grant

Bone marrow niche regulation of disseminated tumor cell dormancy, reactivation, and metastasis.

Organization UNIVERSITY OF MINNESOTALocation MINNEAPOLIS, UNITED STATESPosted 10 Feb 2022Deadline 31 Aug 2027
NIHUS FederalResearch GrantFY20253-D Imaging3D imagingAntibodiesAssayAwardBM Stem CellBM derived progenitorBM progenitorBM- derived Stem CellsBioassayBiocompatible MaterialsBioinformaticsBiological AssayBiomaterialsBiopsyBiopsy SampleBiopsy SpecimenBlood VesselsBody TissuesBone MarrowBone Marrow Blood-Deriving CellBone Marrow Blood-Forming CellBone Marrow CellsBone Marrow Reticuloendothelial SystemBone Marrow Stem CellBone Marrow progenitorBone marrow biopsyBreast CancerBreast Cancer CellBreast Cancer ModelBreast Cancer PatientBreast Tumor PatientBreast tumor modelCancer BiologyCause of DeathCell BodyCell CommunicationCell InteractionCell LineCell-to-Cell InteractionCellLineCellsCellular MechanotransductionClassificationClinicalClinical OncologyCo-cultureCocultivationCocultureCoculture TechniquesConsultCuesCytometryDNA Molecular BiologyDataDevelopmentDiagnosisER PositiveER+ElementsEndocrine Gland SecretionEstrogen receptor positiveEvaluationExhibitsGelGeneral Prognostic FactorHematopoieticHormone ResponsiveHormonesHydrogelsImageImmuneImmunesImmunocompetentIn VitroInflammationLearningLifeMaintenanceMalignant Breast NeoplasmMalignant CellMechanical Signal TransductionMechanicsMechanosensory TransductionMentorsMetastasisMetastasizeMetastatic LesionMetastatic MassMetastatic NeoplasmMetastatic TumorMiceMice MammalsMicroscopyModelingMolecular BiologyMurineMusNatureNeoplasm MetastasisNormal TissueNormal tissue morphologyOpticsParacrine CommunicationParacrine SignalingPathologyPatientsPhasePhenotypePlayPopulationPreventionPrognostic FactorPrognostic/Survival FactorProliferatingRecurrenceRecurrentRecurrent diseaseRegulationRegulatory PathwayRelapseRelapsed DiseaseResearchRiskRoleSamplingSecondary NeoplasmSecondary TumorSeriesSourceStem Cell likeStrains Cell LinesStressful EventSystematicsTestingTherapeutic HormoneThree-Dimensional ImagingTissuesTrainingTumor CellWorkbiological materialbiomarker identificationbonebone marrow derived progenitorbone marrow derived stem cellsbone marrow stromal cellbone marrow stromal stem cellbreast tumor cellcancer cellcancer metastasiscancer progenitorcancer progenitor cellscancer stem cellcancer stem like cellcomputer based predictionconsultscultured cell linedevelop therapydevelopmentalexperiencehemopoietichigh dimensionalityhigh riskhuman diseaseidentification of biomarkersidentification of new biomarkersimagingimmune competentin vivoindividuals with breast cancerintervention developmentmalignant breast tumormalignant progenitormalignant stem cellmammary cancer modelmammary tumor modelmarker identificationmechanicmechanicalmechanosensingmechanotransductionmouse modelmurine modelneoplastic cellnoveloncogenic progenitoroncogenic stem cellsopticalpatients with breast cancerperson with breast cancerpredictive modelingpreventpreventingprogenitor capacityprogenitor cell likeprogenitor cell nicheprogenitor like cancer cellprogenitor nicheprogenitor-likeprogramsprotein biomarkersprotein markersrecruitscRNA sequencingscRNA-seqsingle cell RNA-seqsingle cell RNAseqsingle cell expression profilingsingle cell transcriptomic profilingsingle-cell RNA sequencingsocial rolestem and progenitor cell nichestem cell characteristicsstem cell nichestem like cancer cellstem-likestemnessstressful experiencestressful life eventstressful life experiencetherapeutic agent developmenttherapeutic developmenttherapeutic targettherapy developmenttissue progenitortissue specific progenitor cellstissue specific stem cellstissue stem cellstreatment developmenttumortumor cell metastasisvascular
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Full Description

PROJECT SUMMARY / ABSTRACT
Metastatic relapse may occur in patients with ER+ breast cancer decades after original diagnosis. Most breast

cancer related deaths are caused by metastasis and thus identifying at-risk patients and developing therapies to

prevent reactivation are a crucial challenge. These efforts have been impeded by a lack of understanding of

cancer cell dormancy in the bone marrow, believed to be the cellular source of metastatic relapse. It is not well

understood how tumor cells interact with the bone marrow microenvironment and how these interactions regulate

tumor cell dormancy and escape. My proposed research seeks to develop a mouse model of dormancy and

investigate the spatial organization of the bone marrow niche in patient samples in the mentored K99 phase and

develop a biomaterial model of dormancy in the independent R00 phase. I hypothesize (i) cancer stem cells are

a subset of disseminated tumor cells responsible for metastatic relapse and (ii) the bone marrow niche, including

the healthy stem cell niche, facilitates dormancy and reactivation of these cells. In Aim 1, I will develop a novel

mouse model of hormone responsive breast cancer dormancy in bone marrow and evaluate the presence,

phenotype, and microenvironmental regulation of disseminated tumor cells using optical tissue clearing/3D

imaging of whole bone. In Aim 2, I will investigate the hypothesis that tumor cell interactions with the bone marrow

niche control tumor cell phenotype via high dimensional spatial analysis of bone marrow biopsies from patients

with breast cancer including imaging mass cytometry (IMC) and spatial single cell RNA sequencing (scRNAseq).

In Aim 3, I will develop a biomaterial model of the dormant bone marrow niche via creating mechanical mimics

of the three distinct compartments of bone marrow and evaluate the role of mechanosensing in induction and

maintenance of dormancy. In the K99 phase of the award, Prof Max Wicha will serve as my main mentor. Dr.

Wicha is a pioneer in the cancer stem cell field and is an expert in breast cancer biology and metastasis. I will

work with and consult my collaborators and mentoring team, including Prof Fei Wen (imaging mass cytometry),

Evan Keller (single cell spatial analysis program), Dr. Dafydd Thomas (pathology core), Prof Gary Luker

(microscopy), Prof Monika Burness (breast cancer clinical oncology) and Prof Sofia Merjaver (breast cancer

molecular biology). My K99 training will consist of developing a novel mouse model of bone marrow dormancy

and learning bioinformatics approaches to analyze spatial contributions to cellular phenotype in IMC and

scRNAseq data to propel me toward developing a synthetic dormant bone marrow niche mimic using

biomaterials during the independent R00 phase. In sum, the proposed research will address an urgent, unmet

need to identify the role of the bone marrow niche in breast cancer dormancy and reactivation, which may provide

a path forward for identifying patients at higher risk of metastasis and developing therapies against reactivation.

Grant Number: 5R00CA267261-04
NIH Institute/Center: NIH

Principal Investigator: Grace Bushnell

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