWN TO EXERT SUCH INTERGENERATIONAL EFFECTS. SINCE ETHANOL EXPOSURE IS A PHYSIOLOGICAL STRESSOR THAT ACTIVATES THE HYPOTHALAMIC-PITUITARY-ADRENAL (HPA) AXIS, WE HYPOTHESIZED THAT PATERNAL ETHANOL EXPOSURE WOULD IMPACT STRESS RESPONSIVITY OF OFFSPRING. ADULT MALE MICE WERE EXPOSED TO CHRONIC INTERMITTENT VAPOR ETHANOL OR CONTROL CONDITIONS FOR 5 WEEKS BEFORE BEING MATED WITH ETHANOL-NAIVE FEMALES TO PRODUCE ETHANOL (E)- AND CONTROL (C)-SIRED OFFSPRING. ADULT MALE AND FEMALE OFFSPRING WERE TESTED FOR PLASMA CORTICOSTERONE (CORT) LEVELS FOLLOWING ACUTE RESTRAINT STRESS AND THE MALE OFFSPRING WERE FURTHER EXAMINED FOR STRESS-EVOKED 2-BOTTLE CHOICE ETHANOL-DRINKING. PATERNAL ETHANOL EXPOSURE BLUNTED PLASMA CORT LEVELS FOLLOWING ACUTE RESTRAINT STRESS SELECTIVELY IN MALE OFFSPRING; FEMALES WERE UNAFFECTED. IN A STRESS-EVOKED ETHANOL-DRINKING ASSAY, THERE WAS NO EFFECT OF STRESS ON ETHANOL CONSUMPTION. HOWEVER, C-SIRED MALES EXHIBITED INCREASED TOTAL FLUID INTAKE (POLYDIPSIA) IN RESPONSE TO STRESS WHILE E-SIRED MALES WERE RESISTANT TO THIS STRESS-INDUCED PHENOTYPE. TAKEN TOGETHER, THESE DATA SUGGEST THAT PATERNAL ETHANOL EXPOSURE IMPARTS STRESS HYPORESPONSIVITY TO MALE OFFSPRING. 2016 16 1091 29 COGNITIVE ENHANCERS AS A TREATMENT FOR HEROIN RELAPSE AND ADDICTION. HEROIN ADDICTION IS A DISORDER THAT STEMS FROM MALADAPTIVE PLASTICITY WITHIN NEURAL CIRCUITS AND PRODUCES BROAD COGNITIVE DEFICITS. DESPITE CONSIDERABLE ADVANCES IN PSYCHOTHERAPY AND PHARMACOTHERAPY FOR HEROIN RELAPSE AND ADDICTION, EFFECTIVE TREATMENTS FOR HEROIN USE DISORDER ARE STILL LACKING. INCREASING PRECLINICAL EVIDENCE INDICATES THAT HEROIN SEEKING BEHAVIOR IS PERSISTENT AFTER WITHDRAWAL, WHILE COGNITIVE DYSFUNCTIONS ASSOCIATED WITH CHRONIC HEROIN USE ARE AN IMPORTANT CONTRIBUTING FACTOR TO RISK OF HEROIN RELAPSE AND ADDICTION. COGNITIVE ENHANCERS MAY BE USED TO STIMULATE TREATMENT SUCCESS AND ENHANCE TREATMENT EFFICACY. THE PURPOSE OF THIS REVIEW IS TO OUTLINE THE LITERATURE THAT DEMONSTRATES THE COGNITIVE DEFICITS DURING THE DEVELOPMENT OF HEROIN ADDICTION AND WITHDRAWAL PROCESS, AND SEVERAL FACTORS THAT UNDERLINE THE EFFICACY OF COGNITIVE ENHANCERS FOR HEROIN USE DISORDERS. THE REVIEW, THEN, EXAMINES THE POTENTIAL USE AND PHARMACOLOGICAL MECHANISMS OF COGNITIVE ENHANCERS THAT ACT ON CHOLINERGIC, GLUTAMATERGIC, DOPAMINERGIC OR ADRENERGIC PATHWAYS. IT ALSO EXAMINES THE EFFECTS OF COMPOUNDS THAT ALTER CREB SIGNALING AND EPIGENETIC MECHANISMS IN ANIMAL MODEL OF HEROIN RELAPSE. THE CURRENT BODY OF RESEARCH REVEALS THE NEW INSIGHTS INTO THE PHARMACOLOGICAL MECHANISMS UNDERLYING HEROIN ADDICTION AND HOLDS A SIGNIFICANT PROMISE FOR COGNITIVE ENHANCERS AS AN IMPROVED APPROACH TO TREAT HEROIN USE DISORDER IN A MORE EFFICIENT AND PERSISTENT WAY. 2019 17 1460 35 DISORDERS OF CONSCIOUSNESS AND PHARMACEUTICALS THAT ACT ON OXYGEN BASED AMINO ACID AND MONOAMINE NEUROTRANSMITTER PATHWAYS OF THE BRAIN. OXYGEN BASED NEUROTRANSMITTERS IN THE SYNAPSES OF THE BRAIN ARE PROPOSED TO PLAY AN IMPORTANT ROLE IN THE GENERATION OF CONSCIOUSNESS. THEY INCLUDE THE AMINO ACIDS GLUTAMATE AND GABA WHICH USE KREBS CYCLE PRECURSORS FOR THEIR SYNTHESIS, AND THE MONOAMINES DOPAMINE, NORADRENALIN, ADRENALIN AND SEROTONIN, WHICH ARE DERIVED FROM TYROSINE AND TRYPTOPHAN. DURING ISCHEMIA AFTER AN ACUTE BRAIN INJURY, A GABA SURGE OFTEN INITIATES BRAIN SUPPRESSION. IT HAS BEEN PROPOSED THAT WITH CHRONIC ISCHEMIA, A SECONDARY, POSSIBLY EPIGENETIC RESPONSE OCCURS WHEN NEUROTRANSMITTERS DEPLETE, A GLUCOSE AND OXYGEN SAVING MECHANISM TERMED NEURODORMANCY THAT MAY INVOKE ALTERNATIVE LONG TERM LOW ENERGY METABOLIC PATHWAYS IN THE BRAIN, ENCOUNTERED IN DISORDERS OF CONSCIOUSNESS. SOME MEDICATIONS CAN REVERSE DISORDERS OF CONSCIOUSNESS IN SOME PATIENTS. VIRTUALLY ALL OF THEM ACT ON NEUROTRANSMITTER SYSTEMS THAT USE OXYGEN AS A BUILDING BLOCK OR AS AN ENERGY SOURCE WITHIN THE BRAIN. PHARMACEUTICALS THAT ACT IN THE OXYGEN BASED AMINO ACID SYSTEMS OF THE BRAIN INCLUDE THE GABAERGIC MEDICATIONS ZOLPIDEM AND BACLOFEN, WHILE THOSE THAT ACT IN THE MONOAMINE AXES INCLUDE THE DOPAMINERGIC MEDICATIONS L DOPA, AMANTADINE, BROMOCRIPTINE, APOMORPHINE AND METHYLPHENIDATE, AND THE NORADRENERGIC AND SEROTONERGIC MEDICATIONS DESIPRAMINE, AMITRIPTYLINE, PROTRIPTYLINE AND FLUOXETINE. ANOTHER GROUP ARE THE CHOLINESTERASE INHIBITORS, RESPONSIBLE FOR INCREASING ACETYLCHOLINE, WHICH IS SYNTHESIZED FROM THE KREBS CYCLE INITIATOR, ACETYL COA. IT APPEARS THAT PHARMACEUTICALS THAT ARE ACTIVE IN THE OXYGEN BASED NEUROTRANSMITTER PATHWAYS OF THE BRAIN ARE SUCCESSFUL TO AROUSE TO CONSCIOUSNESS PATIENTS THAT SUFFER FROM ITS DISORDERS. RESEARCH NEEDS TO BE SUPPORTED AS FOUNDATION TO UNDERSTAND THE BIOCHEMICAL MECHANISMS THAT ARE INVOLVED IN CONSCIOUSNESS DISORDERS AND TO EXPLORE FURTHER THE PHARMACOLOGICAL TREATMENT POSSIBILITIES FOR THESE DEVASTATING NEUROLOGICAL CONDITIONS. 2014 18 23 36 60 YEARS OF NEUROENDOCRINOLOGY: REDEFINING NEUROENDOCRINOLOGY: STRESS, SEX AND COGNITIVE AND EMOTIONAL REGULATION. THE DISCOVERY OF STEROID HORMONE RECEPTORS IN BRAIN REGIONS THAT MEDIATE EVERY ASPECT OF BRAIN FUNCTION HAS BROADENED THE DEFINITION OF 'NEUROENDOCRINOLOGY' TO INCLUDE THE RECIPROCAL COMMUNICATION BETWEEN THE BRAIN AND THE BODY VIA HORMONAL AND NEURAL PATHWAYS. THE BRAIN IS THE CENTRAL ORGAN OF STRESS AND ADAPTATION TO STRESS BECAUSE IT PERCEIVES AND DETERMINES WHAT IS THREATENING, AS WELL AS THE BEHAVIORAL AND PHYSIOLOGICAL RESPONSES TO THE STRESSOR. THE ADULT AND DEVELOPING BRAIN POSSESS REMARKABLE STRUCTURAL AND FUNCTIONAL PLASTICITY IN RESPONSE TO STRESS, INCLUDING NEURONAL REPLACEMENT, DENDRITIC REMODELING, AND SYNAPSE TURNOVER. STRESS CAUSES AN IMBALANCE OF NEURAL CIRCUITRY SUBSERVING COGNITION, DECISION-MAKING, ANXIETY AND MOOD THAT CAN ALTER EXPRESSION OF THOSE BEHAVIORS AND BEHAVIORAL STATES. THIS IMBALANCE, IN TURN, AFFECTS SYSTEMIC PHYSIOLOGY VIA NEUROENDOCRINE, AUTONOMIC, IMMUNE AND METABOLIC MEDIATORS. IN THE SHORT TERM, AS FOR INCREASED FEARFUL VIGILANCE AND ANXIETY IN A THREATENING ENVIRONMENT, THESE CHANGES MAY BE ADAPTIVE. BUT, IF THE DANGER PASSES AND THE BEHAVIORAL STATE PERSISTS ALONG WITH THE CHANGES IN NEURAL CIRCUITRY, SUCH MALADAPTATION MAY NEED INTERVENTION WITH A COMBINATION OF PHARMACOLOGICAL AND BEHAVIORAL THERAPIES, AS IS THE CASE FOR CHRONIC ANXIETY AND DEPRESSION. THERE ARE IMPORTANT SEX DIFFERENCES IN THE BRAIN RESPONSES TO STRESSORS THAT ARE IN URGENT NEED OF FURTHER EXPLORATION. MOREOVER, ADVERSE EARLY-LIFE EXPERIENCE, INTERACTING WITH ALLELES OF CERTAIN GENES, PRODUCE LASTING EFFECTS ON BRAIN AND BODY OVER THE LIFE-COURSE VIA EPIGENETIC MECHANISMS. WHILE PREVENTION IS MOST IMPORTANT, THE PLASTICITY OF THE BRAIN GIVES HOPE FOR THERAPIES THAT TAKE INTO CONSIDERATION BRAIN-BODY INTERACTIONS. 2015 19 1803 15 EFFECT OF PROLONGED EMOTIONAL AND PAIN STRESS ON THE CONTENT OF METHYLCYTOSINE-BINDING PROTEIN MECP2 IN NUCLEI OF HIPPOCAMPAL NEURONS IN RATS WITH DIFFERENT EXCITABILITY OF THE NERVOUS SYSTEM. IN RATS WITH LOW EXCITABILITY THRESHOLD OF THE NERVOUS SYSTEM DEMONSTRATING SIGNIFICANT AND PERSISTENT BEHAVIORAL DISORDERS UNDER STRESS CONDITIONS, THE CONTENT OF METHYLCYTOSINE-BINDING PROTEIN MECP2 IN NEURONAL NUCLEI OF HIPPOCAMPAL FIELD CA3 DECREASED OVER 2 WEEKS AFTER LONG-TERM EMOTIONAL AND PAIN STRESS. IT WAS HYPOTHESIZED THAT PROTEIN MECP2 TRIGGERS EPIGENETIC CHANGES IN DNA THAT UNDERLIE "STRESS MEMORY". 2006 20 881 28 CHRONIC CLOZAPINE TREATMENT RESTRAINS VIA HDAC2 THE PERFORMANCE OF MGLU2 RECEPTOR AGONISM IN A RODENT MODEL OF ANTIPSYCHOTIC ACTIVITY. PRECLINICAL FINDINGS IN RODENT MODELS POINTED TOWARD ACTIVATION OF METABOTROPIC GLUTAMATE 2/3 (MGLU2/3) RECEPTORS AS A NEW PHARMACOLOGICAL APPROACH TO TREAT PSYCHOSIS. HOWEVER, MORE RECENT STUDIES FAILED TO SHOW CLINICAL EFFICACY OF MGLU2/3 RECEPTOR AGONISM IN SCHIZOPHRENIA PATIENTS. WE PREVIOUSLY PROPOSED THAT LONG-TERM ANTIPSYCHOTIC MEDICATION RESTRICTED THE THERAPEUTIC EFFECTS OF THESE GLUTAMATERGIC AGENTS. HOWEVER, LITTLE IS KNOWN ABOUT THE MOLECULAR MECHANISM UNDERLYING THE POTENTIAL REPERCUSSION OF PREVIOUS ANTIPSYCHOTIC EXPOSURE ON THE THERAPEUTIC PERFORMANCE OF MGLU2/3 RECEPTOR AGONISTS. HERE WE SHOW THAT THIS MALADAPTIVE EFFECT OF ANTIPSYCHOTIC TREATMENT IS MEDIATED MOSTLY VIA HISTONE DEACETYLASE 2 (HDAC2). CHRONIC TREATMENT WITH THE ANTIPSYCHOTIC CLOZAPINE LED TO A DECREASE IN MOUSE FRONTAL CORTEX MGLU2 MRNA, AN EFFECT THAT REQUIRED EXPRESSION OF BOTH HDAC2 AND THE SEROTONIN 5-HT(2A) RECEPTOR. THIS TRANSCRIPTIONAL ALTERATION OCCURRED IN ASSOCIATION WITH HDAC2-DEPENDENT REPRESSIVE HISTONE MODIFICATIONS AT THE MGLU2 PROMOTER. WE FOUND THAT CHRONIC CLOZAPINE TREATMENT DECREASED VIA HDAC2 THE CAPABILITIES OF THE MGLU2/3 RECEPTOR AGONIST LY379268 TO ACTIVATE G-PROTEINS IN THE FRONTAL CORTEX OF MICE. CHRONIC CLOZAPINE TREATMENT BLUNTED THE ANTIPSYCHOTIC-RELATED BEHAVIORAL EFFECTS OF LY379268, AN EFFECT THAT WAS NOT OBSERVED IN HDAC2 KNOCKOUT MICE. MORE IMPORTANTLY, CO-ADMINISTRATION OF THE CLASS I AND II HDAC INHIBITOR SAHA (VORINOSTAT) PRESERVED THE ANTIPSYCHOTIC PROFILE OF LY379268 AND FRONTAL CORTEX MGLU2/3 RECEPTOR DENSITY IN WILD-TYPE MICE. THESE FINDINGS RAISE CONCERNS ON THE DESIGN OF PREVIOUS CLINICAL STUDIES WITH MGLU2/3 AGONISTS, PROVIDING THE RATIONALE FOR THE DEVELOPMENT OF HDAC2 INHIBITORS AS A NEW EPIGENETIC-BASED APPROACH TO IMPROVE THE CURRENTLY LIMITED RESPONSE TO TREATMENT WITH GLUTAMATERGIC ANTIPSYCHOTICS. 2019