grant

Endocrine disrupting chemical mixtures and bone health in adolescence

Organization UNIV OF NORTH CAROLINA CHAPEL HILLLocation CHAPEL HILL, UNITED STATESPosted 3 Sept 2021Deadline 30 Jun 2027
NIHUS FederalResearch GrantFY20250-11 years old12 year old12 years of age12-20 years old17 year old17 years of age2-dimensional21+ years old3-D3-Dimensional3DActive Follow-upAdolescenceAdolescentAdolescent YouthAdultAdult HumanAffectAgeAmericanAnimalsAnthropometryAutoregulationBackBiological MarkersBiostatistical MethodsBirthBloodBlood Reticuloendothelial SystemBone DensityBone DiseasesBone Mineral DensityBone MineralizationCAT scanCT X RayCT XrayCT imagingCT scanChemical ExposureChemicalsChildChild YouthChildhoodChildren (0-21)ChronicClinicClinicalCohort StudiesComputed TomographyConcurrent StudiesCross Sectional AnalysisCross-Sectional AnalysesCross-Sectional StudiesCross-Sectional SurveyDEXADXADataDevelopmentDietDisease Frequency SurveysDorsumDual-Energy X-Ray AbsorptiometryDual-Energy Xray AbsorptiometryEndocrineEndocrine DisrupterEndocrine Disrupting ChemicalsEndocrine DisruptorsEndocrine disrupting agentEnrollmentEnvironmentEnvironmental ExposureEpidemiologyEstersEvaluationExposure toFire RetardantsFlame RetardantsForearmFractureFutureGeometryGestationGoalsHealthHistoryHomeostasisHumanIndividualInterventionLaboratory StudyLifeLong-term cohort studyLongitudinal cohort studyMeasuresModern ManMorphologyMothersOhioOrganophosphatesOsteoporosisOsteoporotic riskOutcomePFASParticipantParturitionPeripheralPhysical activityPhysiologic calcificationPhysiological HomeostasisPoly-fluoroalkyl substancesPopulationPredispositionPregnancyProcessProspective StudiesPubertyPublic HealthRadialRadiusRecording of previous eventsRisk FactorsRisk ReductionSiteSusceptibilityTechniquesTomodensitometryUrineVisitWorkX-Ray CAT ScanX-Ray Computed TomographyX-Ray Computerized TomographyXray CAT scanXray Computed TomographyXray computerized tomographyactive followupadolescence (12-20)adulthoodage 12 yearsage 17 yearsagesbio-markersbiologic markerbiomarkerbonebone disorderbone fracturebone geometrybone healthbone imagingbone massbone scanningbone strengthbone turnovercatscanchemical associationclinical significanceclinically significantcomputed axial tomographycomputer tomographycomputerized axial tomographycomputerized tomographyconsumer productcritical perioddesigndesigningdevelopmentaldietsearly adolescenceearly adulthoodearly childhoodemerging adultendocrine disrupting compoundenrollepidemiologicepidemiologicalfollow upfollow-upfollowed upfollowupfracture riskhistoriesindexinginnovateinnovationinnovativejuvenilejuvenile humankidslater in lifelater lifemalemalleable riskmodifiable risknon-contrast CTnoncontrast CTnoncontrast computed tomographyolder adultolder adulthoodosteoporosis riskpediatricperfluorinated alkyl substancesperfluoroalkyl substancesperfluoroalkylated substancesphthalatespolyfluorinated alkyl substancespolyfluoroalkyl substancesprospectivereduce riskreduce risksreduce that riskreduce the riskreduce these risksreduces riskreduces the riskreducing riskreducing the riskrisk developing osteoporosisrisk factor for osteoporosisrisk-reducingseventeen year oldseventeen years of agesexskeletalskeletal imagingthree dimensionaltooltwelve year oldtwelve years of agetwo-dimensionalyoungster
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Full Description

Abstract
Low bone mineral density (BMD) during adolescence is associated with fractures in adolescence and

adulthood as well as increased risk of osteoporosis, a chronic bone disease affecting more than 10 million

older adults in the U.S. The majority of Americans are exposed to perfluoroalkyl substances, phthalates, and

organophosphate esters, synthetic endocrine disrupting chemicals (EDCs) that have adverse skeletal effects in

laboratory studies. In humans, these EDCs are associated with lower BMD in limited cross-sectional studies

and prospectively associated with lower BMD at age 12 years in our preliminary data. However, few studies

have assessed relationships of EDCs with bone health in adolescence, a period of rapid bone mineralization

that may be highly sensitive to environmental exposures and is strongly predictive of adult BMD. Therefore, the

overarching objective of our proposal is to determine whether exposure to individual EDCs or their mixtures

causes reduced bone accrual and strength in adolescence. We will address our aims within the Health

Outcomes and Measures of the Environment (HOME) Study, a prospective birth cohort study of mothers and

their children enrolled in Cincinnati, Ohio. The HOME Study has amassed detailed longitudinal exposure

biomarker measures and covariate data on participants from gestation through 12 years of age. We will

conduct a new follow-up visit of 225 participants at approximately 17 years of age to measure EDC

biomarkers; perform detailed skeletal assessments; and collect information on diet, physical activity,

anthropometry, and pubertal status. Using these data, we will determine whether EDC exposures are

associated with peripheral quantitative computed tomography measures of volumetric BMD, bone geometry,

and strength strain index at age 17 years (Aim 1); dual-energy X-ray absorptiometry measures of areal BMD at

age 17 years and rate of aBMD accrual from age 12 to 17 years (Aim 2); and fracture history at age 17 years

(Aim 3). We will elucidate the impact of lifetime cumulative EDC exposures and identify periods of heightened

susceptibility by applying sophisticated statistical approaches including Bayesian and lagged kernel machine

regression and latent profile analysis. This work will inform the development of targeted interventions for

optimizing bone health in adolescence with the long-term goal of reducing risk of fractures and osteoporosis

throughout life.

Grant Number: 5R01ES033252-05
NIH Institute/Center: NIH

Principal Investigator: Jessie Buckley

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