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Development of PU.1 Inhibitory Modulators as Novel Therapeutics for Alzheimer's Disease

Project Number5U01AG066757-05

Contact PI/Project LeaderTSAI, LI-HUEI
Other PIs

Awardee OrganizationMASSACHUSETTS INSTITUTE OF TECHNOLOGY

Description

Abstract Text

Project Summary/Abstract Alzheimer's disease (AD) is a fatal neurodegenerative disease with a global prevalence close to 50 million people, which is expected to double by 2040. Finding an effective treatment for AD has proven difficult, as evidenced by numerous high profile Phase 3 clinical trial failures, most of which directly target the reduction of ß-amyloid. Thus, it is becoming increasingly urgent to develop new pharmacological strategies to combat AD. Drugs are twice as likely to successfully negotiate the drug development pipeline and obtain FDA approval when their targets are supported from human genetic studies of disease. Human genetic studies have revealed a critical role for microglia involvement in Alzheimer’s disease progression, and it has recently been discovered that the transcription factor PU.1 is a driver of the pro-neurodegenerative phenotype adopted by microglia during aging and disease. This proposal therefore aims to develop novel, newly-discovered PU.1 Inhibitory Modulators (PIMs) for preclinical development, with the long term goal of clinically testing the hypothesis that reducing PU.1 activity in microglia will safely delay the age of AD onset (AAO) in at-risk populations. The studies in this proposal leverage the interdisciplinary structure of the Neurodegeneration Consortium, a unique collaboration between basic science researchers and industry drug development veterans operating under a collaborative agreement to push forward novel therapeutics aimed at treating Alzheimer’s diseaes and other neurodegenerative diseases. Under Specific Aim 1, the in vivo safety and efficacy of PIMs will be determined in mouse models of AD. Under Specific Aim 2, parallel target engagement studies will be performed to identify the target of PIMs, and the identified targets will be used to develop assays to determine the efficacy of PIMs in AD and in ex vivo models. Under Specific Aim 3, selected PIMs will be optimized using PK/PD and ADMET screening to develop lead tool compounds into candidate compounds suitable for future Phase I studies. The combined biology, chemistry, and pharmacology expertise in the Neurodegeneration Consortium, spanning The University of Texas MD Anderson Cancer Center, the Massachussets Institute of Technology, and the Mt. Sinai School of Medicine, make this group of researchers ideally suited to execute the proposed aims.

Public Health Relevance Statement

Project Narrative Alzheimer’s disease is a devastating neurodegenerative disease of aging which poses a massive burden on the health care system but for which there is currently no effective therapy or cure. Accumulating evidence suggests that targeting microglia could be beneficial in slowing disease progression, and our labs have discovered a novel microglial drug target called PU.1, that, when reduced in humans, significantly delays the age of onset of the disease. Therefore, we propose development of a drug discovery program aimed at safely reducing PU.1 activity, restoring beneficial microglial function and ultimately slowing the progression of Alzheimer’s disease.

NIH Spending Category

No NIH Spending Category available.

Project Terms

AdoptedAffectAgeAge of OnsetAgingAgreementAlzheimer's DiseaseAlzheimer's disease modelAlzheimer's disease therapeuticAmyloid beta-ProteinAnimalsBasic ScienceBinding ProteinsBiological AssayBiological MarkersBiologyBrainCanis familiarisCell LineCell PhysiologyCellsChIP-seqChemistryClinicalCollaborationsDataDevelopmentDiseaseDisease ProgressionDisease susceptibilityDrug IndustryDrug TargetingFailureFutureGene ExpressionGenesGeneticGenetic TranscriptionGenetic studyGoalsHaplotypesHealthcare SystemsHumanHuman GeneticsImmuneImmunoprecipitationInnate Immune SystemLeadMacrophageMass Spectrum AnalysisMeasurementMediationMicrogliaMicrosomesModelingModificationMolecular TargetMolecular and Cellular BiologyMusMyeloid CellsNerve DegenerationNeurodegenerative DisordersNo-Observed-Adverse-Effect LevelOnset of illnessPeripheralPeripheral Blood Mononuclear CellPermeabilityPersonsPharmaceutical ChemistryPharmaceutical PreparationsPharmacologyPhase III Clinical TrialsPlasmaPopulations at RiskPost-Translational Protein ProcessingPrevalencePrimatesRattusResearch PersonnelRisk ReductionRoleRouteSPI1 geneSafetySentinelSeriesStructureTechnologyTestingTissuesToxicologyUniversity of Texas M D Anderson Cancer CenterValidationVeteransWild Type Mousebiomarker developmentbiomarker identificationbone marrow hyperplasiacombatcounterscreendrug developmentdrug discoveryeffective therapyefficacy evaluationgenome wide association studygenotoxicityhuman genomicshuman induced pluripotent stem cellsin vivoinduced pluripotent stem cellinnovationlead optimizationmedical schoolsmouse modelneurodegenerative phenotypeneuroinflammationnovelnovel therapeuticspharmacokinetics and pharmacodynamicspharmacologicphase 1 studypreclinical developmentpreclinical studyprogramsproto-oncogene protein Spi-1rational designrisk variantsafety studyscale upscreeningsmall moleculesmall molecule therapeuticstooltranscriptome sequencingtranscriptomics

Details

Contact PI/ Project Leader

Name

TSAI, LI-HUEI

Title

PROFESSOR

Contact

Other PIs

Name

GOATE, ALISON M RAY, WILLIAM J

Program Official

Name

REFOLO, LORENZO

Contact

Organization

Name

MASSACHUSETTS INSTITUTE OF TECHNOLOGY

City

CAMBRIDGE

Country

UNITED STATES (US)

Department Type

CHEMISTRY

Organization Type

SCHOOLS OF ARTS AND SCIENCES

State Code

Congressional District

Other Information

Opportunity Number

PAR-18-820

Study Section

ZAG1-ZIJ-6(J3)

Fiscal Year

2024

Award Notice Date

02-May-2024

Administering Institutes or Centers

National Institute on Aging

CFDA Code

866

DUNS Number

001425594

UEI

E2NYLCDML6V1

Project Start Date

15-May-2020

Project End Date

30-April-2026

Budget Start Date

01-May-2024

Budget End Date

30-April-2026

Project Funding Information for 2024

Total Funding

$1,585,167

Direct Costs

$1,495,487

Indirect Costs

$139,303

Year	Funding IC	FY Total Cost by IC
2024	National Institute on Aging	$1,585,167

Sub Projects

No Sub Projects information available for 5U01AG066757-05

Publications

Publications are associated with projects, but cannot be identified with any particular year of the project or fiscal year of funding. This is due to the continuous and cumulative nature of knowledge generation across the life of a project and the sometimes long and variable publishing timeline. Similarly, for multi-component projects, publications are associated with the parent core project and not with individual sub-projects.

No Publications available for 5U01AG066757-05

Patents

No Patents information available for 5U01AG066757-05

Outcomes

The Project Outcomes shown here are displayed verbatim as submitted by the Principal Investigator (PI) for this award. Any opinions, findings, and conclusions or recommendations expressed are those of the PI and do not necessarily reflect the views of the National Institutes of Health. NIH has not endorsed the content below.

No Outcomes available for 5U01AG066757-05

Clinical Studies

No Clinical Studies information available for 5U01AG066757-05

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