1 1647 131 DOES THE STRESS OF LABORATORY LIFE AND EXPERIMENTATION ON ANIMALS ADVERSELY AFFECT RESEARCH DATA? A CRITICAL REVIEW. RECURRENT ACUTE AND/OR CHRONIC STRESS CAN AFFECT ALL VERTEBRATE SPECIES, AND CAN HAVE SERIOUS CONSEQUENCES. IT IS INCREASINGLY AND WIDELY APPRECIATED THAT LABORATORY ANIMALS EXPERIENCE SIGNIFICANT AND REPEATED STRESS, WHICH IS UNAVOIDABLE AND IS CAUSED BY MANY ASPECTS OF LABORATORY LIFE, SUCH AS CAPTIVITY, TRANSPORT, NOISE, HANDLING, RESTRAINT AND OTHER PROCEDURES, AS WELL AS THE EXPERIMENTAL PROCEDURES APPLIED TO THEM. SUCH STRESS IS DIFFICULT TO MITIGATE, AND LACK OF SIGNIFICANT DESENSITISATION/HABITUATION CAN RESULT IN CONSIDERABLE PSYCHOLOGICAL AND PHYSIOLOGICAL WELFARE PROBLEMS, WHICH ARE MEDIATED BY THE ACTIVATION OF VARIOUS NEUROENDOCRINE NETWORKS THAT HAVE NUMEROUS AND PERVASIVE EFFECTS. PSYCHOLOGICAL DAMAGE CAN BE REFLECTED IN STEREOTYPICAL BEHAVIOURS, INCLUDING REPETITIVE PACING AND CIRCLING, AND EVEN SELF-HARM. PHYSICAL CONSEQUENCES INCLUDE ADVERSE EFFECTS ON IMMUNE FUNCTION, INFLAMMATORY RESPONSES, METABOLISM, AND DISEASE SUSCEPTIBILITY AND PROGRESSION. FURTHER, SOME OF THESE EFFECTS ARE EPIGENETIC, AND ARE THEREFORE POTENTIALLY TRANSGENERATIONAL: THE BIOLOGY OF ANIMALS WHOSE PARENTS/GRANDPARENTS WERE WILD-CAUGHT AND/OR HAVE EXPERIENCED CHRONIC STRESS IN LABORATORIES COULD BE ALTERED, AS COMPARED TO FREE-LIVING INDIVIDUALS. IT IS ARGUED THAT THESE EFFECTS MUST HAVE CONSEQUENCES FOR THE RELIABILITY OF EXPERIMENTAL DATA AND THEIR EXTRAPOLATION TO HUMANS, AND THIS MAY NOT BE RECOGNISED SUFFICIENTLY AMONG THOSE WHO USE ANIMALS IN EXPERIMENTS. 2018 2 6188 30 THE IMPACT OF INSOMNIA ON FRAILTY AND THE HALLMARKS OF AGING. THROUGHOUT THE COURSE OF LIFE, THERE ARE AGE-RELATED CHANGES IN SLEEP. DESPITE THESE NORMAL CHANGES, THERE IS A HIGH PERCENTAGE OF OLDER ADULTS THAT REPORT SLEEP DISSATISFACTION WITH A HIGH PERVASIVENESS OF CHRONIC INSOMNIA, THE MOST COMMON SLEEP DISORDER WORLDWIDE, WITH ITS PREVALENCE BEING EXPECTED TO CONTINUOUSLY INCREASE DUE TO THE GROWING RATES OF AGING AND OBESITY. THIS CAN HAVE DIFFERENT ADVERSE HEALTH OUTCOMES, ESPECIALLY BY PROMOTING BOTH PHYSICAL AND COGNITIVE DECLINE, WHICH ULTIMATELY MAY AGGRAVATE FRAILTY IN OLDER ADULTS. MOREOVER, AGE-RELATED FRAILTY AND SLEEP DYSFUNCTION MAY HAVE A COMMON MECHANISM RELATED TO THE HALLMARKS OF CELLULAR AGING. CELLULAR AGING WAS CATEGORIZED INTO NINE HALLMARKS, SUCH AS DNA DAMAGE, TELOMERE ATTRITION AND EPIGENETIC CHANGES. IN THE CONTEXT OF GERIATRIC AND CHRONIC INSOMNIA RESEARCH, THIS REVIEW AIMS AT DISCUSSING THE CURRENT EVIDENCE FROM BOTH ANIMAL MODELS AND HUMAN COHORTS ADDRESSING THE LINK BETWEEN CHRONIC INSOMNIA, THE HALLMARKS OF AGING AND THEIR IMPACT ON FRAILTY. MOREOVER, THE MOST RECENT RESEARCH ABOUT THE PUTATIVE EFFECT OF INSOMNIA THERAPEUTIC APPROACHES ON HALLMARKS OF AGING WILL BE ALSO HIGHLIGHTED. 2023 3 2023 23 EPIGENETIC CHANGES BY DNA METHYLATION IN CHRONIC AND INTERMITTENT HYPOXIA. DNA METHYLATION OF CYTOSINE RESIDUES IS A WELL-STUDIED EPIGENETIC CHANGE, WHICH REGULATES GENE TRANSCRIPTION BY ALTERING ACCESSIBILITY FOR TRANSCRIPTION FACTORS. HYPOXIA IS A PERVASIVE STIMULUS THAT AFFECTS MANY PHYSIOLOGICAL PROCESSES. THE CIRCULATORY AND RESPIRATORY SYSTEMS ADAPT TO CHRONIC SUSTAINED HYPOXIA, SUCH AS THAT ENCOUNTERED DURING A HIGH-ALTITUDE SOJOURN. MANY PEOPLE LIVING AT SEA LEVEL EXPERIENCE CHRONIC INTERMITTENT HYPOXIA (IH) DUE TO SLEEP APNEA, WHICH LEADS TO CARDIOVASCULAR AND RESPIRATORY MALADAPTATION. THIS ARTICLE PRESENTS A BRIEF UPDATE ON EMERGING EVIDENCE SUGGESTING THAT CHANGES IN DNA METHYLATION CONTRIBUTE TO PATHOLOGIES CAUSED BY CHRONIC IH AND POTENTIALLY MEDIATE ADAPTATIONS TO CHRONIC SUSTAINED HYPOXIA BY AFFECTING THE HYPOXIA-INDUCIBLE FACTOR (HIF) SIGNALING PATHWAY. 2017 4 2727 40 EXPLAINING THE BLACK-WHITE DISPARITY IN PRETERM BIRTH: A CONSENSUS STATEMENT FROM A MULTI-DISCIPLINARY SCIENTIFIC WORK GROUP CONVENED BY THE MARCH OF DIMES. IN 2017-2019, THE MARCH OF DIMES CONVENED A WORKGROUP WITH BIOMEDICAL, CLINICAL, AND EPIDEMIOLOGIC EXPERTISE TO REVIEW KNOWLEDGE OF THE CAUSES OF THE PERSISTENT BLACK-WHITE DISPARITY IN PRETERM BIRTH (PTB). MULTIPLE DATABASES WERE SEARCHED TO IDENTIFY HYPOTHESIZED CAUSES EXAMINED IN PEER-REVIEWED LITERATURE, 33 HYPOTHESIZED CAUSES WERE REVIEWED FOR WHETHER THEY PLAUSIBLY AFFECT PTB AND EITHER OCCUR MORE/LESS FREQUENTLY AND/OR HAVE A LARGER/SMALLER EFFECT SIZE AMONG BLACK WOMEN VS. WHITE WOMEN. WHILE DEFINITIVE PROOF IS LACKING FOR MOST POTENTIAL CAUSES, MOST ARE BIOLOGICALLY PLAUSIBLE. NO SINGLE DOWNSTREAM OR MIDSTREAM FACTOR EXPLAINS THE DISPARITY OR ITS SOCIAL PATTERNING, HOWEVER, MANY LIKELY PLAY LIMITED ROLES, E.G., WHILE GENETIC FACTORS LIKELY CONTRIBUTE TO PTB, THEY EXPLAIN AT MOST A SMALL FRACTION OF THE DISPARITY. RESEARCH LINKS MOST HYPOTHESIZED MIDSTREAM CAUSES, INCLUDING SOCIOECONOMIC FACTORS AND STRESS, WITH THE DISPARITY THROUGH THEIR INFLUENCE ON THE HYPOTHESIZED DOWNSTREAM FACTORS. SOCIOECONOMIC FACTORS ALONE CANNOT EXPLAIN THE DISPARITY'S SOCIAL PATTERNING. CHRONIC STRESS COULD AFFECT PTB THROUGH NEUROENDOCRINE AND IMMUNE MECHANISMS LEADING TO INFLAMMATION AND IMMUNE DYSFUNCTION, STRESS COULD ALTER A WOMAN'S MICROBIOTA, IMMUNE RESPONSE TO INFECTION, CHRONIC DISEASE RISKS, AND BEHAVIORS, AND TRIGGER EPIGENETIC CHANGES INFLUENCING PTB RISK. AS AN UPSTREAM FACTOR, RACISM IN MULTIPLE FORMS HAS REPEATEDLY BEEN LINKED WITH THE PLAUSIBLE MIDSTREAM/DOWNSTREAM FACTORS, INCLUDING SOCIOECONOMIC DISADVANTAGE, STRESS, AND TOXIC EXPOSURES. RACISM IS THE ONLY FACTOR IDENTIFIED THAT DIRECTLY OR INDIRECTLY COULD EXPLAIN THE RACIAL DISPARITIES IN THE PLAUSIBLE MIDSTREAM/DOWNSTREAM CAUSES AND THE OBSERVED SOCIAL PATTERNING. HISTORICAL AND CONTEMPORARY SYSTEMIC RACISM CAN EXPLAIN THE RACIAL DISPARITIES IN SOCIOECONOMIC OPPORTUNITIES THAT DIFFERENTIALLY EXPOSE AFRICAN AMERICANS TO LIFELONG FINANCIAL STRESS AND ASSOCIATED HEALTH-HARMING CONDITIONS. SEGREGATION PLACES BLACK WOMEN IN STRESSFUL SURROUNDINGS AND EXPOSES THEM TO ENVIRONMENTAL HAZARDS. RACE-BASED DISCRIMINATORY TREATMENT IS A PERVASIVE STRESSOR FOR BLACK WOMEN OF ALL SOCIOECONOMIC LEVELS, CONSIDERING BOTH INCIDENTS AND THE CONSTANT VIGILANCE NEEDED TO PREPARE ONESELF FOR POTENTIAL INCIDENTS. RACISM IS A HIGHLY PLAUSIBLE, MAJOR UPSTREAM CONTRIBUTOR TO THE BLACK-WHITE DISPARITY IN PTB THROUGH MULTIPLE PATHWAYS AND BIOLOGICAL MECHANISMS. WHILE MUCH IS UNKNOWN, EXISTING KNOWLEDGE AND CORE VALUES (EQUITY, JUSTICE) SUPPORT ADDRESSING RACISM IN EFFORTS TO ELIMINATE THE RACIAL DISPARITY IN PTB. 2021 5 1523 24 DNA METHYLATION CHANGES AND INFLAMMAGING IN AGING-ASSOCIATED DISEASES. AGING AS AN INEVITABLE PHENOMENON IS ASSOCIATED WITH PERVASIVE CHANGES IN PHYSIOLOGICAL FUNCTIONS. THERE IS A RELATIONSHIP BETWEEN AGING AND THE INCREASE OF SEVERAL CHRONIC DISEASES. MOST AGE-RELATED DISORDERS ARE ACCOMPANIED BY AN UNDERLYING CHRONIC INFLAMMATORY STATE, AS DEMONSTRATED BY LOCAL INFILTRATION OF INFLAMMATORY CELLS AND GREATER LEVELS OF PROINFLAMMATORY CYTOKINES IN THE BLOODSTREAM. WITHIN INFLAMMAGING, MANY EPIGENETIC EVENTS, ESPECIALLY DNA METHYLATION, CHANGE. DURING THE AGING PROCESS, DUE TO ABERRATIONS OF DNA METHYLATION, BIOLOGICAL PROCESSES ARE DISRUPTED, LEADING TO THE EMERGENCE OR PROGRESSION OF A VARIETY OF HUMAN DISEASES, INCLUDING CANCER, NEURODEGENERATIVE DISORDERS, CARDIOVASCULAR DISEASE AND DIABETES. THE FOCUS OF THIS REVIEW IS ON DNA METHYLATION, WHICH IS INVOLVED IN INFLAMMAGING-RELATED ACTIVITIES, AND HOW ITS DYSREGULATION LEADS TO HUMAN DISORDERS. 2022 6 548 30 AUTISM SPECTRUM DISORDER AT THE CROSSROAD BETWEEN GENES AND ENVIRONMENT: CONTRIBUTIONS, CONVERGENCES, AND INTERACTIONS IN ASD DEVELOPMENTAL PATHOPHYSIOLOGY. THE COMPLEX PATHOPHYSIOLOGY OF AUTISM SPECTRUM DISORDER ENCOMPASSES INTERACTIONS BETWEEN GENETIC AND ENVIRONMENTAL FACTORS. ON THE ONE HAND, HUNDREDS OF GENES, CONVERGING AT THE FUNCTIONAL LEVEL ON SELECTIVE BIOLOGICAL DOMAINS SUCH AS EPIGENETIC REGULATION AND SYNAPTIC FUNCTION, HAVE BEEN IDENTIFIED TO BE EITHER CAUSATIVE OR RISK FACTORS OF AUTISM. ON THE OTHER HAND, EXPOSURE TO CHEMICALS THAT ARE WIDESPREAD IN THE ENVIRONMENT, SUCH AS ENDOCRINE DISRUPTORS, HAS BEEN ASSOCIATED WITH ADVERSE EFFECTS ON HUMAN HEALTH, INCLUDING NEURODEVELOPMENTAL DISORDERS. INTERESTINGLY, EXPERIMENTAL RESULTS SUGGEST AN OVERLAP IN THE REGULATORY PATHWAYS PERTURBED BY GENETIC MUTATIONS AND ENVIRONMENTAL FACTORS, DEPICTING CONVERGENCES AND COMPLEX INTERPLAYS BETWEEN GENETIC SUSCEPTIBILITY AND TOXIC INSULTS. THE PERVASIVE NATURE OF CHEMICAL EXPOSURE POSES PIVOTAL CHALLENGES FOR NEUROTOXICOLOGICAL STUDIES, REGULATORY AGENCIES, AND POLICY MAKERS. THIS HIGHLIGHTS AN EMERGING NEED OF DEVELOPING NEW INTEGRATIVE MODELS, INCLUDING BIOMONITORING, EPIDEMIOLOGY, EXPERIMENTAL, AND COMPUTATIONAL TOOLS, ABLE TO CAPTURE REAL-LIFE SCENARIOS ENCOMPASSING THE INTERACTION BETWEEN CHRONIC EXPOSURE TO MIXTURE OF SUBSTANCES AND INDIVIDUALS' GENETIC BACKGROUNDS. IN THIS REVIEW, WE ADDRESS THE INTERTWINED ROLES OF GENETIC LESIONS AND ENVIRONMENTAL INSULTS. SPECIFICALLY, WE OUTLINE THE TRANSFORMATIVE POTENTIAL OF STEM CELL MODELS, COUPLED WITH OMICS ANALYTICAL APPROACHES AT INCREASINGLY SINGLE CELL RESOLUTION, AS CONVERGING TOOLS TO EXPERIMENTALLY DISSECT THE PATHOGENIC MECHANISMS UNDERLYING NEURODEVELOPMENTAL DISORDERS, AS WELL AS TO IMPROVE DEVELOPMENTAL NEUROTOXICOLOGY RISK ASSESSMENT. 2020 7 2500 21 EPIGENETICS AND IMPRINTED GENES: INSIGHTS FROM THE IMPRINTED GNAS LOCUS. THE HALLMARKS OF EPIGENETICS--THE MEMORY OF DEFINING EARLIER DEVELOPMENTAL EVENTS AND THE DISTINCTION OF ACTIVE AND INACTIVE GENES--ARE EXEMPLIFIED BY IMPRINTED GENES. IN THIS ARTICLE, I SHALL CONSIDER THE IMPRINTED GNAS LOCUS IN SOME DETAIL. GNAS ENCODES THE STIMULATORY G-PROTEIN SUBUNIT, GSALPHA, AN ESSENTIAL INTERMEDIATE BETWEEN RECEPTOR COUPLING AND CYCLIC ADENOSINE MONOPHOSPHATE GENERATION. IT PROVIDES AN EXCELLENT ILLUSTRATION OF THE PLEIOTROPIC EFFECTS OF IMPRINTED GENES, PARTICULARLY ON SKELETAL GROWTH AND METABOLISM, AND IS A POWERFUL EXAMPLE OF THE CONFLICTING EFFECTS OF IMPRINTED GENES WITH OPPOSING PATTERNS OF IMPRINTING. I SHALL DESCRIBE THE EFFECTS OF GSALPHA DEFICIENCY IN HUMANS AND THE KNOWLEDGE GAINED FROM GENETIC MANIPULATION IN THE MOUSE. FINALLY, GIVEN THE PERVASIVE EFFECTS OF IMPRINTED GENES, I SHALL DISCUSS THE LIKELIHOOD THAT EPIGENETIC DEREGULATION, FOR EXAMPLE OF IMPRINTED GENES, COULD CONTRIBUTE TO THE DEVELOPMENTAL PROGRAMMING OF CHRONIC ADULT DISEASES. 2009 8 929 25 CHRONIC INFLAMMATION: ACCELERATOR OF BIOLOGICAL AGING. BIOLOGICAL AGING IS CHARACTERIZED BY A CHRONIC LOW-GRADE INFLAMMATION LEVEL. THIS CHRONIC PHENOMENON HAS BEEN NAMED "INFLAMM-AGING" AND IS A HIGHLY SIGNIFICANT RISK FACTOR FOR MORBIDITY AND MORTALITY IN THE OLDER PERSONS. THE MOST COMMON THEORIES OF INFLAMM-AGING INCLUDE REDOX STRESS, MITOCHONDRIAL DYSFUNCTION, GLYCATION, DEREGULATION OF THE IMMUNE SYSTEM, HORMONAL CHANGES, EPIGENETIC MODIFICATIONS, AND DYSFUNCTION TELOMERE ATTRITION. INFLAMM-AGING PLAYS A ROLE IN THE INITIATION AND PROGRESSION OF AGE-RELATED DISEASES SUCH AS TYPE II DIABETES, ALZHEIMER'S DISEASE, CARDIOVASCULAR DISEASE, FRAILTY, SARCOPENIA, OSTEOPOROSIS, AND CANCER. THIS REVIEW WILL COVER THE IDENTIFICATION OF PATHWAYS THAT CONTROL AGE-RELATED INFLAMMATION ACROSS MULTIPLE SYSTEMS AND ITS POTENTIAL CAUSAL ROLE IN CONTRIBUTING TO ADVERSE HEALTH OUTCOMES. 2017 9 5948 18 TARGETING THE MOLECULAR & CELLULAR PILLARS OF HUMAN AGING WITH EXERCISE. BIOLOGICAL AGING IS THE MAIN DRIVER OF AGE-ASSOCIATED CHRONIC DISEASES. IN 2014, THE UNITED STATES NATIONAL INSTITUTE OF AGING (NIA) SPONSORED A MEETING BETWEEN SEVERAL INVESTIGATORS IN THE FIELD OF AGING BIOLOGY, WHO IDENTIFIED SEVEN BIOLOGICAL PILLARS OF AGING AND A CONSENSUS REVIEW, "GEROSCIENCE: LINKING AGING TO CHRONIC DISEASE," WAS PUBLISHED. THE PILLARS OF AGING DEMONSTRATED THE CONSERVATION OF AGING PATHWAYS IN DIVERSE MODEL ORGANISMS AND THUS REPRESENT A USEFUL FRAMEWORK WITH WHICH TO STUDY HUMAN AGING. IN THIS PRESENT REVIEW, WE REVISIT THE SEVEN PILLARS OF AGING FROM THE PERSPECTIVE OF EXERCISE AND DISCUSS HOW REGULAR PHYSICAL EXERCISE CAN MODULATE THESE PILLARS TO STAVE OFF AGE-RELATED CHRONIC DISEASES AND MAINTAIN FUNCTIONAL CAPACITY. 2023 10 49 28 A CURRENT GENETIC AND EPIGENETIC VIEW ON HUMAN AGING MECHANISMS. THE PROCESS OF AGING IS ONE OF THE MOST COMPLEX AND INTRIGUING BIOLOGICAL PHENOMENONS. AGING IS A GENETICALLY REGULATED PROCESS IN WHICH THE ORGANISM'S MAXIMUM LIFESPAN POTENTIAL IS PRE-DETERMINED, WHILE THE RATE OF AGING IS INFLUENCED BY ENVIRONMENTAL FACTORS AND LIFESTYLE. CONSIDERING THE COMPLEXITY OF MECHANISMS INVOLVED IN THE REGULATION OF AGING PROCESS, UP TO THIS DATE THERE ISN'T A MAJOR, UNIFYING THEORY WHICH COULD EXPLAIN THEM. AS GENETIC/EPIGENETIC AND ENVIRONMENTAL FACTORS BOTH INEVITABLY INFLUENCE THE AGING PROCESS, HERE WE PRESENT A REVIEW ON THE GENETIC AND EPIGENETIC REGULATION OF THE MOST IMPORTANT MOLECULAR AND CELLULAR MECHANISMS INVOLVED IN THE PROCESS OF AGING. BASED ON THE STUDIES ON OXIDATIVE STRESS, METABOLISM, GENOME STABILITY, EPIGENETIC MODIFICATIONS AND CELLULAR SENESCENCE IN ANIMAL MODELS AND HUMANS, WE GIVE AN OVERVIEW OF KEY GENETIC AND MOLECULAR PATHWAYS RELATED TO AGING. AS MOST OF GENETIC MANIPULATIONS WHICH INFLUENCE THE AGING PROCESS ALSO AFFECT REPRODUCTION, WE DISCUSS AGING IN HUMANS AS A POST-REPRODUCTIVE GENETICALLY DETERMINED PROCESS. AFTER THE AGE OF REPRODUCTIVE SUCCESS, AGING CONTINOUSLY PROGRESSES WHICH CLINICALLY COINCIDES WITH THE ONSET OF MOST CHRONIC DISEASES, CANCERS AND DEMENTIONS. AS EVOLUTION SHAPES THE GENOMES FOR REPRODUCTIVE SUCCESS AND NOT FOR POST-REPRODUCTIVE SURVIVAL, AGING COULD BE DEFINED AS A PROTECTIVE MECHANISM WHICH ENSURES THE PRESERVATION AND PROGRESS OF SPECIES THROUGH THE MODIFICATION, TRASMISSION AND IMPROVEMENT OF GENETIC MATERIAL. 2009 11 3669 27 INFLAMMAGING AND CANCER: A CHALLENGE FOR THE MEDITERRANEAN DIET. AGING IS CONSIDERED THE MAJOR RISK FACTOR FOR CANCER, ONE OF THE MOST IMPORTANT MORTALITY CAUSES IN THE WESTERN WORLD. INFLAMMAGING, A STATE OF CHRONIC, LOW-LEVEL SYSTEMIC INFLAMMATION, IS A PERVASIVE FEATURE OF HUMAN AGING. CHRONIC INFLAMMATION INCREASES CANCER RISK AND AFFECTS ALL CANCER STAGES, TRIGGERING THE INITIAL GENETIC MUTATION OR EPIGENETIC MECHANISM, PROMOTING CANCER INITIATION, PROGRESSION AND METASTATIC DIFFUSION. THUS, INFLAMMAGING IS A STRONG CANDIDATE TO CONNECT AGE AND CANCER. A COROLLARY OF THIS HYPOTHESIS IS THAT INTERVENTIONS AIMING TO DECREASE INFLAMMAGING SHOULD PROTECT AGAINST CANCER, AS WELL AS MOST/ALL AGE-RELATED DISEASES. EPIDEMIOLOGICAL DATA ARE CONCORDANT IN SUGGESTING THAT THE MEDITERRANEAN DIET (MD) DECREASES THE RISK OF A VARIETY OF CANCERS BUT THE UNDERPINNING MECHANISM(S) IS (ARE) STILL UNCLEAR. HERE WE REVIEW DATA INDICATING THAT THE MD (AS A WHOLE DIET OR SINGLE BIOACTIVE NUTRIENTS TYPICAL OF THE MD) MODULATES MULTIPLE INTERCONNECTED PROCESSES INVOLVED IN CARCINOGENESIS AND INFLAMMATORY RESPONSE SUCH AS FREE RADICAL PRODUCTION, NF-KAPPAB ACTIVATION AND EXPRESSION OF INFLAMMATORY MEDIATORS, AND THE EICOSANOIDS PATHWAY. PARTICULAR ATTENTION IS DEVOTED TO THE CAPABILITY OF MD TO AFFECT THE BALANCE BETWEEN PRO- AND ANTI-INFLAMMAGING AS WELL AS TO EMERGING TOPICS SUCH AS MAINTENANCE OF GUT MICROBIOTA (GM) HOMEOSTASIS AND EPIGENETIC MODULATION OF ONCOGENESIS THROUGH SPECIFIC MICRORNAS. 2015 12 436 30 ANTIFRAGILITY AND ANTIINFLAMMAGING: CAN THEY PLAY A ROLE FOR A HEALTHY LONGEVITY? ONE OF THE MOST EXCITING CHALLENGES OF THE RESEARCH ON AGING IS TO EXPLAIN HOW THE ENVIRONMENTAL FACTORS INTERACT WITH THE GENETIC BACKGROUND TO MODULATE THE CHANCES TO REACH THE EXTREME LIMIT OF HUMAN LIFE IN HEALTHY CONDITIONS. THE COMPLEX EPIGENETIC MECHANISMS CAN EXPLAIN BOTH THE INTERACTION BETWEEN DNA AND ENVIRONMENTAL FACTORS, AND THE LONG-DISTANCE PERSISTENCE OF LIFESTYLE EFFECTS, DUE TO THE SO CALLED "EPIGENETIC MEMORY". ONE OF THE MOST EXTENSIVELY INVESTIGATED THEORIES ON AGING FOCUSES ON THE INFLAMMATORY RESPONSES, SUGGESTING THAT THE AGE-RELATED PROGRESSION OF LOW-GRADE AND THEREFORE FOR LONG TIME SUBCLINICAL, CHRONIC, SYSTEMIC, INFLAMMATORY PROCESS, NAMED "INFLAMMAGING", COULD BE THE MOST RELEVANT RISK FACTOR FOR THE DEVELOPMENT AND PROGRESSION OF THE MOST COMMON AGE-RELATED DISEASES AND ULTIMATELY OF DEATH. THE RESULTS OF MANY STUDIES ON LONG-LIVED PEOPLE, ESPECIALLY ON CENTENARIANS, SUGGESTED THAT HEALTHY OLD PEOPLE CAN COPE WITH INFLAMMAGING UPREGULATING THE ANTIINFLAMMAGING RESPONSES. OVERALL, A GENETIC MAKE-UP CODING FOR A STRONG ANTIINFLAMMAGING RESPONSE AND AN AGE-RELATED ABILITY TO REMODEL KEY METABOLIC PATHWAYS TO COPE WITH A PLETHORA OF ANTIGENS AND STRESSORS SEEM TO BE THE BEST WAYS FOR REACH THE EXTREME LIMIT OF HUMAN LIFESPAN IN HEALTH STATUS. IN THIS SCENARIO, WE WONDERED IF THE ANTIFRAGILITY CONCEPT, RECENTLY DEVELOPED IN THE FRAMEWORK OF BUSINESS AND RISK ANALYSIS, COULD ADD SOME INFORMATION TO DISENTANGLE THE HETEROGENEOUS NATURE OF THE AGING PROCESS IN HUMAN. THE ANTIFRAGILITY IS THE PROPERTY OF THE COMPLEX SYSTEMS TO INCREASE THEIR PERFORMANCES BECAUSE OF HIGH STRESS. BASED ON THIS THEORY WE WERE WONDERING IF SOME SUBJECTS COULD BE ABLE TO MODULATE FASTER THAN OTHERS THEIR EPIGENOME TO COPE WITH A PLETHORA OF STRESSORS DURING LIFE, PROBABLY MODULATING THE INFLAMMATORY AND ANTI-INFLAMMATORY RESPONSES. IN THIS FRAMEWORK, ANTIFRAGILITY COULD SHARE SOME COMMON MECHANISMS WITH ANTI-INFLAMMAGING, MODULATING THE ABILITY TO RESTRAIN THE INFLAMMATORY RESPONSES, SO THAT ANTIFRAGILITY AND ANTIINFLAMMAGING COULD BE VIEWED AS DIFFERENT PIECES OF THE SAME PUZZLE, BOTH IMPINGING UPON THE CHANCES TO TRAVEL ALONG THE HEALTHY AGING TRAJECTORY. 2023 13 2528 26 EPIGENETICS AS A KEY LINK BETWEEN PSYCHOSOCIAL STRESS AND AGING: CONCEPTS, EVIDENCE, MECHANISMS . PSYCHOSOCIAL STRESS-ESPECIALLY WHEN CHRONIC, EXCESSIVE, OR OCCURRING EARLY IN LIFE-HAS BEEN ASSOCIATED WITH ACCELERATED AGING AND INCREASED DISEASE RISK. WITH RAPID AGING OF THE WORLD POPULATION, THE NEED TO ELUCIDATE THE UNDERLYING MECHANISMS IS PRESSING, NOW MORE SO THAN EVER. AMONG MOLECULAR MECHANISMS LINKING STRESS AND AGING, THE PRESENT ARTICLE REVIEWS EVIDENCE ON THE ROLE OF EPIGENETICS, BIOCHEMICAL PROCESSES THAT CAN BE SET INTO MOTION BY STRESSORS AND IN TURN INFLUENCE GENOMIC FUNCTION AND COMPLEX PHENOTYPES, INCLUDING AGING-RELATED OUTCOMES. THE ARTICLE FURTHER PROVIDES A CONCEPTUAL MECHANISTIC FRAMEWORK ON HOW STRESS MAY DRIVE EPIGENETIC CHANGES AT SUSCEPTIBLE GENOMIC SITES, THEREBY EXERTING SYSTEMS-LEVEL EFFECTS ON THE AGING EPIGENOME WHILE ALSO REGULATING THE EXPRESSION OF MOLECULES IMPLICATED IN AGING-RELATED PROCESSES. THIS EMERGING EVIDENCE, TOGETHER WITH WORK EXAMINING RELATED BIOLOGICAL PROCESSES, BEGINS TO SHED LIGHT ON THE EPIGENETIC AND, MORE BROADLY, MOLECULAR UNDERPINNINGS OF THE LONG-HYPOTHESIZED CONNECTION BETWEEN STRESS AND AGING. . 2019 14 6189 32 THE IMPACT OF LIFE STRESS ON HALLMARKS OF AGING AND ACCELERATED SENESCENCE: CONNECTIONS IN SICKNESS AND IN HEALTH. CHRONIC STRESS IS A RISK FACTOR FOR NUMEROUS AGING-RELATED DISEASES AND HAS BEEN SHOWN TO SHORTEN LIFESPAN IN HUMANS AND OTHER SOCIAL MAMMALS. YET HOW LIFE STRESS CAUSES SUCH A VAST RANGE OF DISEASES IS STILL LARGELY UNCLEAR. IN RECENT YEARS, THE IMPACT OF STRESS ON HEALTH AND AGING HAS BEEN INCREASINGLY ASSOCIATED WITH THE DYSREGULATION OF THE SO-CALLED HALLMARKS OF AGING. THESE ARE BASIC BIOLOGICAL MECHANISMS THAT INFLUENCE INTRINSIC CELLULAR FUNCTIONS AND WHOSE ALTERATION CAN LEAD TO ACCELERATED AGING. HERE, WE REVIEW CORRELATIONAL AND EXPERIMENTAL LITERATURE (PRIMARILY FOCUSING ON EVIDENCE FROM HUMANS AND MURINE MODELS) ON THE CONTRIBUTION OF LIFE STRESS - PARTICULARLY STRESS DERIVED FROM ADVERSE SOCIAL ENVIRONMENTS - TO TRIGGER HALLMARKS OF AGING, INCLUDING CELLULAR SENESCENCE, STERILE INFLAMMATION, TELOMERE SHORTENING, PRODUCTION OF REACTIVE OXYGEN SPECIES, DNA DAMAGE, AND EPIGENETIC CHANGES. WE ALSO EVALUATE THE VALIDITY OF STRESS-INDUCED SENESCENCE AND ACCELERATED AGING AS AN ETIOPATHOLOGICAL PROPOSITION. FINALLY, WE HIGHLIGHT CURRENT GAPS OF KNOWLEDGE AND FUTURE DIRECTIONS FOR THE FIELD, AND DISCUSS PERSPECTIVES FOR TRANSLATIONAL GEROSCIENCE. 2023 15 1879 31 EMERGING ROLES OF NON-CODING RNAS IN PSORIASIS PATHOGENESIS. PSORIASIS IS A COMPLEX GENETIC SKIN DISORDER TYPICALLY MANIFESTED BY RED, SCALY, AND ITCHY PLAQUES MOST COMMONLY OVER THE SCALP, TRUNK, ELBOWS, AND KNEES. HISTOPATHOLOGICAL FEATURES INCLUDE THICKENING OF THE EPIDERMAL LAYER DUE TO HYPER-PROLIFERATION AND ABNORMAL DIFFERENTIATION OF EPIDERMAL KERATINOCYTES ALONG WITH INFILTRATION OF IMMUNE CELLS IN THE PSORIATIC SKIN. IT IS A CHRONIC INFLAMMATORY RELAPSING DISEASE, AND THERE IS CURRENTLY NO PERMANENT CURE FOR PSORIASIS. PROPER MEDICATIONS CAN REDUCE THE SEVERITY OF THE DISEASE AND IMPROVE THE QUALITY OF LIFE OF THE PATIENTS. WHILE THE GENETIC COMPONENTS OF PSORIASIS PATHOGENESIS ARE WELL EXPLORED, THE FULL UNDERSTANDING OF ITS EPIGENETIC COMPONENT REMAINS ELUSIVE. NON-CODING RNAS (NCRNAS) ARE DOCUMENTED TO REGULATE VARIOUS EPIGENETIC PROCESSES THAT LEAD TO THE PATHOGENESIS OF DIFFERENT DISEASES INCLUDING PSORIASIS. IN THIS REVIEW, WE HAVE DISCUSSED THE MOLECULAR INTERPLAY OF DIFFERENT NCRNAS IN PSORIASIS PATHOGENESIS. THE ROLES OF MICRORNAS (MIRNAS) IN PSORIASIS ARE PRETTY WELL STUDIED, WHEREAS THE ROLES OF LONG NONCODING RNAS (LNCRNAS) AND CIRCULAR RNAS (CIRCRNAS) ARE EMERGING. THIS REVIEW PROVIDES IDEAS COVERING SOME OF THE LATEST FINDINGS OF DIFFERENT MODES OF FUNCTIONS PLAYED BY THOSE DIFFERENT NCRNAS DOCUMENTED IN THE LITERATURE. AS AN EVER-EVOLVING TOPIC, SOME WORKS ARE STILL ONGOING AS WELL AS THERE ARE SEVERAL FIELDS THAT NEED RIGOROUS SCIENTIFIC VENTURES. WE HAVE PROPOSED THE AREAS WHICH CLAIM MORE EXPLORATIONS TO BETTER UNDERSTAND THE ROLES PLAYED BY THE NCRNAS IN PSORIASIS PATHOGENESIS. 2023 16 28 36 A BIOMIMETIC NATURAL SCIENCES APPROACH TO UNDERSTANDING THE MECHANISMS OF AGEING IN BURDEN OF LIFESTYLE DISEASES. THE WORLDWIDE LANDSCAPE OF AN AGEING POPULATION AND AGE-RELATED DISEASE BRINGS WITH IT HUGE SOCIO-ECONOMIC AND PUBLIC HEALTHCARE CONCERNS ACROSS NATIONS. CORRESPONDINGLY, MONUMENTAL HUMAN AND FINANCIAL RESOURCES HAVE BEEN INVESTED IN BIOMEDICAL RESEARCH, WITH A MISSION TO DECODE THE MECHANISMS OF AGEING AND HOW THESE CONTRIBUTE TO AGE-RELATED DISEASE. MULTIPLE HALLMARKS OF AGEING HAVE BEEN IDENTIFIED THAT ARE COMMON ACROSS TAXA, HIGHLIGHTING THEIR FUNDAMENTAL IMPORTANCE. THESE INCLUDE DYSREGULATED MITOCHONDRIAL METABOLISM AND TELOMERES BIOLOGY, EPIGENETIC MODIFICATIONS, CELL-MATRIX INTERACTIONS, PROTEOSTASIS, DYSREGULATED NUTRIENT SENSING, STEM CELL EXHAUSTION, INFLAMMAGEING AND IMMUNO-SENESCENCE. WHILE OUR UNDERSTANDING OF THE MOLECULAR BASIS OF AGEING IS IMPROVING, IT REMAINS A COMPLEX AND MULTIFACTORIAL PROCESS THAT REMAINS TO BE FULLY UNDERSTOOD. A KEY ASPECT OF THE SHORTFALL IN OUR UNDERSTANDING OF THE AGEING PROCESS LIES IN TRANSLATING DATA FROM STANDARD ANIMAL MODELS TO HUMANS. CONSEQUENTLY, WE SUGGEST THAT A 'BIOMIMETIC' AND COMPARATIVE APPROACH, INTEGRATING KNOWLEDGE FROM SPECIES IN THE WILD, AS OPPOSED TO INBRED GENETICALLY HOMOGENOUS LABORATORY ANIMALS, CAN PROVIDE POWERFUL INSIGHTS INTO HUMAN AGEING PROCESSES. HERE WE DISCUSS SOME PARTICULARITIES AND COMPARATIVE PATTERNS AMONG SEVERAL SPECIES FROM THE ANIMAL KINGDOM, ENDOWED WITH LONGEVITY OR SHORT LIFESPANS AND UNIQUE METABOLIC PROFILES THAT COULD BE POTENTIALLY EXPLOITED TO THE UNDERSTANDING OF AGEING AND AGE-RELATED DISEASES. BASED UPON LESSONS FROM NATURE, WE ALSO HIGHLIGHT SEVERAL AVENUES FOR RENEWED FOCUS IN THE PATHOPHYSIOLOGY OF AGEING AND AGE-RELATED DISEASE (I.E. DIET-MICROBIOME-HEALTH AXIS, OXIDATIVE PROTEIN DAMAGE, ADAPTIVE HOMOEOSTASIS AND PLANETARY HEALTH). WE PROPOSE THAT A BIOMIMETIC ALLIANCE WITH COLLABORATIVE RESEARCH FROM DIFFERENT DISCIPLINES CAN IMPROVE OUR UNDERSTANDING OF AGEING AND AGE-RELATED DISEASES WITH LONG-TERM SUSTAINABLE UTILITY. 2021 17 4183 22 META-HALLMARKS OF AGING AND CANCER. BOTH AGING AND CANCER ARE CHARACTERIZED BY A SERIES OF PARTIALLY OVERLAPPING "HALLMARKS" THAT WE SUBJECT HERE TO A META-ANALYSIS. SEVERAL HALLMARKS OF AGING (I.E., GENOMIC INSTABILITY, EPIGENETIC ALTERATIONS, CHRONIC INFLAMMATION, AND DYSBIOSIS) ARE VERY SIMILAR TO SPECIFIC CANCER HALLMARKS AND HENCE CONSTITUTE COMMON "META-HALLMARKS," WHILE OTHER FEATURES OF AGING (I.E., TELOMERE ATTRITION AND STEM CELL EXHAUSTION) ACT LIKELY TO SUPPRESS ONCOGENESIS AND HENCE CAN BE VIEWED AS PREPONDERANTLY "ANTAGONISTIC HALLMARKS." DISABLED MACROAUTOPHAGY AND CELLULAR SENESCENCE ARE TWO HALLMARKS OF AGING THAT EXERT CONTEXT-DEPENDENT ONCOSUPPRESSIVE AND PRO-TUMORIGENIC EFFECTS. SIMILARLY, THE EQUIVALENCE OR ANTAGONISM BETWEEN AGING-ASSOCIATED DEREGULATED NUTRIENT-SENSING AND CANCER-RELEVANT ALTERATIONS OF CELLULAR METABOLISM IS COMPLEX. THE AGONISTIC AND ANTAGONISTIC RELATIONSHIP BETWEEN THE PROCESSES THAT DRIVE AGING AND CANCER HAS BEARINGS FOR THE AGE-RELATED INCREASE AND OLDEST AGE-RELATED DECREASE OF CANCER MORBIDITY AND MORTALITY, AS WELL AS FOR THE THERAPEUTIC MANAGEMENT OF MALIGNANT DISEASE IN THE ELDERLY. 2023 18 3960 32 LONG NON-CODING RNAS: A DOUBLE-EDGED SWORD IN AGING KIDNEY AND RENAL DISEASE. AGING AS ONE OF INTRINSIC BIOLOGICAL PROCESSES IS A RISK FACTOR FOR MANY CHRONIC DISEASES. KIDNEY DISEASE IS A GLOBAL PROBLEM AND HEALTH CARE BURDEN WORLDWIDE. THE DIAGNOSIS OF KIDNEY DISEASE IS CURRENTLY BASED ON SERUM CREATININE AND UREA LEVELS. NOVEL BIOMARKERS MAY IMPROVE DIAGNOSTIC ACCURACY, THEREBY ALLOWING EARLY PREVENTION AND TREATMENT. OVER THE PAST FEW YEARS, ADVANCES IN GENOME ANALYSES HAVE IDENTIFIED AN EMERGING CLASS OF NONCODING RNAS THAT PLAY CRITICAL ROLES IN THE REGULATION OF GENE EXPRESSION AND EPIGENETIC REPROGRAMMING. LONG NONCODING RNAS (LNCRNAS) ARE PERVASIVELY TRANSCRIBED IN THE GENOME AND COULD BIND DNA, RNA AND PROTEIN. EMERGING EVIDENCE HAS DEMONSTRATED THAT LNCRNAS PLAYED AN IMPORTANT ROLE IN ALL STAGES OF KIDNEY DISEASE. TO DATE, ONLY SOME LNCRNAS WERE WELL IDENTIFIED AND CHARACTERIZED, BUT THE COMPLEXITY OF MULTILEVEL REGULATION OF TRANSCRIPTIONAL PROGRAMS INVOLVED IN THESE PROCESSES REMAINS UNDEFINED. IN THIS REVIEW, WE SUMMARIZED THE LNCRNA EXPRESSION PROFILING OF LARGE-SCALE IDENTIFIED LNCRNAS ON KIDNEY DISEASES INCLUDING ACUTE KIDNEY INJURY, CHRONIC KIDNEY DISEASE, DIABETIC NEPHROPATHY AND KIDNEY TRANSPLANTATION. WE FURTHER DISCUSSED A NUMBER OF ANNOTATED LNCRNAS LINKING WITH COMPLEX ETIOLOGY OF KIDNEY DISEASES. FINALLY, SEVERAL LNCRNAS WERE HIGHLIGHTED AS DIAGNOSTIC BIOMARKERS AND THERAPEUTIC TARGETS. TARGETING LNCRNAS MAY REPRESENT A PRECISE THERAPEUTIC STRATEGY FOR PROGRESSIVE RENAL FIBROSIS. 2021 19 6454 37 THIRD JESUS CULEBRAS LECTURE - MOLECULAR BIOLOGY AND CLINICAL NUTRITION; WHERE DO WE STAND AND WHERE DO WE GO? NUTRITION PLAYS A FUNDAMENTAL ROLE IN THE MAINTENANCE OF HEALTH AND THE TREATMENT OF DISEASE, AND SERVES AS THE CROSSROADS FOR MANY DISCIPLINES. BIOCHEMISTRY AND MOLECULAR BIOLOGY REPRESENTS A KEY BRAND OF SCIENCE TO ASCERTAIN THE MECHANISM OF ACTION OF NUTRIENTS AND OTHER FOOD BIOACTIVE COMPOUNDS IN HEALTH AND DISEASE. THE AIM OF THE PRESENT JESUS M. CULEBRAS LECTURE IS TO CONSIDER THE FUTURE OF THE RELATIONSHIPS BETWEEN MOLECULAR BIOLOGY AND CLINICAL NUTRITION AND TO DISCUSS THE USE OF MOLECULAR AND GENETIC TOOLS TO STUDY MOLECULAR RESPONSES TO DIETARY FACTORS AND THE METABOLIC CONSEQUENCES OF FOOD AND TO CONSIDER MAJOR CHALLENGES ON HUMAN NUTRITION SCIENCES IN THE 21(ST) CENTURY. PARTICULAR EMPHASIS IS GIVEN TO THE IDENTIFICATION AND USE OF NOVEL BIOMARKERS IN INFLAMMATORY DISEASES. LIKEWISE, THE IMPORTANCE OF THE HUMAN MICROBIOME AND HOW MICROORGANISMS CAN BE SAFELY UTILIZED IN THE PREVENTION AND MANAGEMENT OF INFECTIOUS AND CHRONIC DISEASES ARE DISCUSSED. MOREOVER, THE KEY ROLE OF NUTRIGENETICS, NUTRIGENOMICS AND EPIGENETICS IN THE NEW ERA OF NUTRITION IS CONSIDERED. NUTRIGENETICS REFERS TO THE ROLE OF DNA SEQUENCE VARIATION IN THE RESPONSES TO NUTRIENTS, WHEREAS NUTRIGENOMICS IS THE STUDY OF THE ROLE OF NUTRIENTS IN GENE EXPRESSION. EPIGENETICS IS THE STUDY OF MITOTICALLY HERITABLE ALTERATIONS IN GENE EXPRESSION POTENTIAL THAT ARE NOT CAUSED BY DNA SEQUENCE ALTERATIONS. IN THE PAST DECADE, IT HAS INCREASINGLY BEEN RECOGNIZED THAT DYSREGULATION OF EPIGENETIC MECHANISMS MAY PLAY AN IMPORTANT ROLE IN HUMAN DISEASE. INDEED, THERE IS INCREASING INTEREST IN EPIGENETIC MECHANISMS UNDERLYING PHENOTYPE MODIFICATION MODULATED BY NUTRIENTS. FURTHER RESEARCH IN THOSE AREAS SHOULD CONTRIBUTE TO EVALUATE FUNCTIONALITY OF SPECIFIC NUTRIENTS AND BIOACTIVE COMPOUNDS IN CLINICAL NUTRITION AND ALLOW PERSONALIZED NUTRITIONAL ADVICE. 2013 20 1175 27 CONTRIBUTIONS OF AGE-RELATED THYMIC INVOLUTION TO IMMUNOSENESCENCE AND INFLAMMAGING. IMMUNE SYSTEM AGING IS CHARACTERIZED BY THE PARADOX OF IMMUNOSENESCENCE (INSUFFICIENCY) AND INFLAMMAGING (OVER-REACTION), WHICH INCORPORATE TWO SIDES OF THE SAME COIN, RESULTING IN IMMUNE DISORDER. IMMUNOSENESCENCE REFERS TO DISRUPTION IN THE STRUCTURAL ARCHITECTURE OF IMMUNE ORGANS AND DYSFUNCTION IN IMMUNE RESPONSES, RESULTING FROM BOTH AGED INNATE AND ADAPTIVE IMMUNITY. INFLAMMAGING, DESCRIBED AS A CHRONIC, STERILE, SYSTEMIC INFLAMMATORY CONDITION ASSOCIATED WITH ADVANCED AGE, IS MAINLY ATTRIBUTED TO SOMATIC CELLULAR SENESCENCE-ASSOCIATED SECRETORY PHENOTYPE (SASP) AND AGE-RELATED AUTOIMMUNE PREDISPOSITION. HOWEVER, THE INABILITY TO REDUCE SENESCENT SOMATIC CELLS (SSCS), BECAUSE OF IMMUNOSENESCENCE, EXACERBATES INFLAMMAGING. AGE-RELATED ADAPTIVE IMMUNE SYSTEM DEVIATIONS, PARTICULARLY ALTERED T CELL FUNCTION, ARE DERIVED FROM AGE-RELATED THYMIC ATROPHY OR INVOLUTION, A HALLMARK OF THYMIC AGING. RECENTLY, THERE HAVE BEEN MAJOR DEVELOPMENTS IN UNDERSTANDING HOW AGE-RELATED THYMIC INVOLUTION CONTRIBUTES TO INFLAMMAGING AND IMMUNOSENESCENCE AT THE CELLULAR AND MOLECULAR LEVELS, INCLUDING GENETIC AND EPIGENETIC REGULATION, AS WELL AS DEVELOPMENTS OF MANY POTENTIAL REJUVENATION STRATEGIES. HEREIN, WE DISCUSS THE RESEARCH PROGRESS UNCOVERING HOW AGE-RELATED THYMIC INVOLUTION CONTRIBUTES TO IMMUNOSENESCENCE AND INFLAMMAGING, AS WELL AS THEIR INTERSECTION. WE ALSO DESCRIBE HOW T CELL ADAPTIVE IMMUNITY MEDIATES INFLAMMAGING AND PLAYS A CRUCIAL ROLE IN THE PROGRESSION OF AGE-RELATED NEUROLOGICAL AND CARDIOVASCULAR DISEASES, AS WELL AS CANCER. WE THEN BRIEFLY OUTLINE THE UNDERLYING CELLULAR AND MOLECULAR MECHANISMS OF AGE-RELATED THYMIC INVOLUTION, AND FINALLY SUMMARIZE POTENTIAL REJUVENATION STRATEGIES TO RESTORE AGED THYMIC FUNCTION. 2020