Effects of Targeting Immune Activation and Intestinal Barrier on Comorbidities in People with HIV
Project Number1K24AI177089-01A1
Former Number1K24AI177089-01
Contact PI/Project LeaderLO, JANET
Awardee OrganizationMASSACHUSETTS GENERAL HOSPITAL
Description
Abstract Text
Project Summary/Abstract
People living with HIV infection have increased risk of comorbidities including cardiovascular disease, obesity
and diabetes mellitus, despite effective antiretroviral therapy. Emerging evidence show that residual persistent
immune dysregulation contributes to comorbidities in the HIV population. Cardiovascular disease and
metabolic disorders are important comorbidities affecting people aging with HIV. The NIH K24 Midcareer
Investigator Award in Patient-Oriented Research would provide crucial support to enable advancement of my
patient-oriented research into mechanisms and potential prevention and treatment strategies for
atherosclerosis and metabolic diseases including obesity, abnormal adipose tissue, insulin resistance and
diabetes mellitus in people with HIV. I currently lead multidisciplinary teams and our interdisciplinary studies
with rich collaborations with HIV virologists, immunologists, infectious disease clinical trialists, cardiologists,
gastroenterologists, pathologists, and biostatisticians provide an exciting research platform for mentoring.
Importantly, the support of the K24 Award would allow me to have dedicated and protected time to mentor new
physician scientists in clinical investigation. This award would also allow me to develop my own skills in
mentoring, leadership and research, and to advance scientific research on comorbidities in people with HIV,
especially metabolic and cardiovascular comorbidities related to chronic immune inactivation in people living
with chronic HIV. Mentoring training will be provided utilizing my NIH funded studies to provide trainees with
opportunities to 1) investigate gastrointestinal mucosal barrier in people with HIV and its role in chronic
inflammation, immune activation and cardiovascular disease risk using existing data and intestinal biopsy
samples already collected and 2) to prospectively investigate the effects of CCR2 and CCR5 chemokine
receptor antagonism on immune activation, cardiovascular disease risk and metabolism in a multicenter
placebo-controlled, double-blind, 24-week long, randomized trial of cenicriviroc vs. placebo in adult men and
women living with HIV with suppressed HIV-1 RNA on stable ART who have increased CVD risk. This study
will leverage the clinical trial infrastructure of the ACTG and the extensive scientific expertise of collaborating
investigators and laboratories within the ACTG and provide rich training experiences for my mentees in patient
oriented clinical trial research.
Public Health Relevance Statement
Project Narrative
People living with HIV infection have increased inflammation and risk of cardiovascular disease and
metabolic disease. Abnormalities in the gastrointestinal tract and in the immune system can increase the risk
of cardiovascular and metabolic disease. This proposal would enable the PI to advance research on
metabolic and cardiovascular health in people with HIV and to train future physician scientists.
NIH Spending Category
No NIH Spending Category available.
Project Terms
AIDS clinical trial groupAdipose tissueAdultAffectAgingAgonistAtherosclerosisAwardBiologicalBiopsy SpecimenCCR5 geneCardiologyCardiovascular DiseasesCardiovascular systemChronicClinicalClinical InvestigatorClinical ResearchClinical TrialsCollaborationsCommunicable DiseasesConduct Clinical TrialsDataData SetDedicationsDiabetes MellitusDouble-Blind MethodDyslipidemiasEducationEpitheliumFunctional disorderFundingFutureFuture GenerationsGLP-2GastroenterologistGastrointestinal tract structureGoalsHIVHIV InfectionsHIV-1ImmuneImmune TargetingImmune systemImmunologistImmunologyInflammationInfrastructureInsulin ResistanceInterdisciplinary StudyInterventionIntestinesInvestigationLaboratoriesLeadLeadershipMedicineMentorsMetabolicMetabolic DiseasesMetabolismMid-Career Clinical Scientist Award (K24)Midcareer Investigator Award in Patient-Oriented ResearchMucous MembraneMulti-Institutional Clinical TrialObesityPathologistPathologyPersonsPhysiciansPhysiologicalPlacebo ControlPlacebosPopulationPrevention strategyRNARadiology SpecialtyRandomizedResearchResearch PersonnelResidual stateRiskRoleScientific Advances and AccomplishmentsScientistTimeTissue SampleTrainingUnited States National Institutes of HealthWomanantagonistantiretroviral therapycardiovascular disorder riskcardiovascular healthchemokine receptorclinical investigationcomorbidityeffective interventionexperiencegastrointestinalimmune activationimprovedinsightintestinal barriermenmid-career facultymultidisciplinarynovelpatient orientedpatient oriented researchprimary endpointprospectiverandomized placebo controlled trialrandomized trialresearch studyskillsteduglutidetreatment strategy
National Institute of Allergy and Infectious Diseases
CFDA Code
855
DUNS Number
073130411
UEI
FLJ7DQKLL226
Project Start Date
16-August-2024
Project End Date
31-July-2029
Budget Start Date
16-August-2024
Budget End Date
31-July-2025
Project Funding Information for 2024
Total Funding
$206,283
Direct Costs
$191,003
Indirect Costs
$15,280
Year
Funding IC
FY Total Cost by IC
2024
National Institute of Allergy and Infectious Diseases
$206,283
Year
Funding IC
FY Total Cost by IC
Sub Projects
No Sub Projects information available for 1K24AI177089-01A1
Publications
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Outcomes
The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.
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Clinical Studies
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