grant

Role of FSH in postmenopausal obesity and breast cancer

Organization UNIVERSITY OF ARIZONALocation TUCSON, UNITED STATESPosted 1 Mar 2022Deadline 28 Feb 2027
NIHUS FederalResearch GrantFY2025AccountingActive Follow-upAdipose tissueAgeAncillary StudyAquadiolAttentionAutomobile DrivingBMIBMI percentileBMI z-scoreBilateral oophorectomyBilaterial OvariectomyBindingBiological MarkersBlood SerumBody CompositionBody WeightBody fatBody mass indexBreastBreast CancerBreast Cancer PreventionBreast Cancer Risk FactorBreast NeoplasmsBreast TumorsCancer Prevention InterventionCancersCase-Base StudiesCase-Comparison StudiesCase-Compeer StudiesCase-Referent StudiesCase-Referrent StudiesCase/Control StudiesClinicalClinical EvaluationClinical TestingClinical TrialsComputer softwareConjugated Equine EstrogensDEXADXADataDepo-Medroxyprogesterone AcetateDevelopmentDimenformonDiogynDiogynetsDrugsDual-Energy X-Ray AbsorptiometryDual-Energy Xray AbsorptiometryER PositiveER+Endocrine Gland SecretionEndocrine TherapyEndocrinologyEpidemiologic ResearchEpidemiologic StudiesEpidemiological StudiesEpidemiology ResearchEstraceEstradiolEstradiol-17 betaEstradiol-17betaEstraldineEstrogen receptor positiveEstrogensEthnic OriginEthnicityFSH ReceptorsFatty TissueFeedbackFemale CastrationFemale HealthFollicle Stimulating HormoneFollicle Stimulating Hormone ReceptorFollitropinFutureGnRH antagonistGoalsGonadotropin Releasing Hormone InhibitorGonadrotropin Releasing Hormone AntagonistsGoserelinGrowth AgentsGrowth FactorGrowth SubstancesHormonalHormonal TherapyHormonesHumanHysterectomyImageIncidenceInflammatoryInvestigationJointsLeptinMalignant Breast NeoplasmMalignant NeoplasmsMalignant TumorMalignant neoplasm of prostateMalignant prostatic tumorMammary CancerMammary NeoplasmsMarketingMeasuresMediatingMediatorMedicationMedroxyprogesterone 17-AcetateMedroxyprogesterone AcetateMedroxyprogesteroni AcetasMenopauseMetabolism and EndocrinologyMethylacetoxyprogesteroneMetipregnoneModelingModern ManMolecular InteractionOb Gene ProductOb ProteinObese Gene ProductObese ProteinObesityObservation researchObservation studyObservational StudyObservational researchOsteoporosisOvarianOvocyclinOvocylinParticipantPharmaceutical PreparationsPilot ProjectsPost-MenopausePost-menopausal PeriodPostmenopausal PeriodPostmenopausePre-Clinical ModelPre-MenopausePre-menopausal PeriodPreclinical ModelsPreclinical dataPremenopausalPremenopausal PeriodPremenopausePreventative therapyPreventionPreventive therapyProcessProductionProgynonProstate CAProstate CancerProstate malignancyProteins Growth FactorsQuetelet indexRaceRacesRandomizedReceptor ProteinReportingResearch ResourcesResourcesRisk FactorsRoleSafetySamplingScanningSerumSoftwareSourceTestingTherapeuticTherapeutic EstradiolTherapeutic EstrogenTherapeutic HormoneTherapy trialTimeTranslationsVisceralWomanWomen's Healthactive followupadiposeadiposityadjudicationadjudicative process and procedureafter menopauseagesarmbio-markersbiologic markerbiomarkerbonebreast cancer diagnosisbreast cancer riskbreast tumorigenesiscancer sub-typescancer subtypescase controlcase-controlledcase-controlled studiesclinical testcohortcorpulencedesigndesigningdevelopmentaldrivingdrug/agentdruggable targetepidemiologic investigationepidemiology studyexperiencefollow upfollow-upfollowed upfollowing menopausefollowuphormone therapyimagingimprovedinnovateinnovationinnovativeinsightinterestlarge data setslarge datasetsmalignancymalignant breast tumormammary cancer preventionmammary tumormammary tumor preventionneoplasm/cancernovelobesity developmentpast menopausephase 3 evaluationphase 3 testingphase III evaluationphase III testingpilot studypost-menopausalpostmenopausalpostmenopausal statuspre-clinicalpre-menopausalpreclinicalpreclinical findingspreclinical informationpremenopausal statusprevent breast cancerracialracial backgroundracial originrandomisationrandomizationrandomly assignedreceptorresearch clinical testingsocial rolesubcutaneoussubdermaltranslationwaist circumferencewhite adipose tissueyellow adipose tissue
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Full Description

ABSTRACT
There is strong and consistent evidence for an association between obesity and post-menopausal breast
cancer; however, the exact mechanisms are not clear. Follicle stimulating hormone (FSH) increases with
menopause, concomitant with increased adiposity, particularly visceral adipose tissue (VAT). Recent
preclinical data suggests that FSH may drive the deleterious shift in adiposity, independent of estrogen (E2).
Further, FSH receptors are now known to be expressed in breast tumors. To date, there have been no large-
scale human investigations of these FSH-adiposity-breast cancer associations. Using the Women's Health
Initiative (WHI), a long-term national epidemiologic study of postmenopausal women, we will test the
hypothesis that FSH drives adiposity postmenopausally, both cross-sectionally and longitudinally. Large
subsets of WHI participants completed repeat dual energy x-ray absorptiometry (DXA) scans, and therefore
have available robust measures of adiposity (including a novel measure of VAT) and banked serum from the
randomized hormone therapy trials (N=1400) and the observational study (OS; N=1499). Second, using a
case-control design, we will test the hypothesis that higher baseline FSH levels associate with increased risk of
breast cancer using adjudicated cancer incidence data spanning >25 years follow-up (N=785 cases; N=2510
non-cases). Further, we will determine whether adiposity mediates the FSH-breast cancer risk associations.
For all analyses, we will account for exogenous HT use (conjugated equine estrogen ± medroxyprogesterone
acetate or reported HT use in the OS), endogenous estrogen (E2), and adipose-derived hormones that directly
or indirectly regulate FSH (e.g. leptin). Our study is the first comprehensive epidemiologic investigation of FSH
and obesity to measure and study FSH levels in the years prior to breast cancer diagnosis to assess the
potential role of FSH in breast cancer. This study, which includes rich hormone and body composition data will
enable immediate translation to more precise breast cancer prevention interventions aligned with new
medications in the pipeline or currently in use for other cancers and osteoporosis, such as FSH and FSH
receptor modulators, upstream GnRH antagonists (e.g. goserelin), and estetrol (E4).

Grant Number: 5R01CA258436-04
NIH Institute/Center: NIH
Principal Investigator: Jennifer Bea

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