1 6583 132 TRICLOSAN INDUCES ZEBRAFISH NEUROTOXICITY BY ABNORMAL EXPRESSION OF MIR-219 TARGETING OLIGODENDROCYTE DIFFERENTIATION OF CENTRAL NERVOUS SYSTEM. TRICLOSAN (TCS) IS UBIQUITOUS IN A WIDE RANGE OF PERSONAL CARE AND CONSUMER PRODUCTS, AND IT IS ACUTE/CHRONIC EXPOSURE MAY RESULT IN SEVERAL NERVOUS SYSTEM DISORDERS. PREVIOUS STUDIES DEMONSTRATED TCS-INDUCED ABNORMAL EXPRESSION OF MIRNAS, BUT NO INVESTIGATIONS FOCUSED ON UPSTREAM CHANGES OF MIRNAS AND ASSOCIATED MOLECULAR MECHANISMS. HEREIN, PHENOTYPE OBSERVATION AND BEHAVIORAL ANALYSIS CONFIRMED THAT TCS EXPOSURE (0, 62.5, 125, 250 MUG/L) LED TO DEVELOPMENTAL NEUROTOXICITY IN ZEBRAFISH LARVAE, ESPECIALLY FOR OLIGODENDROCYTE PRECURSOR CELLS (OPCS). HIGH-THROUGHPUT SEQUENCING DEMONSTRATED THE CRITICAL ROLE OF MIR-219 IN THE DIFFERENTIATION OF OPCS. LARVAE WITH MIR-219 DEPLETION SHOWED THE SAME PHENOTYPE CAUSED BY TCS. FUNCTIONAL TESTS WITH MIR-219 KNOCK-DOWN AND OVER-EXPRESSION SHOWED THAT MIR-219 PROMOTED DIFFERENTIATION OF OPCS BY ACTING ON MYELINATION INHIBITORS. THE MIR-219 ALSO PROTECTED AGAINST TCS-INDUCED INHIBITION OF CELL DIFFERENTIATION. SEVERAL EPIGENETIC FEATURES WERE IDENTIFIED TO REVEAL POTENTIAL UPSTREAM REGULATORY MECHANISMS OF MIR-219. IN PARTICULAR, FIVE CPG ISLANDS HYPER-METHYLATED WITH INCREASING TCS CONCENTRATIONS IN THE PROMOTER REGION OF MIR-219. TCS INHIBITED OPC DIFFERENTIATION BY INFLUENCING EPIGENETIC EFFECTS ON MIR-219-RELATED PATHWAYS, CONTRIBUTING TO SEVERE NEUROTOXICITY. THESE FINDINGS ENHANCE OUR UNDERSTANDING OF EPIGENETIC MECHANISMS AFFECTING DEMYELINATION DISEASES DUE TO TCS EXPOSURE, AND ALSO PROVIDE THEORETICAL GUIDANCE FOR EARLY INTERVENTION AND GENE THERAPY OF ENVIRONMENTALLY INDUCED DISEASES. 2020 2 5087 23 PIMECROLIMUS FOR THE TREATMENT OF ATOPIC DERMATITIS IN INFANTS: AN ASIAN PERSPECTIVE. ATOPIC DERMATITIS (AD) IS A COMMON CHRONIC, MULTISYSTEM INFLAMMATORY SKIN DISEASE IN PEDIATRIC PATIENTS. THERE HAS BEEN AN INCREASE IN THE INCIDENCE OF AD IN THE PEDIATRIC POPULATION OF THE ASIA-PACIFIC REGION. STUDIES HAVE SHOWN THAT GENETIC, EPIGENETIC, ENVIRONMENTAL AND CULTURAL FACTORS MAY LEAD TO DIFFERENCES IN THE CLINICAL MANIFESTATION AND PREVALENCE OF AD BETWEEN RACES. EARLY TREATMENT OF AD IS NECESSARY TO PREVENT THE ATOPIC MARCH LEADING TO COMORBIDITIES SUCH AS ASTHMA AND ALLERGIC RHINITIS. TOPICAL CORTICOSTEROIDS (TCS) ARE USED AS FIRST-LINE THERAPY FOR THE TREATMENT OF AD, BUT THEIR LONG-TERM USAGE POSES A RISK TO THE PATIENT'S HEALTH. PIMECROLIMUS (1%) IS A TOPICAL CALCINEURIN INHIBITOR (TCI) THAT IS INDICATED FOR THE TREATMENT OF MILD TO MODERATE AD. PIMECROLIMUS HAS NO APPARENT INCREASE IN ADVERSE EVENTS COMPARED TO TCS, AND IT CAUSES LESS OF A BURNING SENSATION THAN TACROLIMUS. THE SAFETY AND EFFICACY OF PIMECROLIMUS HAS BEEN ESTABLISHED THROUGH VARIOUS CLINICAL TRIALS; YET, IN MANY ASIAN COUNTRIES, THE USE OF PIMECROLIMUS IN INFANTS IS STILL RESTRICTED DUE TO SAFETY CONCERNS. BASED ON THE AVAILABLE EVIDENCE, THE EXPERT PANEL RECOMMENDS PIMECROLIMUS IN INFANTS BETWEEN 3 MONTHS AND 2 YEARS OF AGE IN THE ASIAN POPULATION. 2023 3 429 20 ANTI-INFLAMMATORY TOPICAL MEDICATION - NEW DEVELOPMENTS IN THE TREATMENT OF ATOPIC DERMATITIS. ATOPIC DERMATITIS IS A CHRONIC INFLAMMATORY DISEASE THAT ARISES FROM POLYGENIC DISPOSITION, A DYSFUNCTION OF THE PHYSICOCHEMICAL EPITHELIAL BARRIER, A CUTANEOUS DYSBIOSIS, AND A FAULTY NEUROSENSORY ACTIVITY AND SHOWS A HIGHLY INDIVIDUAL ACUITY DUE TO EPIGENETIC FACTORS. AN ESSENTIAL COMPONENT OF THERAPEUTIC MANAGEMENT IS THE APPLICATION OF ANTI-INFLAMMATORY TOPICAL MEDICATION. CURRENTLY, TOPICAL GLUCOCORTICOIDS AND TOPICAL CALCINEURIN INHIBITORS ARE ROUTINELY USED IN REACTIVE AND PROACTIVE THERAPY. IN RECENT YEARS, THE DEVELOPMENT OF MOLECULAR MEDICINE HAS IDENTIFIED SEVERAL NEW THERAPEUTIC TARGETS THAT HAVE ENABLED THE DEVELOPMENT OF INNOVATIVE THERAPEUTIC APPROACHES. IN ADDITION TO PHOSPHODIESTERASE-4 INHIBITORS AND ARYL HYDROCARBON RECEPTOR MODULATORS, IT IS MAINLY JANUS KINASE INHIBITORS WITH DIFFERENT SELECTIVITY THAT ARE EMERGING AS NEW EFFECTIVE AND SAFE OPTIONS FOR TOPICAL THERAPY. THE CURRENT DATA SUGGESTS THAT IN THE COMING MONTHS AND YEARS REPRESENTATIVES OF THE ABOVE-MENTIONED SUBSTANCE CLASSES WILL BE APPROVED FOR TOPICAL USE. 2021 4 2856 32 FROM METHYLATION TO MYELINATION: EPIGENOMIC AND TRANSCRIPTOMIC PROFILING OF CHRONIC INACTIVE DEMYELINATED MULTIPLE SCLEROSIS LESIONS. IN THE PROGRESSIVE PHASE OF MULTIPLE SCLEROSIS (MS), THE HAMPERED DIFFERENTIATION CAPACITY OF OLIGODENDROCYTE PRECURSOR CELLS (OPCS) EVENTUALLY RESULTS IN REMYELINATION FAILURE. WE HAVE PREVIOUSLY SHOWN THAT DNA METHYLATION OF ID2/ID4 IS HIGHLY INVOLVED IN OPC DIFFERENTIATION AND REMYELINATION. IN THIS STUDY, WE TOOK AN UNBIASED APPROACH BY DETERMINING GENOME-WIDE DNA METHYLATION PATTERNS WITHIN CHRONICALLY DEMYELINATED MS LESIONS AND INVESTIGATED HOW CERTAIN EPIGENETIC SIGNATURES RELATE TO OPC DIFFERENTIATION CAPACITY. WE COMPARED GENOME-WIDE DNA METHYLATION AND TRANSCRIPTIONAL PROFILES BETWEEN CHRONICALLY DEMYELINATED MS LESIONS AND MATCHED NORMAL-APPEARING WHITE MATTER (NAWM), MAKING USE OF POST-MORTEM BRAIN TISSUE (N = 9/GROUP). DNA METHYLATION DIFFERENCES THAT INVERSELY CORRELATED WITH MRNA EXPRESSION OF THEIR CORRESPONDING GENES WERE VALIDATED FOR THEIR CELL-TYPE SPECIFICITY IN LASER-CAPTURED OPCS USING PYROSEQUENCING. THE CRISPR-DCAS9-DNMT3A/TET1 SYSTEM WAS USED TO EPIGENETICALLY EDIT HUMAN-IPSC-DERIVED OLIGODENDROCYTES TO ASSESS THE EFFECT ON CELLULAR DIFFERENTIATION. OUR DATA SHOW HYPERMETHYLATION OF CPGS WITHIN GENES THAT CLUSTER IN GENE ONTOLOGIES RELATED TO MYELINATION AND AXON ENSHEATHMENT. CELL TYPE-SPECIFIC VALIDATION INDICATES A REGION-DEPENDENT HYPERMETHYLATION OF MBP, ENCODING FOR MYELIN BASIC PROTEIN, IN OPCS OBTAINED FROM WHITE MATTER LESIONS COMPARED TO NAWM-DERIVED OPCS. BY ALTERING THE DNA METHYLATION STATE OF SPECIFIC CPGS WITHIN THE PROMOTOR REGION OF MBP, USING EPIGENETIC EDITING, WE SHOW THAT CELLULAR DIFFERENTIATION AND MYELINATION CAN BE BIDIRECTIONALLY MANIPULATED USING THE CRISPR-DCAS9-DNMT3A/TET1 SYSTEM IN VITRO. OUR DATA INDICATE THAT OPCS WITHIN CHRONICALLY DEMYELINATED MS LESIONS ACQUIRE AN INHIBITORY PHENOTYPE, WHICH TRANSLATES INTO HYPERMETHYLATION OF CRUCIAL MYELINATION-RELATED GENES. ALTERING THE EPIGENETIC STATUS OF MBP CAN RESTORE THE DIFFERENTIATION CAPACITY OF OPCS AND POSSIBLY BOOST (RE)MYELINATION. 2023 5 363 31 AMBIENT AIR POLLUTION: HEALTH HAZARDS TO CHILDREN. AMBIENT AIR POLLUTION IS PRODUCED BY SOURCES INCLUDING VEHICULAR TRAFFIC, COAL-FIRED POWER PLANTS, HYDRAULIC FRACTURING, AGRICULTURAL PRODUCTION, AND FOREST FIRES. IT CONSISTS OF PRIMARY POLLUTANTS GENERATED BY COMBUSTION AND SECONDARY POLLUTANTS FORMED IN THE ATMOSPHERE FROM PRECURSOR GASES. AIR POLLUTION CAUSES AND EXACERBATES CLIMATE CHANGE, AND CLIMATE CHANGE WORSENS HEALTH EFFECTS OF AIR POLLUTION. INFANTS AND CHILDREN ARE UNIQUELY SENSITIVE TO AIR POLLUTION, BECAUSE THEIR ORGANS ARE DEVELOPING AND THEY HAVE HIGHER AIR PER BODY WEIGHT INTAKE. HEALTH EFFECTS LINKED TO AIR POLLUTION INCLUDE NOT ONLY EXACERBATIONS OF RESPIRATORY DISEASES BUT ALSO REDUCED LUNG FUNCTION DEVELOPMENT AND INCREASED ASTHMA INCIDENCE. ADDITIONAL OUTCOMES OF CONCERN INCLUDE PRETERM BIRTH, LOW BIRTH WEIGHT, NEURODEVELOPMENTAL DISORDERS, IQ LOSS, PEDIATRIC CANCERS, AND INCREASED RISKS FOR ADULT CHRONIC DISEASES. THESE EFFECTS ARE MEDIATED BY OXIDATIVE STRESS, CHRONIC INFLAMMATION, ENDOCRINE DISRUPTION, AND GENETIC AND EPIGENETIC MECHANISMS ACROSS THE LIFE SPAN. NATURAL EXPERIMENTS DEMONSTRATE THAT WITH INITIATIVES SUCH AS INCREASED USE OF PUBLIC TRANSPORTATION, BOTH AIR QUALITY AND COMMUNITY HEALTH IMPROVE. SIMILARLY, THE CLEAN AIR ACT HAS IMPROVED AIR QUALITY, ALTHOUGH EXPOSURE INEQUITIES PERSIST. OTHER EFFECTIVE STRATEGIES FOR REDUCING AIR POLLUTION INCLUDE ENDING RELIANCE ON COAL, OIL, AND GAS; REGULATING INDUSTRIAL EMISSIONS; REDUCING EXPOSURE WITH ATTENTION TO PROXIMITY OF RESIDENCES, SCHOOLS, AND CHILD CARE FACILITIES TO TRAFFIC; AND A GREATER AWARENESS OF THE AIR QUALITY INDEX. THIS POLICY REVIEWS BOTH SHORT- AND LONG-TERM HEALTH CONSEQUENCES OF AMBIENT AIR POLLUTION, ESPECIALLY IN RELATION TO DEVELOPMENTAL EXPOSURES. IT EXAMINES INDIVIDUAL, COMMUNITY, AND LEGISLATIVE STRATEGIES TO MITIGATE AIR POLLUTION. 2021 6 1226 28 CRITICAL ROLE OF GUT MICROBIOTA AND EPIGENETIC FACTORS IN THE PATHOGENESIS OF BEHCET'S DISEASE. BEHCET'S DISEASE (BD) IS A CHRONIC REFRACTORY MULTISYSTEM AUTOINFLAMMATORY DISEASE, CHARACTERIZED BY TYPICAL CLINICAL FEATURES OF NON-SPECIFIC VASCULITIS, ORAL AND GENITAL ULCERS, UVEITIS, AS WELL AS SKIN LESIONS. THE EXACT ETIOPATHOGENESIS OF BD REMAINS UNKNOWN, EXISTING STUDIES HAVE INDICATED THAT GENETICS AND ENVIRONMENTAL FACTORS CONTRIBUTE TO THE INCREASED DEVELOPMENT OF BD. RECENTLY, SEVERAL STUDIES HAVE SHOWN THAT EXTERNAL ENVIRONMENTAL FACTORS CAN AFFECT THE PROCESS OF EPIGENETIC MODIFICATION, AND ABNORMALITIES OF EPIGENETIC FACTORS HAVE BEEN CONFIRMED TO BE INVOLVED IN THE OCCURRENCE OF BD. AT THE SAME TIME, ABNORMALITIES OF GUT MICROBIOTA (GM) IN THE BODY, HAVE ALSO BEEN CONFIRMED TO PARTICIPATE IN THE PATHOGENESIS OF BD BY REGULATING THE BALANCE OF TH17/TREGS. THIS ARTICLE REVIEWS THE PATHOGENESIS OF BD AND SUMMARIZES NUMEROUS CLINICAL STUDIES, FOCUSING ON THE MECHANISM OF GM AND EPIGENETIC FACTORS IMPACTING ON BD, AND PROVIDING NEW IDEAS FOR FURTHER ELUCIDATING THE PATHOGENESIS OF BD. 2021 7 1205 39 COULD THE INHIBITOR OF DNA BINDING 2 AND 4 PLAY A ROLE IN WHITE MATTER INJURY? WHITE MATTER INJURY (WMI) PREVENTS THE NORMAL DEVELOPMENT OF MYELINATION, LEADING TO CENTRAL NERVOUS SYSTEM MYELINATION DISORDERS AND THE PRODUCTION OF CHRONIC SEQUELAE ASSOCIATED WITH WMI, SUCH AS CHRONIC DYSKINESIA, COGNITIVE IMPAIRMENT AND CEREBRAL PALSY. THIS RESULTS IN A LARGE EMOTIONAL AND SOCIOECONOMIC BURDEN. DECREASED MYELINATION IN PRETERM INFANT WMI IS ASSOCIATED WITH THE DELAYED DEVELOPMENT OR DESTRUCTION OF OLIGODENDROCYTE (OL) LINEAGE CELLS, PARTICULARLY OLIGODENDROCYTE PRECURSOR CELLS (OPCS). THE DEVELOPMENT OF CELLS FROM THE OL LINEAGE INVOLVES THE MIGRATION, PROLIFERATION AND DIFFERENT STAGES OF OL DIFFERENTIATION, FINALLY LEADING TO MYELINATION. A SERIES OF COMPLEX INTRINSIC, EXTRINSIC AND EPIGENETIC FACTORS REGULATE THE OPC CELL CYCLE WITHDRAWAL, OL LINEAGE PROGRESSION AND MYELINATION. WE FOCUS ON THE INHIBITOR OF DNA BINDING 2 (ID2), BECAUSE IT IS WIDELY INVOLVED IN THE DIFFERENT STAGES OF OL DIFFERENTIATION AND GENESIS. ID2 IS A KEY TRANSCRIPTION FACTOR FOR THE NORMAL DEVELOPMENT OF OL LINEAGE CELLS, AND THE PATHOGENESIS OF WMI IS CLOSELY LINKED WITH OL DEVELOPMENTAL DISORDERS. ID4, ANOTHER FAMILY MEMBER OF THE IDS PROTEIN, ALSO PLAYS A SIMILAR ROLE IN OL DIFFERENTIATION AND GENESIS. ID2 AND ID4 BELONG TO THE HELIX-LOOP-HELIX FAMILY; THEY LACK THE DNA-BINDING SEQUENCES AND INHIBIT OLIGODENDROGENESIS AND OPC DIFFERENTIATION. IN THIS REVIEW, WE MAINLY DISCUSS THE ROLES OF ID2 IN OL DEVELOPMENT, ESPECIALLY DURING OPC DIFFERENTIATION, AND SUMMARIZE THE ID2-MEDIATED INTRACELLULAR AND EXTRACELLULAR SIGNALING PATHWAYS THAT REGULATE THESE PROCESSES. WE ALSO DISCUSS ID4 IN RELATION TO BONE MORPHOGENETIC PROTEIN SIGNALING AND OLIGODENDROGENESIS. IT IS LIKELY THAT THESE DEVELOPMENTAL MECHANISMS ARE ALSO INVOLVED IN THE MYELIN REPAIR OR REMYELINATION IN HUMAN NEUROLOGICAL DISEASES. 2019 8 5208 27 PRENATAL STRESS, PREMATURITY, AND ASTHMA. ASTHMA IS THE MOST COMMON CHRONIC DISEASE OF CHILDHOOD, AFFECTING MILLIONS OF CHILDREN IN THE UNITED STATES AND WORLDWIDE. PREMATURITY IS A RISK FACTOR FOR ASTHMA, AND CERTAIN ETHNIC OR RACIAL MINORITIES SUCH AS PUERTO RICANS AND NON-HISPANIC BLACKS ARE DISPROPORTIONATELY AFFECTED BY BOTH PREMATURITY AND ASTHMA. IN THIS REVIEW, WE EXAMINE CURRENT EVIDENCE TO SUPPORT MATERNAL PSYCHOSOCIAL STRESS AS A PUTATIVE LINK BETWEEN PREMATURITY AND ASTHMA, WHILE ALSO FOCUSING ON DISRUPTION OF THE HYPOTHALAMIC-PITUITARY-ADRENAL (HPA) AXIS AND IMMUNE RESPONSES AS POTENTIAL UNDERLYING MECHANISMS FOR STRESS-INDUCED "PREMATURE ASTHMA." PRENATAL STRESS MAY CAUSE NOT ONLY ABNORMALITIES IN THE HPA AXIS BUT ALSO EPIGENETIC CHANGES IN THE FETAL GLUCOCORTICOID RECEPTOR GENE (NR3C1), LEADING TO IMPAIRED GLUCOCORTICOID METABOLISM. MOREOVER, MATERNAL STRESS CAN ALTER FETAL CYTOKINE BALANCE, FAVORING TH2 (ALLERGIC) IMMUNE RESPONSES CHARACTERISTIC OF ATOPIC ASTHMA: INTERLEUKIN 6 (IL-6), WHICH HAS BEEN ASSOCIATED WITH PREMATURE LABOR, CAN PROMOTE TH2 RESPONSES BY STIMULATING PRODUCTION OF IL-4 AND IL-13. GIVEN A LINK AMONG STRESS, PREMATURITY, AND ASTHMA, FUTURE RESEARCH SHOULD INCLUDE BIRTH COHORTS AIMED AT CONFIRMING AND BETTER CHARACTERIZING "PREMATURE ASTHMA." IF CONFIRMED, CLINICAL TRIALS OF PRENATAL MATERNAL STRESS REDUCTION WOULD BE WARRANTED TO REDUCE THE BURDEN OF THESE COMMON COMORBIDITIES. WHILE AWAITING THE RESULTS OF SUCH STUDIES, SOUND POLICIES TO PREVENT DOMESTIC AND COMMUNITY VIOLENCE (EG, FROM FIREARMS) ARE JUSTIFIED, NOT ONLY BY PUBLIC SAFETY BUT ALSO BY GROWING EVIDENCE OF DETRIMENTAL EFFECTS OF VIOLENCE-INDUCED STRESS ON PSYCHIATRIC AND SOMATIC HEALTH. 2015 9 846 30 CHILDHOOD EXPOSURE TO AMBIENT POLYCYCLIC AROMATIC HYDROCARBONS IS LINKED TO EPIGENETIC MODIFICATIONS AND IMPAIRED SYSTEMIC IMMUNITY IN T CELLS. BACKGROUND: EVIDENCE SUGGESTS THAT EXPOSURE TO POLYCYCLIC AROMATIC HYDROCARBONS (PAHS) INCREASES ATOPY; IT IS UNCLEAR HOW PAH EXPOSURE IS LINKED TO INCREASED SEVERITY OF ATOPIC DISEASES. OBJECTIVE: WE HYPOTHESIZED THAT AMBIENT PAH EXPOSURE IS LINKED TO IMPAIRMENT OF IMMUNITY IN ATOPIC CHILDREN (DEFINED AS CHILDREN WITH ASTHMA AND/OR ALLERGIC RHINITIS) FROM FRESNO, CALIFORNIA, AN AREA WITH ELEVATED AMBIENT PAHS. METHODS: WE RECRUITED 256 SUBJECTS FROM FRESNO, CA. AMBIENT PAH CONCENTRATIONS (NG/M(3) ) WERE MEASURED USING A SPATIAL-TEMPORAL REGRESSION MODEL OVER MULTIPLE TIME PERIODS. ASTHMA DIAGNOSIS WAS DETERMINED BY CURRENT NHLBI CRITERIA. PHENOTYPING AND FUNCTIONAL IMMUNE MEASUREMENTS WERE PERFORMED FROM ISOLATED CELLS. FOR EPIGENETIC MEASUREMENTS, DNA WAS ISOLATED AND PYROSEQUENCED. RESULTS: WE SHOW THAT HIGHER AVERAGE PAH EXPOSURE WAS SIGNIFICANTLY ASSOCIATED WITH IMPAIRED TREG FUNCTION AND INCREASED METHYLATION IN THE FORKHEAD BOX PROTEIN 3 (FOXP3) LOCUS (P < 0.05), CONDITIONAL ON ATOPIC STATUS. THESE EPIGENETIC MODIFICATIONS WERE SIGNIFICANTLY LINKED TO DIFFERENTIAL PROTEIN EXPRESSION OF FOXP3 (P < 0.001). METHYLATION WAS ASSOCIATED WITH CELLULAR FUNCTIONAL CHANGES, SPECIFICALLY TREG DYSFUNCTION, AND AN INCREASE IN TOTAL PLASMA IGE LEVELS. PROTEIN EXPRESSION OF IL-10 DECREASED AND IFN-GAMMA INCREASED AS THE EXTENT OF PAH EXPOSURE INCREASED. THE STRENGTH OF THE ASSOCIATIONS GENERALLY INCREASED AS THE TIME WINDOW FOR AVERAGE PAH EXPOSURE INCREASED FROM 24 HR TO 1 YEAR, SUGGESTING MORE OF A CHRONIC RESPONSE. SIGNIFICANT ASSOCIATIONS WITH CHRONIC PAH EXPOSURE AND IMMUNE OUTCOMES WERE ALSO OBSERVED IN SUBJECTS WITH ALLERGIC RHINITIS. CONCLUSIONS AND CLINICAL RELEVANCE: COLLECTIVELY, THESE RESULTS DEMONSTRATE THAT INCREASED AMBIENT PAH EXPOSURE IS ASSOCIATED WITH IMPAIRED SYSTEMIC IMMUNITY AND EPIGENETIC MODIFICATIONS IN A KEY LOCUS INVOLVED IN ATOPY: FOXP3, WITH A HIGHER IMPACT ON ATOPIC CHILDREN. THE RESULTS SUGGEST THAT INCREASED ATOPIC CLINICAL SYMPTOMS IN CHILDREN COULD BE LINKED TO INCREASED PAH EXPOSURE IN AIR POLLUTION. 2015 10 5426 42 REGULATION OF SIRTUIN EXPRESSION IN AUTOIMMUNE NEUROINFLAMMATION: INDUCTION OF SIRT1 IN OLIGODENDROCYTE PROGENITOR CELLS. IN MULTIPLE SCLEROSIS (MS) REGENERATION OF OLIGODENDROCYTES FOLLOWING INFLAMMATORY DEMYELINATION IS LIMITED BY THE COMPROMISED ABILITY OF PROGENITORS TO REPOPULATE LESIONED AREAS AND TRANSITION TO FUNCTIONALLY COMPETENT OLIGODENDROCYTES. REGARDING UNDERLYING MECHANISMS, THE INVOLVEMENT OF EPIGENETIC PROCESSES HAS BEEN SUGGESTED, E.G. THE CONTRIBUTION OF HISTONE DEACETYLASES (HDAC) KNOWN TO REGULATE OLIGODENDROCYTE PROGENITOR CELL (OPC) DIFFERENTIATION. HOWEVER, THEIR PRECISE EXPRESSION PATTERNS, PARTICULAR OF REDOX-SENSITIVE NAD(+) HDACS, REMAINS LARGELY UNKNOWN. IN THIS STUDY, WE DETERMINED THE EXPRESSION AND ACTIVITY OF SIRTUINS, MEMBERS OF THE HDAC CLASS III FAMILY WITH A SPECIFIC FOCUS ON SIRT1, PREVIOUSLY ASSOCIATED WITH NEURODEGENERATIVE, INFLAMMATORY AND DEMYELINATING DISORDERS OF THE CENTRAL NERVOUS SYSTEM (CNS). BY INVESTIGATING MOUSE EXPERIMENTAL AUTOIMMUNE ENCEPHALOMYELITIS (EAE), A MODEL FOR MS, WE FOUND THAT TRANSCRIPTION OF SIRT1, SIRT2 AND SIRT6 WAS SIGNIFICANTLY INCREASED IN THE CNS DURING CHRONIC DISEASE STAGES. WE CONFIRMED THIS FINDING FOR SIRT1 PROTEIN EXPRESSION AND WERE ABLE TO LOCALIZE UPREGULATED SIRT1 IN NUCLEI OF NG2(+) OR PDGFRALPHA(+) OPCS IN DEMYELINATED BRAIN LESIONS. IN CULTURED MOUSE A2B5(+) OPCS BLOCKADE OF SIRT1 ACTIVITY BY THE SMALL MOLECULE COMPOUND EX527 ENHANCED MITOTIC ACTIVITY BUT DID NOT AFFECT THE CAPACITY TO DIFFERENTIATE. A SIMILAR PATTERN WAS DETECTABLE IN OPCS DERIVED FROM SIRT1-DEFICIENT ANIMALS. TAKEN TOGETHER, OUR DATA SUGGEST THAT SIRT1 INHIBITION MAY HELP TO EXPAND THE ENDOGENOUS POOL OF OPCS WITHOUT AFFECTING THEIR DIFFERENTIATION. 2019 11 300 28 AIR POLLUTION AND INDOOR SETTINGS. INDOOR ENVIRONMENTS CONTRIBUTE SIGNIFICANTLY TO TOTAL HUMAN EXPOSURE TO AIR POLLUTANTS, AS PEOPLE SPEND MOST OF THEIR TIME INDOORS. HOUSEHOLD AIR POLLUTION (HAP) RESULTING FROM COOKING WITH POLLUTING ("DIRTY") FUELS, WHICH INCLUDE COAL, KEROSENE, AND BIOMASS (WOOD, CHARCOAL, CROP RESIDUES, AND ANIMAL MANURE) IS A GLOBAL ENVIRONMENTAL HEALTH PROBLEM. INDOOR POLLUTANTS ARE GASES, PARTICULATES, TOXINS, AND MICROORGANISMS AMONG OTHERS, THAT CAN HAVE AN IMPACT ESPECIALLY ON THE HEALTH OF CHILDREN AND ADULTS THROUGH A COMBINATION OF DIFFERENT MECHANISMS ON OXIDATIVE STRESS AND GENE ACTIVATION, EPIGENETIC, CELLULAR, AND IMMUNOLOGICAL SYSTEMS. AIR POLLUTION IS A MAJOR RISK FACTOR AND CONTRIBUTOR TO MORBIDITY AND MORTALITY FROM MAJOR CHRONIC DISEASES. CHILDREN ARE SIGNIFICANTLY AFFECTED BY THE IMPACT OF THE ENVIRONMENT DUE TO BIOLOGICAL IMMATURITY, PRENATAL AND POSTNATAL LUNG DEVELOPMENT. POOR AIR QUALITY HAS BEEN RELATED TO AN INCREASED PREVALENCE OF CLINICAL MANIFESTATIONS OF ALLERGIC ASTHMA AND RHINITIS. HEALTH PROFESSIONALS SHOULD INCREASE THEIR ROLE IN MANAGING THE EXPOSURE OF CHILDREN AND ADULTS TO AIR POLLUTION WITH BETTER METHODS OF CARE, PREVENTION, AND COLLECTIVE ACTION. INTERVENTIONS TO REDUCE HOUSEHOLD POLLUTANTS MAY PROMOTE HEALTH AND CAN BE ACHIEVED WITH EDUCATION, COMMUNITY, AND HEALTH PROFESSIONAL INVOLVEMENT. 2021 12 2924 23 GENERAL ANESTHETIC NEUROTOXICITY IN THE YOUNG: MECHANISM AND PREVENTION. GENERAL ANESTHESIA (GA) IS USUALLY CONSIDERED TO SAFELY INDUCE A REVERSIBLE UNCONSCIOUS STATE ALLOWING SURGERY TO BE PERFORMED WITHOUT PAIN. A GROWING NUMBER OF STUDIES, IN PARTICULAR PRE-CLINICAL STUDIES, HOWEVER, DEMONSTRATE THAT GENERAL ANESTHETICS CAN CAUSE NEURONAL DEATH AND EVEN LONG-TERM NEUROLOGICAL DEFICITS. HEREIN, WE REPORT OUR LITERATURE REVIEW AND META-ANALYSIS DATA OF THE NEUROLOGICAL OUTCOMES AFTER ANESTHESIA IN THE YOUNG. WE ALSO REVIEW AVAILABLE MECHANISTIC AND EPIGENETIC DATA OF GA EXPOSURE RELATED TO COGNITIVE IMPAIRMENT PER SE AND THE POTENTIAL PREVENTIVE STRATEGIES INCLUDING NATURAL HERBAL COMPOUNDS TO ATTENUATE THOSE SIDE EFFECTS. IN SUMMARY, ANESTHETIC-INDUCED NEUROTOXICITY MAY BE TREATABLE AND NATURAL HERBAL COMPOUNDS AND OTHER MEDICATIONS MAY HAVE GREAT POTENTIAL FOR SUCH USE BUT WARRANTS FURTHER STUDY BEFORE CLINICAL APPLICATIONS CAN BE INITIATED. 2019 13 1203 28 COULD EPIGENETICS HELP EXPLAIN RACIAL DISPARITIES IN CHRONIC PAIN? AFRICAN AMERICANS DISPROPORTIONATELY SUFFER MORE SEVERE AND DEBILITATING MORBIDITY FROM CHRONIC PAIN THAN DO NON-HISPANIC WHITES. THESE DIFFERENCES MAY ARISE FROM DIFFERENTIAL EXPOSURE TO PSYCHOSOCIAL AND ENVIRONMENTAL FACTORS SUCH AS ADVERSE CHILDHOOD EXPERIENCES, RACIAL DISCRIMINATION, LOW SOCIOECONOMIC STATUS, AND DEPRESSION, ALL OF WHICH HAVE BEEN ASSOCIATED WITH CHRONIC STRESS AND CHRONIC PAIN. RACE, AS A SOCIAL CONSTRUCT, MAKES IT SUCH THAT AFRICAN AMERICANS ARE MORE LIKELY TO EXPERIENCE DIFFERENT EARLY LIFE CONDITIONS, WHICH MAY INDUCE EPIGENETIC CHANGES THAT SUSTAIN RACIAL DIFFERENCES IN CHRONIC PAIN. EPIGENETICS IS ONE MECHANISM BY WHICH ENVIRONMENTAL FACTORS SUCH AS CHILDHOOD STRESS, RACIAL DISCRIMINATION, ECONOMIC HARDSHIP, AND DEPRESSION CAN AFFECT GENE EXPRESSION WITHOUT ALTERING THE UNDERLYING GENETIC SEQUENCE. THIS ARTICLE PROVIDES A NARRATIVE REVIEW OF THE LITERATURE ON EPIGENETICS AS A MECHANISM BY WHICH DIFFERENTIAL ENVIRONMENTAL EXPOSURE COULD EXPLAIN RACIAL DIFFERENCES IN CHRONIC PAIN. MOST STUDIES OF EPIGENETIC CHANGES IN CHRONIC PAIN EXAMINE DNA METHYLATION. DNA METHYLATION IS ALTERED IN THE GLUCOCORTICOID (STRESS RESPONSE) RECEPTOR GENE, NR3C1, WHICH HAS BEEN ASSOCIATED WITH DEPRESSION, CHILDHOOD STRESS, LOW SOCIOECONOMIC STATUS, AND CHRONIC PAIN. SIMILARLY, DNA METHYLATION PATTERNS OF IMMUNE CYTOKINE GENES HAVE BEEN ASSOCIATED WITH CHRONIC STRESS STATES. THUS, DNA METHYLATION CHANGES MAY PLAY AN ESSENTIAL ROLE IN THE EPIGENETIC MODULATION OF CHRONIC PAIN IN DIFFERENT RACES WITH A HIGHER INCIDENCE OF EPIGENETIC ALTERATIONS CONTRIBUTING TO MORE SEVERE AND DISABLING CHRONIC PAIN IN AFRICAN AMERICANS. 2019 14 529 21 ASTHMA IN URBAN CHILDREN: EPIDEMIOLOGY, ENVIRONMENTAL RISK FACTORS, AND THE PUBLIC HEALTH DOMAIN. ASTHMA IS THE MOST COMMONLY REPORTED CHRONIC CONDITION OF CHILDHOOD IN DEVELOPED COUNTRIES, WITH 6.5 MILLION CHILDREN AFFECTED IN THE USA. A DISPARATE BURDEN OF CHILDHOOD ASTHMA IS SEEN AMONG SOCIOECONOMICALLY DISADVANTAGED YOUTH, OFTEN CONCENTRATED IN URBAN AREAS WITH HIGH POVERTY RATES. HOST FACTORS THAT PREDISPOSE A CHILD TO ASTHMA INCLUDE ATOPY, MALE GENDER, PARENTAL HISTORY OF ASTHMA, AND ALSO RACE, ETHNICITY, AND GENETIC AND EPIGENETIC SUSCEPTIBILITIES. ENVIRONMENTAL FACTORS, SUCH AS IMPROVED HYGIENE, AMBIENT AIR POLLUTION, AND EARLY LIFE EXPOSURES TO MICROBES AND AEROALLERGENS, ALSO INFLUENCE THE DEVELOPMENT OF ASTHMA. WITH GREATER THAN 90% OF TIME SPENT INDOORS, HOME EXPOSURES (SUCH AS COCKROACH, RODENT, AND INDOOR AIR POLLUTION) ARE HIGHLY RELEVANT FOR URBAN ASTHMA. MORBIDITY REDUCTION MAY REQUIRE FOCUSED PUBLIC HEALTH INITIATIVES FOR ENVIRONMENTAL INTERVENTION IN HIGH PRIORITY RISK GROUPS AND THE ADDITION OF IMMUNE MODULATORY AGENTS IN CHILDREN WITH POORLY CONTROLLED DISEASE. 2016 15 537 18 ASYMPTOMATIC HYPERURICEMIA: IS IT REALLY ASYMPTOMATIC? PURPOSE OF REVIEW: HYPERURICEMIA IS HIGHLY PREVALENT, AFFECTING APPROXIMATELY 38 MILLION INDIVIDUALS IN THE UNITED STATES. HOWEVER, THE SIGNIFICANCE OF ASYMPTOMATIC HYPERURICEMIA - HYPERURICEMIA IN THE ABSENCE OF GOUT - CONTINUES TO BE DEBATED. RECENT FINDINGS: ASYMPTOMATIC HYPERURICEMIA RESULTS IN MONOSODIUM URATE CRYSTAL DEPOSITION IN TISSUES, WHICH MAY PROMOTE CHRONIC INFLAMMATION. INTRACELLULARLY, HYPERURICEMIA INHIBITS THE MASTER REGULATOR ADENOSINE MONOPHOSPHATE (AMP)-ASSOCIATED PROTEIN KINASE AND MAY CONDITION INNATE IMMUNE RESPONSES THROUGH DURABLE EPIGENETIC MODIFICATIONS. AT THE POPULATION LEVEL, ASYMPTOMATIC HYPERURICEMIA IS ASSOCIATED WITH MULTIPLE COMORBIDITIES, INCLUDING HYPERTENSION, CHRONIC KIDNEY DISEASE, CORONARY ARTERY DISEASE, AND DIABETES; LIMITATIONS OF THESE STUDIES INCLUDE THAT MOST ARE RETROSPECTIVE AND SOME DO NOT RIGOROUSLY DISTINGUISH BETWEEN ASYMPTOMATIC HYPERURICEMIA AND GOUT. TREATMENT STUDIES SUGGEST THAT URATE LOWERING MAY REDUCE THE RISK OF INCIDENCE OR PROGRESSION OF SOME OF THESE COMORBIDITIES; UNFORTUNATELY, MANY OF THESE TREATMENT STUDIES ARE SMALL OR FLAWED, AND NOT ALL STUDY RESULTS ARE CONSISTENT. SUMMARY: ACCUMULATING EVIDENCE SUGGESTS THAT ASYMPTOMATIC HYPERURICEMIA CONTRIBUTES TO THE COMORBIDITIES WITH WHICH IT ASSOCIATES AND THAT PROPER ASYMPTOMATIC HYPERURICEMIA TREATMENT MAY REDUCE FUTURE RISK. ADDITIONAL PROSPECTIVE TRIALS ARE NEEDED TO DEFINITELY ESTABLISH CAUSALITY AND SUPPORT DECISION-MAKING AS TO WHETHER, AND WHICH PATIENTS WITH ASYMPTOMATIC HYPERURICEMIA WOULD WARRANT URATE-LOWERING TREATMENT. 2020 16 2605 23 EPIGENETICS-A POTENTIAL MEDIATOR BETWEEN AIR POLLUTION AND PRETERM BIRTH. PRETERM BIRTH IS A MAJOR CAUSE OF INFANT MORBIDITY AND MORTALITY AND A POTENTIAL RISK FACTOR FOR ADULT CHRONIC DISEASE. WITH OVER 15 MILLION INFANTS BORN PRETERM WORLDWIDE EACH YEAR, PRETERM BIRTH POSES A GLOBAL HEALTH CONCERN. THERE IS A POSSIBLE ASSOCIATION BETWEEN AIR POLLUTION AND PRETERM BIRTH, THOUGH STUDIES HAVE BEEN INCONSISTENT, LIKELY DUE TO VARIATION IN STUDY DESIGN. HOW AIR POLLUTION INDUCES HEALTH EFFECTS IS UNCERTAIN; HOWEVER, STUDIES HAVE REPEATEDLY DEMONSTRATED THE EFFECTS OF AIR POLLUTION ON EPIGENETIC MODIFICATIONS. MORE RECENT EVIDENCE SUGGESTS THAT EPIGENETICS MAY, IN TURN, BE LINKED TO PRETERM BIRTH. DISCOVERY OF ENVIRONMENTALLY MODIFIABLE EPIGENETIC PROCESSES CONNECTED TO PRETERM BIRTH MAY HELP TO IDENTIFY WOMEN AT RISK OF PRETERM BIRTH, AND ULTIMATELY LEAD TO DEVELOPMENT OF NEW PRETERM BIRTH PREVENTION MEASURES. 2016 17 1225 29 CRITICAL ROLE OF EPIGENETIC MODIFICATION IN THE PATHOGENESIS OF ATOPIC DERMATITIS. ATOPIC DERMATITIS IS A CHRONIC INFLAMMATORY SKIN DISEASE CHARACTERISED BY RECURRENT ECZEMA-LIKE LESIONS AND SEVERE PRURITUS, ALONG WITH DRYING AND DECRUSTATION OF SKIN. CURRENT RESEARCH RELATES THE PATHOGENESIS OF ATOPIC DERMATITIS MAINLY TO GENETIC SUSCEPTIBILITY, ABNORMAL SKIN BARRIER FUNCTION, IMMUNE DISORDERS, STAPHYLOCOCCUS AUREUS COLONISATION, MICROBIOLOGICAL DYSFUNCTION AND VITAMIN D INSUFFICIENCY. EPIGENETIC MODIFICATIONS ARE DISTINCT GENETIC PHENOTYPES RESULTING FROM ENVIRONMENT-DRIVEN CHANGES IN CHROMOSOME FUNCTIONS IN THE ABSENCE OF NUCLEAR DNA SEQUENCE VARIATION. CLASSIC EPIGENETIC EVENTS INCLUDE DNA METHYLATION, HISTONE PROTEIN MODIFICATIONS AND NON-CODING RNA REGULATION. INCREASING EVIDENCE HAS INDICATED THAT EPIGENETIC EVENTS ARE INVOLVED IN THE PATHOGENESIS OF ATOPIC DERMATITIS BY THEIR EFFECTS ON MULTIPLE SIGNALLING PATHWAYS WHICH IN TURN INFLUENCE THE ABOVE FACTORS. THIS REVIEW PRIMARILY ANALYSES THE FUNCTION OF EPIGENETIC REGULATION IN THE PATHOGENESIS OF ATOPIC DERMATITIS. IN ADDITION, IT TRIES TO MAKE RECOMMENDATIONS FOR PERSONALISED EPIGENETIC TREATMENT STRATEGIES FOR ATOPIC DERMATITIS IN THE FUTURE. 2023 18 4062 27 MATERNAL AND CHILD HEALTH SERVICES AND AN INTEGRATED, LIFE-CYCLE APPROACH TO THE PREVENTION OF NON-COMMUNICABLE DISEASES. DESCRIBED AS THE 'INVISIBLE EPIDEMIC', NON-COMMUNICABLE DISEASES (NCDS) ARE THE WORLD'S LEADING CAUSE OF DEATH. MOST ARE CAUSED BY PREVENTABLE FACTORS, INCLUDING POOR DIET, TOBACCO USE, HARMFUL USE OF ALCOHOL AND PHYSICAL INACTIVITY. DIABETES, CANCER AND CARDIOVASCULAR AND CHRONIC LUNG DISEASES WERE RESPONSIBLE FOR 38 MILLION (68%) OF GLOBAL DEATHS IN 2012. SINCE 1990, PROPORTIONATE NCD MORTALITY HAS INCREASED SUBSTANTIALLY AS POPULATIONS HAVE AGED AND COMMUNICABLE DISEASES DECLINE. THE MAJORITY OF NCD DEATHS, ESPECIALLY PREMATURE NCD DEATHS (<70 YEARS, 82%), OCCUR IN LOW-INCOME AND MIDDLE-INCOME COUNTRIES, AND AMONG POOR COMMUNITIES WITHIN THEM. ADDRESSING NCDS IS RECOGNISED AS CENTRAL TO THE POST-2015 AGENDA; ACCORDINGLY, NCDS HAVE A SPECIFIC OBJECTIVE AND TARGET IN THE SUSTAINABLE DEVELOPMENT GOALS. WHILE DEATHS FROM NCDS OCCUR MAINLY IN ADULTHOOD, MANY HAVE THEIR ORIGINS IN EARLY LIFE, INCLUDING THROUGH EPIGENETIC MECHANISMS OPERATING BEFORE CONCEPTION. GOOD NUTRITION BEFORE CONCEPTION AND INTERVENTIONS AIMED AT PREVENTING NCDS DURING THE FIRST 1000 DAYS (FROM CONCEPTION TO AGE 2 YEARS), CHILDHOOD AND ADOLESCENCE MAY BE MORE COST-EFFECTIVE THAN MANAGING ESTABLISHED NCDS IN LATER LIFE WITH COSTLY TESTS AND DRUGS. FOLLOWING A LIFE-COURSE APPROACH, MATERNAL AND CHILD HEALTH INTERVENTIONS, BEFORE DELIVERY AND DURING CHILDHOOD AND ADOLESCENCE, CAN PREVENT NCDS AND SHOULD INFLUENCE GLOBAL HEALTH AND SOCIOECONOMIC DEVELOPMENT. THIS PAPER DESCRIBES HOW SUCH AN APPROACH MAY BE PURSUED, INCLUDING THROUGH THE ENGAGEMENT OF NON-HEALTH SECTORS. IT ALSO EMPHASISES EVALUATING AND DOCUMENTING RELATED INITIATIVES TO UNDERWRITE SYSTEMATIC AND EVIDENCE-BASED CROSS-SECTORAL ENGAGEMENT ON NCD PREVENTION IN THE FUTURE. 2017 19 4272 28 MICROBIOME AND BEHCET'S DISEASE: A SYSTEMATIC REVIEW. THE AIM OF THIS REVIEW WAS TO DESCRIBE THE CHANGES IN THE MICROBIOTA OF PATIENTS WITH BEHCET'S DISEASE (BD) AND THE MECHANISMS INVOLVED IN THE RELATIONSHIP BETWEEN THE MICROBIOME AND IMMUNITY IN BD. A SYSTEMATIC SEARCH FOR RELEVANT ARTICLES WAS MADE ON PUBMED AND THE COCHRANE LIBRARY DATABASE USING THE FOLLOWING TERMS: "MICROBIOTA AND BEHCET'S DISEASE" OR "MICROBIOME AND BEHCET'S DISEASE". SIXTEEN ARTICLES WERE INCLUDED IN A QUALITATIVE SYNTHESIS. THIS SYSTEMATIC REVIEW ON THE MICROBIOME AND BEHCET'S DISEASE UNDERLINES THE PRESENCE OF GUT DYSBIOSIS IN BD PATIENTS. THIS DYSBIOSIS IS MARKED BY (I) A DECREASE IN BUTYRATE-PRODUCING BACTERIA, WHICH COULD AFFECT T CELL DIFFERENTIATION AND EPIGENETIC REGULATION OF IMMUNE-RELATED GENES, (II) A MODIFICATION OF TRYPTOPHAN-METABOLISING BACTERIA, WHICH COULD BE LINKED TO DYSREGULATED IL-22 SECRETION, AND (III) A DECREASE IN BACTERIA KNOWN TO HAVE ANTI-INFLAMMATORY PROPERTIES. REGARDING ORAL MICROBIOTA, THIS REVIEW UNDERLINES THE POSSIBLE ROLE OF STREPTOCOCCUS SANGUINIS THROUGH MOLECULAR MIMICRY AND NETOSIS. CLINICAL STUDIES OF BD HAVE SHOWN THAT (I) NEED FOR DENTISTRY IS ASSOCIATED WITH A MORE SEVERE COURSE IN BD, AND (II) ANTIBIOTIC-SUPPLEMENTED MOUTHWASH REDUCES PAIN AND ULCERS. FECAL TRANSPLANTATION OF BD PATIENTS' MICROBIOTA INTO MOUSE MODELS LED TO DECREASED SCFA PRODUCTION, NEUTROPHIL ACTIVATION, AND TH1/TH17 RESPONSES.RECIPIENT MICE SHOWED EXACERBATED EXPERIMENTAL AUTOIMMUNE UVEITIS (EAU) AND EXPERIMENTAL AUTOIMMUNE ENCEPHALOMYELITIS (EAE). IN HERPES VIRUS SIMPLEX-1 (HSV-1) INFECTED MICE MIMICKING BD, ADMINISTRATION OF BUTYRATEPRODUCING BACTERIA IMPROVED SYMPTOMS AND IMMUNE VARIABLES. THE MICROBIOME MAY THUS BE INVOLVED IN BD THROUGH IMMUNITY REGULATION AND EPIGENETIC MODIFICATIONS. 2023 20 4313 39 MICRORNAS AS CANDIDATES FOR BIPOLAR DISORDER BIOMARKERS. BIPOLAR DISORDER (BD) IS A COMMON, RECURRING PSYCHIATRIC ILLNESS WITH UNKNOWN PATHOGENESIS. MUCH LIKE OTHER PSYCHIATRIC DISEASES, BD SUFFERS FROM THE CHRONIC LACK OF RELIABLE BIOMARKERS AND INNOVATIVE PHARMACOLOGICAL INTERVENTIONS. BETTER CHARACTERIZATION OF CLINICAL PROFILES, EXPERIMENTAL MEDICINE, GENOMIC DATA MINING, AND THE UTILIZATION OF EXPERIMENTAL MODELS, INCLUDING STEM CELL AND GENETICALLY MODIFIED MICE, ARE SUGGESTED WAYS FORWARD. ENVIRONMENT, INCLUDING EARLY CHILDHOOD EXPERIENCES, HAS BEEN DOCUMENTED TO MODULATE THE RISK FOR THE DEVELOPMENT OF PSYCHIATRIC DISORDERS VIA EPIGENETIC MECHANISMS. KEY EPIGENETIC REGULATORS, MICRORNAS (MIRNAS, MIRS), GOVERN NORMAL NEURONAL FUNCTIONING AND SHOW ALTERED EXPRESSION IN DIVERSE BRAIN PATHOLOGIES. WE OBSERVED SIGNIFICANT ALTERATIONS OF EXOSOMAL MIR-29C LEVELS IN PREFRONTAL CORTEX (BRODMANN AREA 9, BA9) OF BD PATIENTS. WE ALSO DEMONSTRATED THAT EXOSOMES EXTRACTED FROM THE ANTERIOR CINGULATE CORTEX (BA24), A CRUCIAL AREA FOR MODULATING EMOTIONAL EXPRESSION AND AFFECT, HAVE INCREASED LEVELS OF MIR-149 IN BD PATIENTS COMPARED TO CONTROLS. BECAUSE MIR-149 HAS BEEN SHOWN TO INHIBIT GLIAL PROLIFERATION, WE HYPOTHESIZED THAT INCREASED MIR-149 EXPRESSION IN BA24-DERIVED EXOSOMES MAY BE CONSISTENT WITH THE PREVIOUSLY REPORTED REDUCED GLIAL CELL NUMBERS IN BA24 OF PATIENTS DIAGNOSED WITH FAMILIAL BD. QPCR ANALYSIS OF LASER-MICRODISSECTED NEURONAL AND GLIAL CELLS FROM BA24 CORTICAL SAMPLES OF BD PATIENTS VERIFIED THAT THE GLIAL, BUT NOT NEURONAL, POPULATION EXHIBITS SIGNIFICANTLY INCREASED MIR-149 EXPRESSION. THESE FINDINGS SUPPORT NEURON-GLIA INTERACTION AS A POSSIBLE TARGET MECHANISM IN BD, IMPLICATED BY OTHERS IN NEUROIMAGING, POSTMORTEM, AND IN VIVO STUDIES OF THE PATHOLOGICAL CHANGES MEDIATED BY GLIAL CELLS. 2021