grant

Obesogenic origins of maternal and child metabolic health involving dolutegravir (ORCHID)

Organization COLUMBIA UNIVERSITY HEALTH SCIENCESLocation NEW YORK, UNITED STATESPosted 25 Sept 2020Deadline 30 Jun 2026
NIHUS FederalResearch GrantFY20240-11 years old1st trimesterACRP30 proteinAIDS VirusAcquired Immune Deficiency Syndrome VirusAcquired Immunodeficiency Syndrome VirusAddressAdipocytesAdipose CellAdipose tissueAffectAirAnti-InflammatoriesAnti-Inflammatory AgentsAnti-Retroviral AgentsAnti-inflammatoryArachidonic AcidsAutoregulationB cell differentiation factorB cell stimulating factor 2B-Cell Differentiation FactorB-Cell Differentiation Factor-2B-Cell Stimulatory Factor-2BCDFBSF-2BSF2Breast MilkBreastmilkC-PeptideCaloric IntakeChildChild HealthChild YouthChildren (0-21)ChronicClinicalComplexCord BloodDataDocosahexaenoateDocosahexaenoic AcidsDocosahexenoic AcidsDrugsDysfunctionDyslipidemiasEarly Placental PhaseEicosanoidsEicosapentaenoic AcidEnergy ExpenditureEnergy IntakeEnergy MetabolismEnrollmentEquilibriumExposure toFat CellsFatty AcidsFatty TissueFemale HealthFibrosisFirst Pregnancy TrimesterFirst TrimesterFunctional disorderFundingGestationGoalsHIVHIV InfectionsHPGFHTLV-III InfectionsHTLV-III-LAV InfectionsHealthHepatocyte-Stimulating FactorHomeostasisHuman Immunodeficiency VirusesHuman MilkHuman Mother's MilkHuman T-Lymphotropic Virus Type III InfectionsHumulin RHungerHybridoma Growth FactorHypertrophyHypoxiaHypoxicIFN-beta 2IFNB2IL-6IL6 ProteinInflammationInflammatoryInsulinInsulin ResistanceIntegrase InhibitorsInterleukin-6InterventionIntervention StrategiesLAV-HTLV-IIILeptinLifeLife CycleLife Cycle StagesLinkLipidsLipocytesLymphadenopathy-Associated VirusLysolecithinsLysophosphatidylcholinesMGI-2Mammary Gland MilkMaternal HealthMature LipocyteMature fat cellMeasuresMedicationMelanocortin-1MetabolicMetabolic DiseasesMetabolic DisorderMitochondriaMother's MilkMothersMyeloid Differentiation-Inducing ProteinN-3 polyunsaturated fatty acidN-6 Fatty AcidsNational Institutes of HealthNeonatalNovolin ROb Gene ProductOb ProteinObese Gene ProductObese ProteinObesityOmega-3 Fatty AcidsOmega-3 PUFAOmega-3 Polyunsaturated Fatty AcidOmega-6Omega-6 Fatty AcidsOmega-6 PUFAsOmega3Over weightOverweightOxygen DeficiencyPathway interactionsPersonsPharmaceutical PreparationsPhosphatidesPhospholipidsPhysiological HomeostasisPhysiopathologyPlasmacytoma Growth FactorPlayPlethysmographyPolyunsaturated Fatty AcidsPopulationPostpartum PeriodPregnancyPregnant WomenPublic HealthR-Series Research ProjectsR01 MechanismR01 ProgramRegimenRegular InsulinResearch GrantsResearch InfrastructureResearch Project GrantsResearch ProjectsResearch SupportRespirationRestRisk ReductionRoleSatiationSeriesShapesSouth AfricaTechniquesThesaurismosisTimeTimnodonic AcidTriacylglycerolTriglyceridesUmbilical Cord BloodUnited States National Institutes of HealthVirus-HIVWeightWeight GainWeight IncreaseWomanWomen's Healthadipocyte complement-related protein 30-kDaadipocyte, C1q and collagen domain containing proteinadiponectinadiposeadiposityalpha-Melanotropinanti-retroviralantiretroviral therapyantiretroviral treatmentapM-1 proteinapM1 (adipose-specific) proteinbalancebalance functionbody weight gainbody weight increasecaloric dietary contentco-morbidco-morbiditycohortcomorbidityconnecting peptidecorpulencecritical perioddesigndesigningdrug/agenteicosapentanoic acidenrollexcessive weight gainexpectant motherexpecting motherexposed in uteroextreme weight gainfetalfetal cord bloodfetal exposuregestational weight gainghrelinin uteroin utero exposureinsightinsulin resistantinsulin toleranceinterferon beta 2interventional strategyintestinal fatty acid binding proteinintra-uterine environmental exposureintrauterine environmental exposurekidslife coursematernal milkmaternal outcomemetabolism disordermetabolism measurementmetabolomicsmetabonomicsmitochondrialmother outcomen-3 Fatty Acidsn-3 PUFAn-3-PUFAobesigenicobesity during pregnancyobesity in pregnancyobesogenobesogenicomega-3pathophysiologypathwaypoor health outcomepost-partumpost-partum healthpost-partum weightpostpartum healthpostpartum weightpregnantpregnant mothersprenatal exposureprenatally exposedprepregnancyrecruitreduce riskreduce risksreduce that riskreduce the riskreduce these risksreduced health outcomereduces riskreduces the riskreducing riskreducing the riskrespiratory mechanismrisk-reducingsatietyscale upserious weight gainsevere weight gainsocial rolesubcutaneoussubdermalweightswhite adipose tissueworse health outcomewt gainyellow adipose tissueyoungsterα-MSHα-Melanocyte stimulating hormoneω-3 fatty acidsω-6
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Full Description

PROJECT ABSTRACT
More than 8 million people are living with HIV in South Africa (SA), including >250,000 women who become

pregnant annually, and >50% of SA women are overweight/obese.1 In SA and globally, Dolutegravir (DTG)-

based antiretroviral therapy (ART) is being scaled up as part of the preferred 1st-line ART regimen. However,

DTG has recently been implicated as an obesogen that is associated with increased weight and adipose tissue

gain compared to other antiretroviral agents.2,3 Obesity in pregnancy is associated with poor health outcomes

for both mother and child4-9 as pregnancy is a critical period during which exposures leading to alterations in

metabolic health may influence not only long-term maternal health but also fetal, neonatal, and ultimately child

health. For women living with HIV (WLHIV) and their children, these exposures are myriad, including HIV/ART,

weight gain, & obesity. The overall goal of our study is to investigate the impact of DTG in pregnancy

and its obesogenic effects on the metabolic health of women living with HIV (WLHIV) and their

children, compared to women without HIV and their children. To address this goal, we will leverage:

(i) existing NIH-funded research infrastructure in SA and (ii) the NIH large R01 mechanism to enroll 1900

pregnant women in the 1st trimester (633 WLHIV initiating DTG in pregnancy, 633 WLHIV continuing DTG use

from pre-pregnancy, and 633 women without HIV) and their children, following them to two years. Within this

cohort, we will first examine how HIV and/or DTG use (HIV/DTG) impacts longitudinal changes in weight and

adipose tissue mass in pregnancy using air displacement plethysmography. We will further investigate

pathways of excess gestational weight gain and adipose accrual by evaluating: a) the balance between caloric

intake and resting energy expenditure, b) markers of systemic and adipose inflammation, gut integrity, and

satiety/hunger, and c) subcutaneous adipose tissue (SAT) function and homeostasis. Following this, we will go

on to examine how HIV/DTG use in pregnancy and postpartum affects maternal metabolic health postpartum

(postpartum weight retention, adiposity, dysglycemia, insulin resistance, and dyslipidemia) as well as neonatal

and child metabolic health (weight, adiposity, insulin resistance and dyslipidemia). To understand whether

signature clusters of metabolites and lipid subspecies are associated with maternal and child metabolic health,

we will apply widely targeted metabolomics techniques to measure maternal (in pregnancy) and cord blood

metabolites, lipid subspecies, and eicosanoids. To address the different specific aims we will use a series of

nested substudies, including smaller nested cohorts and efficient case-cohort designs, within the main cohort.

This study will play a pivotal role in defining the obesogenic mechanisms and clinical consequences of DTG

use in pregnancy in WLHIV and their children. The results of our study will provide insights into metabolic

disease risk reduction in the context of HIV/ART, identify potential targets for interventions, and inform public

health approaches to diminish chronic co-morbidities over the life course for WLHIV and their children.

Grant Number: 5R01HD104599-05
NIH Institute/Center: NIH

Principal Investigator: ELAINE ABRAMS

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