1 3620 100 IN VIVO AND IN VITRO GENOTOXIC AND EPIGENETIC EFFECTS OF TWO TYPES OF COLA BEVERAGES AND CAFFEINE: A MULTIASSAY APPROACH. THE AIM OF THIS WORK WAS TO ASSESS THE BIOLOGICAL AND FOOD SAFETY OF TWO DIFFERENT BEVERAGES: CLASSIC COCA COLA (CCC) AND CAFFEINE-FREE COCA COLA (CFCC). TO THIS END, WE DETERMINED THE GENOTOXICOLOGICAL AND BIOLOGICAL EFFECTS OF DIFFERENT DOSES OF LYOPHILISED CCC AND CFCC AND CAFFEINE (CAF), THE MAIN DISTINCTIVE CONSTITUENT. THEIR TOXIC/ANTITOXIC, GENOTOXIC/ANTIGENOTOXIC, AND CHRONIC TOXICITY (LIFESPAN ASSAY) EFFECTS WERE DETERMINED IN VIVO USING THE DROSOPHILA MODEL. THEIR CYTOTOXIC ACTIVITIES WERE DETERMINED USING THE HL-60 IN VITRO CANCER MODEL. IN ADDITION, CLASTOGENIC DNA TOXICITY WAS MEASURED USING INTERNUCLEOSOMAL FRAGMENTATION AND SCGE ASSAYS. THEIR EPIGENETIC EFFECTS WERE ASSESSED ON THE HL-60 METHYLATION STATUS USING SOME REPETITIVE ELEMENTS. THE EXPERIMENTAL RESULTS SHOWED A SLIGHT CHEMOPREVENTIVE EFFECT OF THE TWO COLA BEVERAGES AGAINST HL-60 LEUKAEMIA CELLS, PROBABLY MEDIATED BY NONAPOPTOTIC MECHANISMS. FINALLY, CCC AND CAF INDUCED A GLOBAL GENOME HYPOMETHYLATION EVALUATED IN LINE-1 AND ALU M1 REPETITIVE ELEMENTS. OVERALL, WE DEMONSTRATED FOR THE FIRST TIME THE SAFETY OF THIS FAMOUS BEVERAGE IN IN VIVO AND IN VITRO MODELS. 2016 2 2077 24 EPIGENETIC DISRUPTION OF PLACENTAL GENES BY CHRONIC MATERNAL CAFETERIA DIET IN RATS. MATERNAL DIET HAS IMPACT ON REPRODUCTION, FETAL DEVELOPMENT AND OFFSPRING BEHAVIOR, ALTHOUGH MOLECULAR MECHANISMS REMAINED UNKNOWN. OUR AIMS WERE TO ASSESS (1) THE EFFECTS OF A CAFETERIA (CAF) DIET (WESTERN DIET HABITS) ON FEMALE REPRODUCTIVE PERFORMANCE, FETAL AND PLACENTAL PARAMETERS ON GESTATIONAL DAY 21 AND LITTER SIZE AND PUP WEIGHT AT BIRTH; AND (2) PLACENTAL MESSENGER RNA (MRNA) EXPRESSION AND EPIGENETIC REGULATION OF INSULIN-LIKE GROWTH FACTOR (IGF) AND VASCULAR ENDOTHELIAL GROWTH FACTOR (VEGF) AND THEIR RECEPTORS. FEMALE WISTAR RATS WERE FED WITH CONTROL OR CAF DIET FROM WEANING UNTIL PARTURITION. AT WEEK 14 AFTER DIETS STARTED, FEMALES WERE MATED AND HALF OF THE ANIMALS WERE EUTHANIZED ON GESTATIONAL DAY 21 TO EVALUATE REPRODUCTIVE PARAMETERS INCLUDING THE PREGNANCY RATE, NUMBER OF CORPORA LUTEA, IMPLANTATION SITES AND RESORPTION SITES. MOREOVER, FETAL WEIGHT AND LENGTH, PLACENTAL WEIGHT, AND PLACENTAL INDEX WERE RECORDED. PLACENTAS WERE COLLECTED FOR MRNA QUANTIFICATION AND DNA METHYLATION ANALYSIS. THE REMAINING ANIMALS WERE ALLOWED TO GIVE BIRTH AND THE NUMBER AND WEIGHT OF THE PUPS WERE EVALUATED. CAF DIET DID NOT AFFECT REPRODUCTIVE PERFORMANCE OR FETAL WEIGHT AND LENGTH. HOWEVER, CAF-FED ANIMALS SHOWED A DECREASE IN PLACENTAL WEIGHT AND INDEX AND THE PUPS EXHIBITED A LOW BIRTH WEIGHT. ADDITIONALLY, WE FOUND AN UPREGULATION OF IGF2 AND A DOWN REGULATION OF VEGF PLACENTAL MRNA EXPRESSION IN CAF DAMS, ASSOCIATED WITH METHYLATION STATUS CHANGES OF THEIR PROMOTERS. WE CONCLUDE THAT FEMALE CHRONIC CAF DIET CONSUMPTION IMPAIRS FETO-PLACENTAL DEVELOPMENT AND COULD BE EXPLAINED BY AN EPIGENETIC DISRUPTION OF IGF AND VEGF SYSTEMS. 2022 3 2813 15 FIBROBLAST REPROGRAMMING IN GASTROINTESTINAL CANCER. GASTROINTESTINAL CANCERS ARE A SIGNIFICANT CAUSE OF CANCER MORTALITY WORLDWIDE AND HAVE BEEN STRONGLY LINKED WITH CHRONIC INFLAMMATION. CURRENT THERAPIES FOCUS ON EPITHELIAL/CANCER CELLS; HOWEVER, THE IMPORTANCE OF THE TUMOR MICROENVIRONMENT IN THE DEVELOPMENT AND TREATMENT OF THE DISEASE IS ALSO NOW WELL ESTABLISHED. CANCER-ASSOCIATED FIBROBLASTS (CAFS) ARE A MAJOR COMPONENT OF THE TUMOR MICROENVIRONMENT, AND ARE ACTIVELY PARTICIPATING IN TUMOR INITIATION, PROMOTION AND METASTASIS. THEY STRUCTURALLY AND FUNCTIONALLY AFFECT CANCER CELL PROLIFERATION, TUMOR IMMUNITY, ANGIOGENESIS, EXTRACELLULAR MATRIX REMODELING AND METASTASIS THROUGH A VARIETY OF SIGNALING PATHWAYS. CAFS ORIGINATE PREDOMINANTLY FROM RESIDENT MESENCHYMAL CELLS, WHICH ARE ACTIVATED AND REPROGRAMMED IN RESPONSE TO CUES FROM CANCER CELLS. IN RECENT YEARS, CHRONIC INFLAMMATION OF THE GASTROINTESTINAL TRACT HAS ALSO PROVEN AN IMPORTANT DRIVER OF MESENCHYMAL CELL ACTIVATION AND SUBSEQUENT CAF DEVELOPMENT, WHICH IN TURN ARE CAPABLE OF REGULATING THE TRANSITION FROM ACUTE TO CHRONIC INFLAMMATION AND CANCER. IN THIS REVIEW, WE WILL PROVIDE A CONCISE OVERVIEW OF THE MECHANISMS THAT DRIVE FIBROBLAST REPROGRAMMING IN CANCER AND THE RECENT ADVANCES ON THE DOWNSTREAM SIGNALING PATHWAYS THAT REGULATE THE FUNCTIONAL PROPERTIES OF THE ACTIVATED MESENCHYME. THIS NEW MECHANISTIC INSIGHT COULD PAVE THE WAY FOR NEW THERAPEUTIC STRATEGIES AND BETTER PROGNOSIS FOR CANCER PATIENTS. 2020 4 3615 21 IN VITRO FOLATE DEFICIENCY INDUCES DEOXYNUCLEOTIDE POOL IMBALANCE, APOPTOSIS, AND MUTAGENESIS IN CHINESE HAMSTER OVARY CELLS. THE GENETIC AND EPIGENETIC EFFECTS OF NUTRITIONAL FOLATE DEFICIENCY WERE STUDIED IN TWO CHINESE HAMSTER OVARY (CHO) CELL LINES. THE CHO-AA8 CELL LINE (HEMIZYGOUS AT THE APRT LOCUS) AND CHO-UV5 (DNA REPAIR-DEFICIENT MUTANT OF AA8) WERE CULTURED IN HAM'S F-12 MEDIUM OR IN CUSTOM-PREPARED HAM'S F-12 MEDIUM LACKING FOLIC ACID, THYMIDINE, AND HYPOXANTHINE. CELLS CULTURED ACUTELY IN THE FOLATE DEFICIENT MEDIUM EXHIBITED INITIAL GROWTH ARREST, FOLLOWED BY MASSIVE CELL DEATH AND DNA FRAGMENTATION INTO NUCLEOSOMAL MULTIMERS CHARACTERISTIC OF APOPTOSIS. ALTHOUGH PROLONGED CULTURE IN THE FOLATE DEFICIENT MEDIUM WAS CYTOSTATIC AND LETHAL TO THE MAJORITY CELLS, MINOR SUBPOPULATIONS IN BOTH CELL LINES FAILED TO INITIATE CELL DEATH, EXHIBITED PHENOTYPIC ABNORMALITIES, AND ADAPTED A SELECTIVE GROWTH ADVANTAGE UNDER MARGINAL FOLATE CONDITIONS. THESE "RESISTANT" CLONES EXHIBITED MAJOR ALTERATIONS IN DEOXYNUCLEOTIDE POOLS ASSOCIATED WITH AN INCREASE IN MUTANT FREQUENCY AT THE APRT LOCUS AS DETECTED BY RESISTANCE TO CYTOTOXICITY IN 8-AZAADENOSINE. THE MUTATION FREQUENCY IN THE DNA REPAIR-DEFICIENT CHO-UV5 CELLS WAS APPROXIMATELY 100-FOLD GREATER THAN THAT IN THE PARENTAL AA8 CLONES, UNDERSCORING THE IMPORTANCE OF DNA REPAIR UNDER CONDITIONS OF FOLATE DEFICIENCY AND NUCLEOTIDE POOL IMBALANCE. THE ENHANCED MUTATION FREQUENCY IN THE DNA REPAIR-COMPETENT FOLATE-DEFICIENT CHO-AA8 CELLS SUGGESTS THAT DNA REPAIR ACTIVITY IS LESS EFFECTIVE UNDER FOLATE-DEFICIENT CONDITIONS. THESE RESULTS ADD TO THE ACCUMULATING CLINICAL AND EXPERIMENTAL EVIDENCE RELATING CHRONIC FOLATE DEFICIENCY TO GENOMIC INSTABILITY AND CARCINOGENESIS. 1994 5 6777 18 [ASSOCIATION OF P-MOBILE ELEMENT ACTIVITY AND DNA METHYLATION PATTERN CHANGES IN THE CONDITIONS OF DROSOPHILA MELANOGASTER PROLONGED IRRADIATION]. ASSOCIATION OF THE RADIOSENSITIVITY AND EPIGENETIC PATTERN DNA CHANGES AT THE CONDITIONS OF PROLONGED IRRADIATION WAS INVESTIGATED. TWO LABORATORY DROSOPHILA MELANOGASTER STRAINS (CANTON-S AND RI) IRRADIATED FOR 20 GENERATIONS TO LOW DOSES RATE (1.2 X 10(-1), 0.8 X 10(-8) AND 0.12 X 10(-8) GY/S) WERE USED AS EXPERIMENTAL OBJECTS. DNA FOR THE ANALYSIS WAS EXTRACTED SEPARATELY FOR THE FLIES OF MALES AND FEMALES. RESTRICTION ENDONUCLEASES GLUL, GLAL WERE USED. RESTRICTION ANALYSIS HAS SHOWN THAT THERE ARE DIFFERENT DNA METHYLATED PATTERNS FOR MALES AND FEMALES AS FOR CONTROL AND EXPOSED VARIANTS. AT THE CHRONIC IRRADIATION THERE WAS THE DECLINE OF METHYLATION LEVEL AT THE ENZYMES GLUL, GLAL SITES RECOGNITION. 2010 6 6514 20 TRANSCRIPTIONAL ACTIVATION OF THE GP91PHOX NADPH OXIDASE SUBUNIT BY TPA IN HL-60 CELLS. THE EXPOSURE TO EPIGENETIC EFFECTORS CAPABLE OF INDUCING COPIOUS PRODUCTION OF REACTIVE OXYGEN SPECIES (ROS) HAS BEEN ASSOCIATED WITH CHRONIC INFLAMMATION, TUMOR INITIATION, AND PROMOTION. THE OBJECTIVE OF THIS STUDY WAS TO EXAMINE THE REGULATION OF GP91PHOX, THE CATALYTIC SUBUNIT OF THE NADPH OXIDASE, AND THE KINETICS OF ROS PRODUCTION IN PROMYELOCYTIC LEUKEMIA HL-60 CELLS INDUCED WITH 12-O-TETRADECONYLPHORBOL-13-ACETATE (TPA). THE TREATMENT OF HL-60 CELLS WITH TPA (0.1 MICROM) INDUCED CELLULAR DIFFERENTIATION, WHICH WAS FOLLOWED AFTER 48 H BY A TENFOLD INCREASE IN CHEMILUMINESCENCE FROM LUCIGENIN AND A 2.5-FOLD INCREASE IN THE INTRACELLULAR OXIDATION OF 2',7'-DICHOLOROFLUORESCIN (DCFH). WHEREAS HIGHER CONCENTRATIONS (1.0 MICROM) OF TPA DID NOT STIMULATE FURTHER ROS PRODUCTION, REPEATED STIMULATION WITH 0.1 MICROM TPA OF DIFFERENTIATED CELLS INDUCED A MODEST (1.2-FOLD) BUT RAPID (15 MIN) INCREASE IN CHEMILUMINESCENCE. IN CELLS TREATED WITH TPA, THE BURST IN ROS AT 48 H WAS PRECEDED BY ACCUMULATION AT 12 H OF GP91PHOX (8.8-FOLD) AND P47PHOX MRNA (THREEFOLD), WHEREAS UNTREATED CELLS CONTAINED STEADY-STATE LEVELS OF BOTH TRANSCRIPTS. TIME-COURSE EXPERIMENTS WITH ACTINOMYCIN D TO INHIBIT TRANSCRIPTION REVEALED THAT TPA DID NOT IMPROVE THE STABILITY OF GP91PHOX. IN TRANSIENT TRANSFECTIONS, LUCIFERASE REPORTER ACTIVITY DIRECTED FROM A 1.5-KB GP91PHOX PROMOTER FRAGMENT WAS ENHANCED THREEFOLD UPON TREATMENT WITH TPA FOR 24 H. WE CONCLUDE THAT TPA CAN COMMIT HL-60 CELLS TO DIFFERENTIATION AND ELICIT TRANSCRIPTION FROM THE PROXIMAL GP91PHOX PROMOTER. 2001 7 4226 19 METHYLATION IN PERICYTES AFTER ACUTE INJURY PROMOTES CHRONIC KIDNEY DISEASE. THE ORIGIN AND FATE OF RENAL MYOFIBROBLASTS IS NOT CLEAR AFTER ACUTE KIDNEY INJURY (AKI). HERE, WE DEMONSTRATE THAT MYOFIBROBLASTS WERE ACTIVATED FROM QUIESCENT PERICYTES (QPERICYTES) AND THE CELL NUMBERS INCREASED AFTER ISCHEMIA/REPERFUSION INJURY-INDUCED AKI (IRI-AKI). MYOFIBROBLASTS UNDERWENT APOPTOSIS DURING RENAL RECOVERY BUT ONE-FIFTH OF THEM SURVIVED IN THE RECOVERED KIDNEYS ON DAY 28 AFTER IRI-AKI AND THEIR CELL NUMBERS INCREASED AGAIN AFTER DAY 56. MICROARRAY DATA SHOWED THE DISTINCTIVE GENE EXPRESSION PATTERNS OF QPERICYTES, ACTIVATED PERICYTES (APERICYTES, MYOFIBROBLASTS), AND INACTIVATED PERICYTES (IPERICYTES) ISOLATED FROM KIDNEYS BEFORE, ON DAY 7, AND ON DAY 28 AFTER IRI-AKI. HYPERMETHYLATION OF THE ACTA2 REPRESSOR YBX2 DURING IRI-AKI RESULTED IN EPIGENETIC MODIFICATION OF IPERICYTES TO PROMOTE THE TRANSITION TO CHRONIC KIDNEY DISEASE (CKD) AND AGGRAVATED FIBROGENESIS INDUCED BY A SECOND AKI INDUCED BY ADENINE. MECHANISTICALLY, TRANSFORMING GROWTH FACTOR-BETA1 DECREASED THE BINDING OF YBX2 TO THE PROMOTER OF ACTA2 AND INDUCED YBX2 HYPERMETHYLATION, THEREBY INCREASING ALPHA-SMOOTH MUSCLE ACTIN EXPRESSION IN APERICYTES. DEMETHYLATION BY 5-AZACYTIDINE RECOVERED THE MICROVASCULAR STABILIZING FUNCTION OF APERICYTES, REVERSED THE PROFIBROTIC PROPERTY OF IPERICYTES, PREVENTED AKI-CKD TRANSITION, AND ATTENUATED FIBROGENESIS INDUCED BY A SECOND ADENINE-AKI. IN CONCLUSION, INTERVENTION TO ERASE HYPERMETHYLATION OF PERICYTES AFTER AKI PROVIDES A STRATEGY TO STOP THE TRANSITION TO CKD. 2020 8 6556 24 TRANSGENERATIONAL EFFECTS OF POLYETHYLENE MICROPLASTIC FRAGMENTS CONTAINING BENZOPHENONE-3 ADDITIVE IN DAPHNIA MAGNA. MATERNAL EXPOSURE TO MICROPLASTICS (MPS) PLAYS AN IMPORTANT ROLE IN THE FITNESS OF UNEXPOSED PROGENY. IN THIS STUDY, THE TRANSGENERATIONAL EFFECTS OF POLYETHYLENE MP FRAGMENTS (17.35 +/- 5.50 MICROM) CONTAINING BENZOPHENONE-3 (BP-3; 2.85 +/- 0.16% W/W) ON CHRONIC TOXICITY (21 D) IN DAPHNIA MAGNA WERE INVESTIGATED ACROSS FOUR GENERATIONS. ONLY D. MAGNA IN THE F0 GENERATION WAS EXPOSED TO MP FRAGMENTS, MP/BP-3 FRAGMENTS, AND BP-3 LEACHATE TO IDENTIFY THE TRANSGENERATIONAL EFFECT IN THE F3 GENERATION. THE MORTALITY OF D. MAGNA INDUCED BY MP AND MP/BP-3 FRAGMENTS WAS RECOVERED IN THE F3 GENERATION, BUT SOMATIC GROWTH AND REPRODUCTION SIGNIFICANTLY DECREASED COMPARED TO THE CONTROL. ADDITIONALLY, REPRODUCTION OF D. MAGNA EXPOSED TO BP-3 LEACHATE SIGNIFICANTLY DECREASED IN THE F3 GENERATION. THESE FINDINGS CONFIRMED THE TRANSGENERATIONAL EFFECTS OF MP FRAGMENT AND BP-3 ADDITIVE ON D. MAGNA. PARTICULARLY, THE ADVERSE EFFECT ON D. MAGNA REPRODUCTION SEEMED TO BE CUMULATIVE ACROSS FOUR GENERATIONS FOR MP/BP-3 FRAGMENTS, WHILE IT WAS AN ACCLIMATION TREND FOR BP-3 LEACHATE. HOWEVER, THERE WAS NO SIGNIFICANT DIFFERENCE IN GLOBAL DNA METHYLATION IN D. MAGNA ACROSS FOUR GENERATIONS, THUS REQUIRING A GENE-SPECIFIC DNA METHYLATION STUDY TO IDENTIFY DIFFERENT EPIGENETIC TRANSGENERATIONAL INHERITANCE. 2022 9 4020 23 LOW-MOLECULAR-WEIGHT FIBROBLAST GROWTH FACTOR 2 ATTENUATES HEPATIC FIBROSIS BY EPIGENETIC DOWN-REGULATION OF DELTA-LIKE1. LIVER FIBROSIS, A MAJOR CAUSE OF END-STAGE LIVER DISEASES, IS CLOSELY REGULATED BY MULTIPLE GROWTH FACTORS AND CYTOKINES. THE CORRELATION OF FIBROBLAST GROWTH FACTOR 2 (FGF2) WITH CHRONIC LIVER INJURY HAS BEEN REPORTED, BUT THE EXACT FUNCTIONS OF DIFFERENT FGF2 ISOFORMS IN LIVER FIBROGENESIS REMAIN UNCLEAR. HERE, WE REPORT ON THE DIFFERENTIAL EXPRESSION PATTERNS AND FUNCTIONS OF LOW- AND HIGH-MOLECULAR-WEIGHT FGF2 (NAMELY, FGF2(LMW) AND FGF2(HMW) , RESPECTIVELY) IN HEPATIC FIBROGENESIS USING A CCL4 -INDUCED MOUSE LIVER FIBROSIS MODEL. FGF2(HMW) DISPLAYED A ROBUST INCREASE IN CCL4 -INDUCED HEPATIC FIBROSIS AND PROMOTED FIBROGENESIS. IN CONTRAST, ENDOGENOUS FGF2(LMW) EXHIBITED A SLIGHT INCREASE IN HEPATIC FIBROSIS AND SUPPRESSED THIS PATHOLOGICAL PROGRESSION. MOREOVER, EXOGENOUS ADMINISTRATION OF RECOMBINANT FGF2(LMW) POTENTLY AMELIORATED CCL4 -INDUCED LIVER FIBROSIS. MECHANISTICALLY, WE SHOWED THAT FGF2(LMW) TREATMENT ATTENUATED HEPATIC STELLATE CELL ACTIVATION AND FIBROSIS BY EPIGENETIC DOWN-REGULATION OF DELTA-LIKE 1 EXPRESSION THROUGH THE P38 MITOGEN-ACTIVATED PROTEIN KINASE PATHWAY. CONCLUSION: FGF2(LMW) AND FGF2(HMW) HAVE DISTINCT ROLES IN LIVER FIBROGENESIS. THESE FINDINGS DEMONSTRATE A POTENT ANTIFIBROTIC EFFECT OF FGF2(LMW) ADMINISTRATION, WHICH MAY PROVIDE A NOVEL APPROACH TO TREAT CHRONIC LIVER DISEASES. 2015 10 385 20 AN IMMORTALIZED CELL LINE DERIVED FROM RENAL ERYTHROPOIETIN-PRODUCING (REP) CELLS DEMONSTRATES THEIR POTENTIAL TO TRANSFORM INTO MYOFIBROBLASTS. THE ERYTHROID GROWTH FACTOR ERYTHROPOIETIN (EPO) IS PRODUCED BY RENAL INTERSTITIAL FIBROBLASTS, CALLED REP (RENAL EPO-PRODUCING) CELLS, IN A HYPOXIA-INDUCIBLE MANNER. IN CHRONIC KIDNEY DISEASE (CKD), REP CELLS LOSE THEIR EPO-PRODUCTION ABILITY, LEADING TO RENAL ANAEMIA. CONCURRENTLY, REP CELLS ARE SUGGESTED TO BE TRANSFORMED INTO MYOFIBROBLASTS, WHICH ARE THE MAJOR PLAYER OF RENAL FIBROSIS. ALTHOUGH ESTABLISHMENT OF CULTURED CELL LINES DERIVED FROM REP CELLS HAS BEEN A LONG-TERM CHALLENGE, WE HERE SUCCESSFULLY ESTABLISHED A REP-CELL-DERIVED IMMORTALIZED AND CULTIVABLE CELL LINE (REPLIC CELLS) BY USING A GENETICALLY MODIFIED MOUSE LINE. REPLIC CELLS EXHIBITED MYOFIBROBLASTIC PHENOTYPES AND LOST THEIR EPO-PRODUCTION ABILITY, REFLECTING THE SITUATION IN RENAL FIBROSIS. ADDITIONALLY, WE FOUND THAT CELL-AUTONOMOUS TGFBETA SIGNALLING CONTRIBUTES TO MAINTENANCE OF THE MYOFIBROBLASTIC FEATURES OF REPLIC CELLS. FURTHERMORE, THE PROMOTERS OF GENES FOR EPO AND HIF2ALPHA, A MAJOR ACTIVATOR OF EPO GENE EXPRESSION, WERE HIGHLY METHYLATED IN REPLIC CELLS. THUS, THESE RESULTS STRONGLY SUPPORT OUR CONTENTION THAT REP CELLS ARE THE ORIGIN OF MYOFIBROBLASTS IN FIBROTIC KIDNEYS AND DEMONSTRATE THAT CELL-AUTONOMOUS TGFBETA SIGNALLING AND EPIGENETIC SILENCING ARE INVOLVED IN RENAL FIBROSIS AND RENAL ANAEMIA, RESPECTIVELY, IN CKD. THE REPLIC CELL LINE IS A USEFUL TOOL TO FURTHER INVESTIGATE THE MOLECULAR MECHANISMS UNDERLYING RENAL FIBROSIS. 2019 11 5100 28 POLYCHLORINATED BIPHENYLS (PCBS) ALTER DNA METHYLATION AND GENOMIC INTEGRITY OF SHEEP FETAL CELLS IN A SIMPLIFIED IN VITRO MODEL OF PREGNANCY EXPOSURE. POLYCHLORINATED BIPHENYLS (PCBS) ARE PERSISTENT ORGANIC POLLUTANTS UBIQUITOUSLY DETECTABLE IN THE ENVIRONMENT AND IN THE FOOD CHAIN. PRENATAL EXPOSURE TO PCBS NEGATIVELY AFFECTS FETAL DEVELOPMENT AND PRODUCES LONG-TERM DETRIMENTAL EFFECTS ON CHILD HEALTH. THE PRESENT STUDY SOUGHT TO EVALUATE THE CYTOTOXIC AND GENOTOXIC EFFECTS OF CHRONIC PCB EXPOSURE ON FETAL CELLS DURING PREGNANCY. TO THIS AIM, SHEEP EMBRYONIC FIBROBLASTS (SEF) AND AMNIOCYTES (SA) WERE CULTURED IN VITRO IN THE PRESENCE OF LOW DOSES OF PCBS FOR A PERIOD OF 120DAYS, COMPARABLE TO THE FULL TERM OF OVINE PREGNANCY. CELLULAR PROLIFERATION RATES, GLOBAL DNA METHYLATION, CHROMOSOME INTEGRITY, AND MARKERS OF DNA DAMAGE WERE EVALUATED AT DIFFERENT TIME POINTS. MOREOVER, SEF TREATED WITH PCBS FOR 60DAYS WERE LEFT UNTREATED FOR ONE FURTHER MONTH AND THEN EXAMINED IN ORDER TO EVALUATE THE REVERSIBILITY OF PCB-INDUCED EPIGENETIC DEFECTS. PCB-TREATED SEF WERE MORE SENSITIVE THAN SA TREATED WITH PCBS, IN TERMS OF LOW CELL PROLIFERATION, AND INCREASED DNA DAMAGE AND GLOBAL DNA METHYLATION, WHICH WERE STILL DETECTABLE AFTER INTERRUPTION OF PCB TREATMENT. THESE DATA INDICATE THAT CHRONIC EXPOSURE OF FETAL CELLS TO PCBS CAUSES PERMANENT GENOMIC AND EPIGENETIC INSTABILITY, WHICH MAY INFLUENCE BOTH PRENATAL AND POST-NATAL GROWTH UP TO ADULTHOOD. OUR IN VITRO MODEL OFFER A SIMPLE AND CONTROLLED MEANS OF STUDYING THE EFFECTS OF DIFFERENT CONTAMINANTS ON FETAL CELLS - ONE THAT COULD SET THE STAGE FOR TARGETED IN VIVO STUDIES. 2018 12 3192 22 HDAC INHIBITION COUNTERACTS METASTATIC RE-ACTIVATION OF PROSTATE CANCER CELLS INDUCED BY CHRONIC MTOR SUPPRESSION. THIS STUDY WAS DESIGNED TO INVESTIGATE WHETHER EPIGENETIC MODULATION BY HISTONE DEACETYLASE (HDAC) INHIBITION MIGHT CIRCUMVENT RESISTANCE TOWARDS THE MECHANISTIC TARGET OF RAPAMYCIN (MTOR) INHIBITOR TEMSIROLIMUS IN A PROSTATE CANCER CELL MODEL. PARENTAL (PAR) AND TEMSIROLIMUS-RESISTANT (RES) PC3 PROSTATE CANCER CELLS WERE EXPOSED TO THE HDAC INHIBITOR VALPROIC ACID (VPA), AND TUMOR CELL ADHESION, CHEMOTAXIS, MIGRATION, AND INVASION WERE EVALUATED. TEMSIROLIMUS RESISTANCE WAS CHARACTERIZED BY REDUCED BINDING OF PC3(RES) CELLS TO ENDOTHELIUM, IMMOBILIZED COLLAGEN, AND FIBRONECTIN, BUT INCREASED ADHESION TO LAMININ, AS COMPARED TO THE PARENTAL CELLS. CHEMOTAXIS, MIGRATION, AND INVASION OF PC3(RES) CELLS WERE ENHANCED FOLLOWING TEMSIROLIMUS RE-TREATMENT. INTEGRIN ALPHA AND BETA RECEPTORS WERE SIGNIFICANTLY ALTERED IN PC3(RES) COMPARED TO PC3(PAR) CELLS. VPA SIGNIFICANTLY COUNTERACTED TEMSIROLIMUS RESISTANCE BY DOWN-REGULATING TUMOR CELL(-)MATRIX INTERACTION, CHEMOTAXIS, AND MIGRATION. EVALUATION OF INTEGRIN EXPRESSION IN THE PRESENCE OF VPA REVEALED A SIGNIFICANT DOWN-REGULATION OF INTEGRIN ALPHA5 IN PC3(RES) CELLS. BLOCKING STUDIES DEMONSTRATED A CLOSE ASSOCIATION BETWEEN ALPHA5 EXPRESSION ON PC3(RES) AND CHEMOTAXIS. IN THIS IN VITRO MODEL, TEMSIROLIMUS RESISTANCE DROVE PROSTATE CANCER CELLS TO BECOME HIGHLY MOTILE, WHILE HDAC INHIBITION REVERSED THE METASTATIC ACTIVITY. THE VPA-INDUCED INHIBITION OF METASTATIC ACTIVITY WAS ACCOMPANIED BY A LOWERED INTEGRIN ALPHA5 SURFACE LEVEL ON THE TUMOR CELLS. 2018 13 4528 21 MULTIGENERATIONAL EFFECTS OF CADMIUM ON THE LIFESPAN AND FERTILITY OF DROSOPHILA MELANOGASTER. ALTHOUGH THE DAMAGE AND TOLERANCE MECHANISMS OF CD STRESS ARE KNOWN, THE DATA ON GENETIC RISK ARE LIMITED. THE AIM OF THIS STUDY WAS TO ASSESS THE CHRONIC TOXICITY OF CD, GENETIC RESPONSES, AND MULTIGENERATIONAL EFFECTS IN FIVE GENERATIONS OF DROSOPHILA MELANOGASTER. FOR EACH GENERATION, LIFESPAN AND FERTILITY WERE STATISTICALLY ANALYSED AND THE EXPRESSION OF APOPTOSIS- (P53 AND CASPASE-3) AND EPIGENESIS-RELATED (DDNMT2 AND DMBD2/3) GENES WAS EXAMINED. LIFESPAN AND FERTILITY SIGNIFICANTLY DECLINED UNDER CD STRESS AND THESE EFFECTS WERE MAINTAINED FOR TWO GENERATIONS AND ONE GENERATION, RESPECTIVELY, WHEN CD STRESS WAS REMOVED. THE EXPRESSION OF P53 AND CASPASE-3 WAS SIGNIFICANTLY UP-REGULATED AFTER EXPOSURE, SUGGESTING THAT APOPTOSIS CONTRIBUTES TO THE RESISTANCE MECHANISM. THEIR ALTERED EXPRESSION WAS RETAINED FOR TWO GENERATIONS. FURTHERMORE, HIGH EXPRESSION OF DDNMT2 AND DMBD2/3 ACCOMPANIED CD EXPOSURE, WHICH WAS PASSED ON TO THREE GENERATIONS, SUGGESTING THAT GENETIC MODIFICATIONS IN APOPTOSIS-RELATED GENES ARE CARRIED TO THE OFFSPRING THROUGH EPIGENETIC REGULATION. 2020 14 1684 23 DRUG-TOLERANT CANCER CELLS SHOW REDUCED TUMOR-INITIATING CAPACITY: DEPLETION OF CD44 CELLS AND EVIDENCE FOR EPIGENETIC MECHANISMS. CANCER STEM CELLS (CSCS) POSSESS HIGH TUMOR-INITIATING CAPACITY AND HAVE BEEN REPORTED TO BE RESISTANT TO THERAPEUTICS. VICE VERSA, THERAPY-RESISTANT CANCER CELLS SEEM TO MANIFEST CSC PHENOTYPES AND PROPERTIES. IT HAS BEEN GENERALLY ASSUMED THAT DRUG-RESISTANT CANCER CELLS MAY ALL BE CSCS ALTHOUGH THE GENERALITY OF THIS ASSUMPTION IS UNKNOWN. HERE, WE CHRONICALLY TREATED DU145 PROSTATE CANCER CELLS WITH ETOPOSIDE, PACLITAXEL AND SOME EXPERIMENTAL DRUGS (I.E., STAUROSPORINE AND 2 PACLITAXEL ANALOGS), WHICH LED TO POPULATIONS OF DRUG-TOLERANT CELLS (DTCS). SURPRISINGLY, THESE DTCS, WHEN IMPLANTED EITHER SUBCUTANEOUSLY OR ORTHOTOPICALLY INTO NOD/SCID MICE, EXHIBITED MUCH REDUCED TUMORIGENICITY OR WERE EVEN NON-TUMORIGENIC. DRUG-TOLERANT DLD1 COLON CANCER CELLS SELECTED BY A SIMILAR CHRONIC SELECTION PROTOCOL ALSO DISPLAYED REDUCED TUMORIGENICITY WHEREAS DRUG-TOLERANT UC14 BLADDER CANCER CELLS DEMONSTRATED EITHER INCREASED OR DECREASED TUMOR-REGENERATING CAPACITY. DRUG-TOLERANT DU145 CELLS DEMONSTRATED LOW PROLIFERATIVE AND CLONOGENIC POTENTIAL AND WERE VIRTUALLY DEVOID OF CD44(+) CELLS. PROSPECTIVE KNOCKDOWN OF CD44 IN DU145 CELLS INHIBITED CELL PROLIFERATION AND TUMOR REGENERATION, WHEREAS RESTORATION OF CD44 EXPRESSION IN DRUG-TOLERANT DU145 CELLS INCREASED CELL PROLIFERATION AND PARTIALLY INCREASED TUMORIGENICITY. INTERESTINGLY, DRUG-TOLERANT DU145 CELLS SHOWED BOTH INCREASES AND DECREASES IN MANY "STEMNESS" GENES. FINALLY, EVIDENCE WAS PROVIDED THAT CHRONIC DRUG EXPOSURE GENERATED DTCS VIA EPIGENETIC MECHANISMS INVOLVING MOLECULES SUCH AS CD44 AND KDM5A. OUR RESULTS THUS REVEAL THAT 1) NOT ALL DTCS ARE NECESSARILY CSCS; 2) CONVENTIONAL CHEMOTHERAPEUTIC DRUGS SUCH AS TAXOL AND ETOPOSIDE MAY DIRECTLY TARGET CD44(+) TUMOR-INITIATING CELLS; AND 3) DTCS GENERATED VIA CHRONIC DRUG SELECTION INVOLVE EPIGENETIC MECHANISMS. 2011 15 1816 21 EFFECTS OF CHRONIC EXPOSURE TO BENZOPHENONE AND DICLOFENAC ON DNA METHYLATION LEVELS AND REPRODUCTIVE SUCCESS IN A MARINE COPEPOD. THE UV-FILTER BENZOPHENONE AND THE ANTI-INFLAMMATORY DICLOFENAC ARE COMMONLY DETECTED IN THE ENVIRONMENT. THE AIM OF THIS STUDY WAS TO ASSESS THE MULTIGENERATIONAL EFFECTS OF CHRONIC EXPOSURE TO LOW CONCENTRATIONS OF THESE CHEMICALS ON TOXICITY AND DNA METHYLATION LEVELS IN THE COPEPOD GLADIOFERENS PECTINATUS. ACUTE TOXICITY TESTS WERE CONDUCTED TO DETERMINE THE SENSITIVITY OF G. PECTINATUS TO THE CHEMICALS. ALL CHEMICALS IMPACTED BREEDING, HATCHING AND EGG VIABILITY. DICLOFENAC (1 MG.L(-1)) REDUCED THE NUMBER OF EGGS PER GRAVID FEMALE. BENZOPHENONE (0.5 MG.L(-1)) DECREASED EGG HATCHING SUCCESS. EXPOSURE TO THE REFERENCE TOXICANT COPPER (0.02 MG.L(-1)) LED TO UNSUCCESSFUL HATCHING. EFFECTS ON DNA METHYLATION WAS ESTIMATED BY THE PERCENTAGE OF 5- METHYLCYTOSINE. THE TREATMENTS RESULTED IN STRONG DIFFERENCES IN DNA METHYLATION WITH INCREASED METHYLATION IN THE EXPOSED ANIMALS. THE TWO CHEMICALS IMPACTED BOTH EGG VIABILITY AND THE INDUCTION OF DIFFERENTIAL DNA METHYLATION, SUGGESTING POTENTIAL INTRA- AND TRANS-GENERATIONAL EVOLUTIONARY EFFECTS. 2018 16 227 22 ADAPTATION OF AN OUTBREAKING INSECT DEFOLIATOR TO CHRONIC NUTRITIONAL STRESS. DURING INSECT OUTBREAKS, THE HIGH NUMBER OF INDIVIDUALS FEEDING ON ITS HOST PLANT CAUSES A DEPLETION OF THE FOOD SOURCE. REDUCED AVAILABILITY AND DECREASED QUALITY OF NUTRIENTS NEGATIVELY INFLUENCE LIFE-HISTORY TRAITS OF INSECTS DRIVING THEM TO DEVELOP ADAPTIVE STRATEGIES TO PERSIST IN THE ENVIRONMENT. IN A LABORATORY EXPERIMENT WITH THREE REPETITIONS, WE TESTED THE EFFECT OF CHRONIC NUTRITIONAL STRESS ON SPRUCE BUDWORM PERFORMANCE DURING THREE GENERATIONS TO DETERMINE THE ADAPTIVE STRATEGIES EMPLOYED BY THE INSECT TO DEAL WITH A SELECTION PRESSURE PRODUCED BY LOW-QUALITY DIET. OUR RESULTS SHOW THAT ALL TESTED LIFE-HISTORY TRAITS (MORTALITY, DEVELOPMENTAL TIME, PUPAL MASS, GROWTH RATE AND FEMALE FECUNDITY) BUT FEMALE FERTILITY WERE NEGATIVELY INFLUENCED BY THE LOW-QUALITY DIET SIMULATING FOOD DEPLETION DURING OUTBREAK CONDITIONS. HOWEVER, ESPECIALLY FEMALES IN THE THIRD GENERATION UNDER CHRONIC NUTRITIONAL STRESS SHOW AN ADAPTIVE RESPONSE IN LIFE-HISTORY TRAITS WHEN COMPARED TO THOSE REARED ONLY ONE GENERATION ON LOW-QUALITY DIET. LARVAL DEVELOPMENTAL TIME SIGNIFICANTLY DECREASED AND PUPAL MASS, GROWTH RATE AND FECUNDITY SIGNIFICANTLY INCREASED. THE STUDY DEMONSTRATES THE CAPACITY OF SPRUCE BUDWORM TO REACT TO CHRONIC NUTRITIONAL STRESS WITH ADAPTATIONS THAT MAY BE CAUSED BY EPIGENETIC PARENTAL EFFECTS. THIS INFORMATION CAN HELP TO UNDERSTAND THE COURSE OF AN OUTBREAK ESPECIALLY AT PEAK DENSITIES AND DURING THE COLLAPSE. 2015 17 512 28 ASSOCIATION OF SAT-A AND ALU METHYLATION STATUS WITH HCV-INDUCED CHRONIC LIVER DISEASE AND HEPATOCELLULAR CARCINOMA. BACKGROUND: THE COMBINATION OF EPIGENETIC AND GENETIC ABNORMALITIES CONTRIBUTES TOGETHER TO THE DEVELOPMENT OF LIVER CANCER. THE METHYLATION STATUS OF THE REPETITIVE ELEMENTS (RES) IN DNA HAS BEEN INVESTIGATED IN A VARIETY OF HUMAN ILLNESSES. HOWEVER, THE METHYLATION PATTERNS OF SAT-ALPHA AND ALU RES IN CHRONIC LIVER DISEASE (CLD) AND HEPATOCELLULAR CARCINOMA (HCC) CAUSED BY HEPATITIS C VIRUS (HCV) HAVE NEVER BEEN STUDIED BEFORE. METHODOLOGY: IN THIS STUDY, 3 GROUPS OF PARTICIPANTS INCLUDING 50 PATIENTS HAVING HCV-INDUCED CLD, 50 PATIENTS HAVING HCV-INDUCED HCC, AND 46 HEALTHY SUBJECTS WERE SUBJECTED TO MEASUREMENT OF SAT-ALPHA AND ALU METHYLATION USING THE QUANTITATIVE METHYLIGHT ASSAY. RESULTS: SAT-ALPHA AND ALU METHYLATION PERCENTAGES DECREASED SIGNIFICANTLY IN BOTH CLD AND HCC, COMPARED TO CONTROL. ALSO, A SIGNIFICANT SAT-ALPHA HYPOMETHYLATION WAS DETECTED IN HCC, COMPARED TO CLD. IN ADDITION, SAT-ALPHA AND ALU METHYLATION SHOWED A SIGNIFICANT DECLINE AS LESION SIZE GREW. HOWEVER, ONLY SAT-ALPHA HYPOMETHYLATION WAS SIGNIFICANTLY INCREASED IN ASSOCIATION WITH PORTAL VEIN THROMBOSIS AND THE MELD SCORE. SAT-ALPHA METHYLATION PERCENTAGE HAD THE HIGHEST SENSITIVITY AND SPECIFICITY FOR DIAGNOSING HCC (100% AND 84.4%) FOLLOWED BY ALPHA-FETOPROTEIN (80% AND 84.4%) AND ALU METHYLATION (66% AND 61.5%). FURTHERMORE, THERE WAS A STRONG POSITIVE CORRELATION BETWEEN SAT-ALPHA AND ALU METHYLATION. CONCLUSIONS: MEASURING SAT-ALPHA AND ALU METHYLATION PROVIDES US WITH A NEW TOOL FOR EARLY DETECTING HCV-INDUCED CLD AND HEPATOCARCINOGENESIS. SAT-ALPHA HAS THE POTENTIAL TO BE UTILIZED AS AN INDEPENDENT PREDICTIVE PARAMETER FOR HCC DEVELOPMENT AND PROGRESSION BECAUSE OF ITS ABILITY TO DISTINGUISH BETWEEN CLD AND HCC WITH THEIR DIFFERENT MELD SCORES. 2022 18 6555 22 TRANSGENERATIONAL EFFECTS OF GAMMA RADIATION DOSE AND DOSE RATE ON DROSOPHILA FLIES IRRADIATED AT AN EARLY EMBRYONAL STAGE. IONIZING RADIATION (IR) KILLS CELLS MAINLY THROUGH INDUCTION OF DNA DAMAGES AND THE SURVIVING CELLS MAY SUFFER FROM MUTATIONS. TRANSGENERATIONAL EFFECTS OF IR ARE WELL DOCUMENTED, BUT THE EXACT MECHANISMS UNDERLYING THEM ARE LESS WELL UNDERSTOOD; THEY INCLUDE INDUCTION OF MUTATIONS IN GERM CELLS AND EPIGENETIC INHERITANCE. PREVIOUSLY, EFFECTS IN THE OFFSPRING OF MICE AND ZEBRAFISH EXPOSED TO IR HAVE BEEN REPORTED. A FEW STUDIES ALSO SHOWED INDICATIONS OF TRANSGENERATIONAL EFFECTS OF RADIATION IN HUMANS, PARTICULARLY IN NUCLEAR POWER WORKERS. IN THE PRESENT PROJECT, SHORT- AND LONG-TERM EFFECTS OF LOW-DOSE-RATE (LDR; 50 AND 97 MGY/H) AND HIGH-DOSE-RATE (HDR; 23.4, 47.1 AND 495 GY/H) IR IN DROSOPHILA EMBRYOS WERE INVESTIGATED. THE EMBRYOS WERE IRRADIATED AT DIFFERENT DOSES AND DOSE RATES AND RADIOSENSITIVITY AT DIFFERENT DEVELOPMENTAL STAGES WAS INVESTIGATED. ALSO, THE SURVIVAL OF LARVAE, PUPAE AND ADULTS DEVELOPED FROM EMBRYOS IRRADIATED AT AN EARLY STAGE (30 MIN AFTER EGG LAYING) WERE STUDIED. THE LARVAL CRAWLING AND PUPATION HEIGHT ASSAYS WERE APPLIED TO INVESTIGATE RADIATION EFFECTS ON LARVAL LOCOMOTION AND PUPATION BEHAVIOR, RESPECTIVELY. IN PARALLEL, THE OFFSPRING FROM 3 GY IRRADIATED EARLY-STAGE EMBRYOS WERE FOLLOWED UP TO 12 GENERATIONS AND ABNORMAL PHENOTYPES WERE STUDIED. ACUTE EXPOSURE OF EMBRYOS AT DIFFERENT STAGES OF DEVELOPMENT SHOWED THAT THE EARLY STAGE EMBRYO IS THE MOST SENSITIVE. THE EFFECTS ON LARVAL LOCOMOTION SHOWED NO SIGNIFICANT DIFFERENCES BETWEEN THE DOSE RATES BUT A SIGNIFICANT DECREASE OF LOCOMOTION ACTIVITY ABOVE 7 GY WAS OBSERVED. THE RESULTS INDICATE THAT EMBRYOS EXPOSED TO THE LOW DOSE RATES HAVE SHORTER ECLOSION TIMES. AT THE SAME CUMULATIVE DOSE (1 UP TO 7 GY), HDR IS MORE EMBRYOTOXIC THAN LDR. WE ALSO FOUND A RADIATION-INDUCED DEPIGMENTATION ON MALES (A5 SEGMENT OF THE DORSAL ABDOMEN, A5PIG(-)) THAT CAN BE TRANSMITTED UP TO 12 GENERATIONS. THE PHENOMENON DOES NOT FOLLOW THE CLASSICAL MENDELIAN LAWS OF SEGREGATION. 2022 19 5934 31 TARGETING FEATURES OF CURAXIN CBL0137 ON HEMATOLOGICAL MALIGNANCIES IN VITRO AND IN VIVO. THE ANTICANCER ACTIVITY OF CURAXIN CBL0137, A DNA-BINDING SMALL MOLECULE WITH CHROMATIN REMODULATING EFFECT, HAS BEEN DEMONSTRATED IN DIFFERENT CANCERS. HEREIN, A COMPARATIVE EVALUATION OF CBL0137 ACTIVITY WAS PERFORMED IN RESPECT TO ACUTE MYELOID LEUKEMIA (AML), ACUTE LYMPHOBLASTIC LEUKEMIA (ALL), CHRONIC MYELOID LEUKEMIA AND MULTIPLE MYELOMA (MM) CULTURED IN VITRO. MTT ASSAY SHOWED AML AND MM HIGHER SENSITIVITY TO CBL0137'S CYTOSTATIC EFFECT COMPARATIVELY TO OTHER HEMATOLOGICAL MALIGNANCY CELLS. FLOW CYTOMETRY CELL CYCLE ANALYSIS REVEALED AN INCREASE IN SUBG1 AND G2/M POPULATIONS AFTER CBL0137 CELL TREATMENT, BUT THE PREVALENT TYPE OF ARREST VARIED. APOPTOSIS ACTIVATION BY CBL0137 MEASURED BY ANNEXIN-V/PI DUAL STAINING WAS MORE ACTIVE IN AML AND MM CELLS. RT2 PCR ARRAY SHOWED THAT CHANGES CAUSED BY CBL0137 IN SIGNALING PATHWAYS INVOLVED IN CANCER PATHOGENESIS WERE MORE INTENSIVE IN AML AND MM CELLS. ON THE MURINE MODEL OF AML WEHI-3, CBL0137 SHOWED SIGNIFICANT ANTICANCER EFFECTS IN VIVO, WHICH WERE EVALUATED BY CORRESPONDING CHANGES IN SPLEEN AND LIVER. THUS, MORE PRONOUNCED ANTICANCER EFFECTS OF CBL0137 IN VITRO WERE OBSERVED IN RESPECT TO AML AND MM. EXPERIMENTS IN VIVO ALSO INDICATED THE PERSPECTIVE OF CBL0137 USE FOR AML TREATMENT. THIS IN ACCORDANCE WITH THE FRONTLINE TREATMENT APPROACH IN AML USING EPIGENETIC DRUGS. 2023 20 3912 20 LIFE-SPAN EXTENSION BY CALORIC RESTRICTION IS DETERMINED BY TYPE AND LEVEL OF FOOD REDUCTION AND BY REPRODUCTIVE MODE IN BRACHIONUS MANJAVACAS (ROTIFERA). WE MEASURED LIFE SPAN AND FECUNDITY OF THREE REPRODUCTIVE MODES IN A CLONE OF THE MONOGONONT ROTIFER BRACHIONUS MANJAVACAS SUBJECTED TO CHRONIC CALORIC RESTRICTION (CCR) OVER A RANGE OF FOOD CONCENTRATIONS OR TO INTERMITTENT FASTING (IF). IF INCREASED LIFE SPAN 50%-70% FOR ALL THREE MODES, WHEREAS CCR INCREASED LIFE SPAN OF ASEXUAL FEMALES DERIVED FROM SEXUALLY OR ASEXUALLY PRODUCED EGGS, BUT NOT THAT OF SEXUAL FEMALES. THE MAIN EFFECT OF CR ON BOTH ASEXUAL MODES WAS TO DELAY DEATH AT YOUNG AGES, RATHER THAN TO PREVENT DEATH AT MIDDLE AGES OR TO GREATLY EXTEND MAXIMUM LIFE SPAN; IN CONTRAST CR IN SEXUAL FEMALES GREATLY INCREASED THE LIFE SPAN OF A FEW LONG-LIVED INDIVIDUALS. LIFETIME FECUNDITY DID NOT DECREASE WITH CCR, SUGGESTING A LACK OF RESOURCE ALLOCATION TRADE-OFF BETWEEN SOMATIC MAINTENANCE AND REPRODUCTION. MULTIPLE OUTCOMES FOR A CLONAL LINEAGE INDICATE THAT DIFFERENT RESPONSES ARE ESTABLISHED THROUGH EPIGENETIC PROGRAMMING, WHEREAS DIFFERENCES IN LIFE-SPAN ALLOCATIONS SUGGEST THAT MULTIPLE GENETIC MECHANISMS MEDIATE LIFE-SPAN EXTENSION. 2013