grant

Development of resident memory T cells in the synovium

Organization BOSTON CHILDREN'S HOSPITALLocation BOSTON, UNITED STATESPosted 4 Apr 2022Deadline 31 Mar 2027
NIHUS FederalResearch GrantFY20263-D3-D modeling3-Dimensional3D3D modelingAML2Adoptive TransferAdvisory CommitteesAffectAntibodiesAntigensAreaArthralgiaArthritisAtrophic ArthritisAttenuatedAutoimmune DiseasesBioinformaticsBiologyBody TissuesBostonCD8CD8 CellCD8 T cellsCD8 lymphocyteCD8+ T cellCD8+ T-LymphocyteCD8-Positive LymphocytesCD8-Positive T-LymphocytesCD8BCD8B1CD8B1 geneCITE sequencingCITE-seqCITEseqCRISPRCRISPR approachCRISPR based approachCRISPR methodCRISPR methodologyCRISPR techniqueCRISPR technologyCRISPR toolsCRISPR-CAS-9CRISPR-based methodCRISPR-based techniqueCRISPR-based technologyCRISPR-based toolCRISPR/CAS approachCRISPR/Cas methodCRISPR/Cas systemCRISPR/Cas technologyCRISPR/Cas9CRISPR/Cas9 technologyCas nuclease technologyCell BodyCell Communication and SignalingCell LineageCell SignalingCellsCellular Indexing of Transcriptomes and Epitopes by SequencingCellular biologyChemotactic CytokinesChildhoodChildren's HospitalChronicChronic Childhood ArthritisClustered Regularly Interspaced Short Palindromic RepeatsClustered Regularly Interspaced Short Palindromic Repeats approachClustered Regularly Interspaced Short Palindromic Repeats methodClustered Regularly Interspaced Short Palindromic Repeats methodologyClustered Regularly Interspaced Short Palindromic Repeats techniqueClustered Regularly Interspaced Short Palindromic Repeats technologyCo-cultureCocultivationCocultureCoculture TechniquesCoupledDataDevelopmentDifferential Gene ExpressionDiseaseDisease remissionDisorderDoctor of MedicineDoctor of PhilosophyDrugsDysfunctionEffector CellEndothelial CellsEnvironmentEventExhibitsFatty AcidsFibroblastsFlareFoundationsFunctional disorderFundingFutureGene ExpressionGene Expression MonitoringGene Expression Pattern AnalysisGene Expression ProfilingGene TargetingGene TranscriptionGenesGenetic TranscriptionGoalsHeadHomingHomologous Chemotactic CytokinesHospitalsHumanImmuneImmune Cell ActivationImmunesImmunologyIndividualInflammationInflammatoryInflammatory ArthritisInstitutionIntercrinesInterruptionIntracellular Communication and SignalingInvestigatorsJoint DiseasesJoint PainJointsJuvenile Chronic ArthritisJuvenile Chronic PolyarthritisJuvenile Rheumatoid ArthritisKnowledgeLYT3LaboratoriesLearningLigandsLymph Node Reticuloendothelial SystemLymph node properLymphatic nodesM.D.MHC ReceptorMaintenanceMajor Histocompatibility Complex ReceptorMediatingMediatorMedicationMembrana Synovialis Capsulae ArticularisMembrane Protein GeneMembrane ProteinsMembrane-Associated ProteinsMemoryMentorsMentorshipMethodsMiceMice MammalsModelingModern ManMurineMusNIAMSNational Institute of Arthritis, and Musculoskeletal, and Skin DiseasesOrganoidsPathway interactionsPatientsPatternPediatric HospitalsPeriodicalsPeripheralPersonsPh.D.PhDPharmaceutical PreparationsPhenotypePhysiciansPhysiopathologyPopulationProcessRNA ExpressionRUNX3RUNX3 geneReceptor ProteinRecurrenceRecurrentRecurrent diseaseRelapsed DiseaseRemissionResearch PersonnelResearch ResourcesResearchersResistanceResourcesRheumatoid ArthritisRoleRunt-Related Transcription Factor 3SIS cytokinesScientistSeriesSignal TransductionSignal Transduction SystemsSignalingSingle cell seqSiteSterilityStromal CellsSurfaceSurface ProteinsSynovial MembraneSynoviumSystemT memory cellT-Cell ActivationT-Cell Antigen ReceptorsT-Cell DevelopmentT-Cell OntogenyT-Cell ReceptorT-CellsT-LymphocyteT-Lymphocyte DevelopmentT8 CellsT8 LymphocytesTGF-Beta Type II ReceptorTGFBR2TGFBR2 geneTask ForcesTestingTherapeuticTimeTissue DifferentiationTissue ModelTissue-Specific Differential Gene ExpressionTissue-Specific Gene ExpressionTissuesTrainingTranscript Expression AnalysesTranscript Expression AnalysisTranscriptionTranslational ResearchTranslational ScienceWomanWorkactivate T cellsadvisory teamanalyze gene expressionarthriticarthritis therapyarthropathicarthropathiesarthropathyattenuateattenuatesautoimmune conditionautoimmune disorderautoimmunity diseasebiological signal transductioncareercell biologycellular indexing of transcriptomes and epitopes by single cell sequencingchemoattractant cytokinechemokinechronic autoimmune diseaseconfocal imagingdesigndesigningdevelopmentaldisease controldisorder controldrug/agentexperiencegene expression analysisgene expression assayhuman diseasehuman modelimmune activationimmunogeninflamed jointinsightjoint disorderjoint inflammationjoint swellingjuvenile arthritisjuvenile idiopathic arthritislymph glandlymph nodeslymphnodesmRNA Expressionmedical collegemedical schoolsmemory T lymphocytemigrationmodel of humanmouse modelmurine modelnew approachesnew drug targetnew drug treatmentsnew druggable targetnew drugsnew pharmacological therapeuticnew pharmacotherapy targetnew therapeutic targetnew therapeuticsnew therapynew therapy targetnext generation therapeuticsnovel approachesnovel drug targetnovel drug treatmentsnovel druggable targetnovel drugsnovel pharmaco-therapeuticnovel pharmacological therapeuticnovel pharmacotherapy targetnovel strategiesnovel strategynovel therapeutic targetnovel therapeuticsnovel therapynovel therapy targetpathophysiologypathwaypediatricperiodicperiodicalpreventpreventingprotein expressionreceptorrecruitresidenceresident memory T cellresidential buildingresidential siteresistantrheumatic arthritisrheumatologistscRNA sequencingscRNA-seqschool of medicinesingle cell RNA-seqsingle cell RNAseqsingle cell analysissingle cell expression profilingsingle cell next generation sequencingsingle cell sequencingsingle cell transcriptomic profilingsingle-cell RNA sequencingskillssocial rolesteriletherapeutic targetthree dimensionalthree-dimensional modelingthymus derived lymphocytetissue resident memory T celltranscriptional profilingtranscriptomicstransforming growth factor-beta type II receptortransforming growth factor-β type II receptortranslation researchtranslational investigationuptake
Sign up free to applyApply link · pipeline · email alerts
— or —

Get email alerts for similar roles

Weekly digest · no password needed · unsubscribe any time

Full Description

Project Summary/Abstract
Rheumatoid arthritis (RA) and juvenile idiopathic arthritis (JIA) are chronic autoimmune diseases of the joint
punctuated by periodic arthritis flares. Clinicians have long recognized that each affected person develops an
individual pattern of affected joints, and that this pattern remains stable over time through disease remission and
flares. We recently identified the presence of synovial resident memory T cells (TRM) in arthritic joints and showed
that they mediate arthritis flares. Correspondingly, depleting these cells ameliorates disease recurrence,
indicating that TRM can be targeted as a novel approach in arthritis therapy. The long-term objective of the
proposal is to define the mediators of TRM development and maintenance in the synovium and determine if these
pathways can be therapeutically targeted to treat arthritis.
The specific aims of this proposal utilize 2 complementary approaches in mice and human studies to identify the
mediators of synovial TRM development. Aim 1 utilizes a mouse model of inflammatory arthritis developed by the
PI to define the lineage and differentiation process of synovial TRM. Aim 2 utilizes a human synovial organoid
system to interrogate the impact of the synovial microenvironment, namely synovial stromal cells, on TRM
formation and survival. We expect that these studies will identify critical mediators of TRM development, which
may represent novel therapeutic targets for inflammatory arthritis.
The candidate is an M.D./Ph.D. pediatric rheumatologist at Boston Children’s Hospital. This proposal builds upon
her foundational knowledge of immunology to extend her skillset into antibody-coupled single cell sequencing,
bioinformatics, organoid models of human synovium, and CRISPR gene targeting. The proposal includes a
comprehensive mentoring and didactic plan that will allow her to successfully learn new skills and gain expertise
in each of these important areas. The primary mentor, Dr. Peter Nigrovic, is a rheumatologist and expert in the
pathophysiology of inflammatory arthritis. The candidate has assembled a K08 advisory committee consisting of
Dr. Michael Brenner, Dr. Rachael Clark, and Dr. Soumya Raychaudhuri, who each have specific expertise in
various aspects of this proposal such as analysis of single-cell sequencing data, 3D models of human synovium,
and expertise in TRM biology in human disease. The candidate is committed to a career in translational research
with the goal of becoming an independent lab-based investigator focusing on local mechanisms to autoimmune
disorders. The proposed studies, training plan, and exceptional environment at Boston Children’s Hospital,
Brigham and Women’s Hospital and Harvard Medical School will enable her to successfully transition to an
independent PI and leader in this field.

Grant Number: 5K08AR080992-05
NIH Institute/Center: NIH
Principal Investigator: Margaret Chang

Sign up free to get the apply link, save to pipeline, and set email alerts.

Sign up free →

Agency Plan

7-day free trial

Unlock procurement & grants

Upgrade to access active tenders from World Bank, UNDP, ADB and more — with email alerts and pipeline tracking.

$29.99 / month

  • 🔔Email alerts for new matching tenders
  • 🗂️Track tenders in your pipeline
  • 💰Filter by contract value
  • 📥Export results to CSV
  • 📌Save searches with one click
Start 7-day free trial →

Explore more

📍 More grants in UNITED STATES🏷 More NIH opportunities🏷 More US Federal opportunities🏷 More Research Grant opportunities🏢 All nih_reporter opportunities