grant

Identifying inter-kingdom microbial determinants of altered immunity in HIV exposed infants

Organization UNIVERSITY OF CALIFORNIA RIVERSIDELocation RIVERSIDE, UNITED STATESPosted 12 Sept 2024Deadline 31 Jul 2027
NIHUS FederalResearch GrantFY202516S RNA sequencing16S RNAseq16S gene sequencing16S rDNA amplicon sequencing16S rRNA DNA sequencing16S rRNA amplicon sequencing16S rRNA gene amplicon sequencing16S rRNA gene sequencing16S rRNA genomic profiling16S rRNA sequencing16S ribosomal RNA gene sequencing16S ribosomal RNA sequencing16S seq16S sequencing16s rRNA seq21+ years oldAIDS VirusAcquired Immune Deficiency Syndrome VirusAcquired Immunodeficiency Syndrome VirusAdultAdult HumanAnimalsAssayBCG LiveBCG VaccineBCG immunizationBCG vaccinationBCG-vaccinatedBacille Calmette Guerin vaccineBacille Calmette-Guerin vaccinatedBacille Calmette-Guerin vaccinationBacille Calmette-GuérinBacillus Calmette Guerin VaccineBacillus Calmette GuérinBacillus Calmette-Guerin vaccinationBacillus Calmette-Guérin vaccinationBacillus Calmette-Guérin vaccineBacteriaBacterial VaccinesBacterinBacteriophagesBayesian AnalysisBayesian computationBayesian inferenceBayesian network analysisBayesian spatial analysisBayesian statistical analysisBayesian statistical inferenceBayesian statisticsBioassayBiological AssayCausalityCell BodyCellsColonCommunitiesDataData SetDevelopmentDiathesisDiseaseDisease susceptibilityDisorderEnteralEntericEtiologyFecesFunctional MetagenomicsFundingGI microbiomeGI microbiotaGastrointestinal microbiotaGene ExpressionGerm-FreeGnotobioticGnotobioticsHIVHIV InfectionsHTLV-III InfectionsHTLV-III-LAV InfectionsHealthHumanHuman Immunodeficiency VirusesHuman MicrobiomeHuman T-Lymphotropic Virus Type III InfectionsImmuneImmune responseImmunesImmunityImmunizationImmunizeInfantIntestinalIntestinesLAV-HTLV-IIILifeLinear RegressionsLinkLymphadenopathy-Associated VirusMediatingMetagenomicsMicrobeModelingModern ManMorbidityMorbidity - disease rateMothersMucosaMucosal ImmunityMucosal TissueMucous MembraneNeonatalPeripheralPhagesPlayProbioticsResearchRoleShapesShotgunsSpleenSpleen Reticuloendothelial SystemStatistical Data AnalysesStatistical Data AnalysisStatistical Data InterpretationT cell responseT-Cell SubsetsT-CellsT-LymphocyteT-Lymphocyte SubsetsTechniquesTestingTherapeuticVaccinationViralVirionVirusVirus ParticleVirus-HIVWhole BloodWorkadaptive immunityadulthoodantagonismantagonistbacteria in the gutbacterial communitybacterial microbiomebacterial virusbacteriomebowelcausationcohortcytokinedata integrationdevelopmentaldigestive tract microbiomedisease causationenteric microbial communityenteric microbiomeenteric microbiotaexperimentexperimental groupexperimental researchexperimental studyexperimentsgastrointestinal microbial floragastrointestinal microbiomegut bacteriagut communitygut dysbiosisgut floragut microbe communitygut microbial communitygut microbial compositiongut microbial consortiagut microbiomegut microbiotagut microbioticgut microfloragut-associated microbiomehigh riskhost responsehuman-associated microbiomeimmune system responseimmunoresponseinsightintestinal biomeintestinal floraintestinal microbiomeintestinal microbiotaintestinal microfloraintestinal tract microfloraliability to diseasemetagenomemicrobialmicrobial consortiamicrobial floramicrobiomemicrobiotamicrofloramouse modelmultiomicsmultiple omicsmultispecies consortiamurine modelpanomicspupresponsescRNA sequencingscRNA-seqshot gunsingle cell RNA-seqsingle cell RNAseqsingle cell expression profilingsingle cell transcriptomic profilingsingle-cell RNA sequencingsocial rolestatistical analysisstoolthymus derived lymphocytevaccine responsevaccine responsivenessvaccine-induced responseviral microbiomevirome
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Full Description

PROJECT ABSTRACT
Infants born to HIV-infected mothers are at high risk for HIV acquisition. Additionally, HIV-exposed yet
uninfected infants display reduced vaccine responses and increased disease susceptibility compared to
unexposed infants. The development of certain T cell subsets, both in the mucosa and systemically, is
determined by the presence of specific microbes in the gut and may be important in determining adaptive
immunity. However, the gut microbiota of HIV-exposed uninfected (iHEU) infants differs from that of HIV-
unexposed (iHU) infants, since their mothers have altered gut microbiota. The gut virome also plays a central
role in modulating both the bacterial microbiota and immune response of adults, yet the association between
the infant enteric virome and cellular responses to vaccination has not yet been explored. This study proposes
that the enteric virome is one of the factors influencing the morbidity of HIV-exposed infants, either by directly
altering mucosal immunity or by altering the composition of enteric bacterial communities, as a consequence of
bacteriophage or other viral dynamics. This proposal will utilize an already funded, ongoing cohort to
longitudinally identify interactions between viruses, bacterial microbiota, and cellular responses to vaccination
in 40 iHEU and 40 iHU (Aim 1). Viral metagenome data will be integrated with bacterial community datasets
and T cell cytokine responses to BCG vaccination to identify viral and bacterial taxa correlated with BCG
responses. The effect of the expanded virome on bacterial microbiota and responses to BCG vaccination will
then be assessed for causality in gnotobiotic mouse models (Aim 2). The effect of the expanded iHEU viroem
on mucosa and peripheral gene expression will be assayed using single cell RNA sequencing in Aim 3.
Integrative analyses will be used to identify interactions between specific bacterial and viral taxa, as well as
their associated with BCG responses. Together, these Aims will identify mechanisms of gut dysbiosis in iHEU
and reveal potential therapeutics to restore health to this group. Collectively, this proposal will reveal how
maternal HIV infection shapes the enteric microbiome and immunity of associated infants.

Grant Number: 5R00HD106861-04
NIH Institute/Center: NIH
Principal Investigator: Bryan Brown

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