grant

Sex Differences in Gut Metabolite-Immune Interplay in Hypertension and Renal End-Organ Damage

Organization AUGUSTA UNIVERSITYLocation AUGUSTA, UNITED STATESPosted 24 Sept 2024Deadline 31 Aug 2026
NIHUS FederalResearch GrantFY2024AblationAddressAmericanAminesAntibiotic AgentsAntibiotic DrugsAntibioticsBP controlBP homeostasisBP managementBP regulationBioenergeticsBiologicalBlood PressureBlood SerumCardiovascularCardiovascular Body SystemCardiovascular DiseasesCardiovascular Organ SystemCardiovascular systemCarnitineCause of DeathCell FunctionCell PhysiologyCell ProcessCellular FunctionCellular PhysiologyCellular ProcessCholineColonCommon Rat StrainsCorrelative StudyDahl Hypertensive RatsDahl Salt-Sensitive RatsDataDevelopmentDifferences between sexesDiffers between sexesDiseaseDisease ProgressionDisorderEndocrine Gland SecretionExhibitsExperimental ModelsFecesFemaleFermentationFiberGI microbiotaGastrointestinal microbiotaGeneticGrantHeart VascularHormonesHumanHypertensionImmuneImmune systemImmunesImmunityImmunomodulationInjury to KidneyInterventionIntervention StrategiesKidneyKidney DiseasesKidney Urinary SystemKnowledgeLinkMediatingMediatorMiscellaneous AntibioticModelingModern ManNephropathyOrganOxidesPBMCPathologicPatientsPeripheral Blood Mononuclear CellPhysiologicPhysiologicalPlayPopulationPre-Clinical ModelPre-MenopausePre-menopausal PeriodPreclinical ModelsPremenopausalPremenopausal PeriodPremenopauseProductionPropionatesRatRats MammalsRattusRenal DiseaseResearch DesignRoleSamplingSerumSeveritiesSeverity of illnessSex DifferencesSexual differencesShort-Chain Fatty AcidsSodium ChlorideStudy TypeSubcellular ProcessT cell based therapeuticsT cell based therapyT cell directed therapiesT cell infiltrationT cell targeted therapeuticsT cell therapyT-Cell ActivationT-CellsT-LymphocyteT-cell therapeuticsT-cell transfer therapyTestingTherapeuticTherapeutic HormoneTranslatingTwin Multiple BirthTwin StudiesTwinsUrineVascular Hypertensive DiseaseVascular Hypertensive DisorderVolatile Fatty AcidsWomanWomen's studyWorkactivate T cellsadoptive T cell transferadoptive T-cell therapyaminebiologicblood pressure controlblood pressure homeostasisblood pressure managementblood pressure regulationcardiovascular disease riskcardiovascular disordercardiovascular disorder riskcardiovascular riskcardiovascular risk factorcirculatory systemcohortcomparing females and malescomparing women and mencytokinedamage to kidneydevelopmentaldisease severityenteric microbial communityenteric microbiotaexperimentexperimental researchexperimental studyexperimentsfecal microbial communityfecal microbiotafemale studyfemales compared to malesfemales compared with malesfemales versus malesfemales vs malesgastrointestinal microbial floragut commensalgut communitygut floragut microbe communitygut microbial communitygut microbial compositiongut microbial consortiagut microbiotagut microbioticgut microflorahigh blood pressurehigh riskhyperpiesiahyperpiesishypertensivehypertensive diseasehypertensive disorderimmune modulationimmune regulationimmunologic reactivity controlimmunomodulatoryimmunoregulationimmunoregulatoryimprovedinterventional strategyintestinal floraintestinal microbiotaintestinal microfloraintestinal tract microflorakidney damagekidney disorderkidney injurymalemenmicrobialmicrobial consortiamicrobial floramicrobiotamicrobiota compositionmicrobiota derived metabolitesmicrobiota metabolitesmicrofloramultispecies consortianew drug treatmentsnew drugsnew pharmacological therapeuticnew therapeuticsnew therapynext generation therapeuticsnovelnovel drug treatmentsnovel drugsnovel pharmaco-therapeuticnovel pharmacological therapeuticnovel therapeuticsnovel therapypre-clinicalpre-menopausalpreclinicalpremenopausal statusregulate BPregulate blood pressurerenalrenal damagerenal disorderrenal injurysaltsalt hypertensionsalt induced hypertensionsalt sensitivesalt sensitive hypertensionsexsex based differencessex dimorphismsex-dependent differencessex-related differencessex-specific differencessexual dimorphismsexually dimorphicsocial rolestoolstudy among femalesstudy among womenstudy designstudy in femalesstudy in womenstudy on femalesstudy on womenstudy within womentherapeutic T-cell platformthymus derived lymphocytetranslational studywomen compared to menwomen compared with menwomen versus menwomen vs men
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Full Description

PROJECT SUMMARY/ABSTRACT
Nearly half of the ~116 million Americans with hypertension are salt-sensitive and confer a 3-fold higher risk of

developing cardiovascular disease. Only 26% of hypertensive patients reach blood pressure (BP) control, which

may be due to lack of studies in females despite the growing evidence for sex differences in hypertensive

mechanisms. It is known that the gut microbiota and immune system are critical in hypertension in males; this is

largely unknown in females. The objective of this grant is to address this knowledge gap regarding the role of

the gut microbiota and immune system to mediate sex differences in salt-sensitive hypertension. Mechanistic

studies will be performed in male and female Dahl Salt-Sensitive (SS) rats, with translational studies performed

in samples from opposite-sex twin pairs where the males have hypertension compared to females.

Dahl SS rats, a model consistent with human salt-sensitive hypertension, exhibit a greater degree of salt-

sensitivity and associated end-organ damage in males compared to females. We have observed stark sex

differences in gut microbiota composition and gut-derived metabolites. Through microbiota transfer studies, we

know the gut microbiota plays a causal role in the regulation of BP and renal damage. Linking the microbiota to

immunity, microbiota transfer also influences renal T cell infiltration. Genetic deletion of T cells (SSCD247–/–)

eliminates sex differences in salt-sensitive hypertension, highlighting the role of T cells to mediate BP sex

differences. Since the gut microbiota influences renal T cell infiltration, and T cells amplify salt-sensitive

hypertension, we have strong rationale for studying how sex-specific microbiota impact T cell function and salt-

sensitivity. We will test the central hypothesis that gut microbiota-dependent T cell activation determines

the extent of salt-sensitive hypertension and mediates the sex differences in disease severity.

Our hypothesis will be rigorously tested with three aims: Aim 1 will test the hypothesis that the gut microbiota

drives sex differences in salt-sensitive hypertension. Sex-specific microbiota transfer and gonadectomy studies

will reveal whether the gut microbiota sex- and hormone-dependently contributes to salt-sensitive hypertension

in SS rats. Aim 2 will test the hypothesis that the male versus female gut microbiota influences sex differences

in T cell function and activation. Microbiota transfer in SSCD247–/– rats lacking T cells will assess the impact of sex

and gut microbiota on T cell bioenergetics and cytokine production, and will address whether T cells are required

for gut microbiota-dependent salt-sensitive hypertension. Aim 3 will determine whether the sex-specific

observations in gut microbiota, gut metabolites, and T cell function in the SS rat similarly parallel humans from

a longitudinal opposite-sex twin cohort, where the males exhibit hypertension compared to their female twin pair.

These studies will reveal key mechanisms related to gut microbiota-immune-kidney crosstalk and provide the

preclinical and human basis for developing novel, sex-specific targets to improve BP control and kidney disease.

Grant Number: 1R56HL169434-01A1
NIH Institute/Center: NIH

Principal Investigator: Justine Abais-Battad

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