🗂️

Archived grant — no longer open

This grant has closed and is kept as a historical reference. Browse current grants for active opportunities.

grant

Lactate production by tumor associated macrophages promotes tumorigenesis

Organization UNIVERSITY OF CHICAGOLocation CHICAGO, UNITED STATESPosted 1 Mar 2021Deadline 28 Feb 2026 ⚠️

NIHUS FederalResearch GrantFY2025AdoptedAnimalsAntibodiesAttenuatedB-Cell Stimulatory Factor 1 GeneBSF-1 GeneBSF1 GeneBacteriaBiochemicalBiochemical ProcessBlood monocyteBone MarrowBone Marrow Reticuloendothelial SystemCD8CD8 CellCD8 T cellsCD8 lymphocyteCD8+ T cellCD8+ T-LymphocyteCD8-Positive LymphocytesCD8-Positive T-LymphocytesCD8BCD8B1CD8B1 geneCancer TreatmentCancersCell BodyCellsDevelopmentE1A Binding Protein p300EP300EP300 geneEpigeneticEpigenetic ChangeEpigenetic MechanismEpigenetic ProcessExperimental Animal ModelGEM modelGEMM modelGene ExpressionGene TranscriptionGenesGeneticGenetic TranscriptionGenetically Engineered MouseGlycolysisGoalsHeterogeneityHistonesHumanHypoxiaHypoxicIL-13IL-4 GeneIL13IL4IL4 geneImmuneImmune responseImmunesIn VitroInflammatoryInterleukin-13Interleukin-4 GeneInterleukin-4 Precursor GeneKAT3BKnowledgeL-LysineLDH-ALDH-MLYT3LysineMacrophageMalignant Neoplasm TherapyMalignant Neoplasm TreatmentMalignant NeoplasmsMalignant TumorMarrow monocyteMediatingMetabolicMetastasisMetastasizeMetastatic LesionMetastatic MassMetastatic NeoplasmMetastatic TumorMiceMice MammalsMitochondriaModelingModern ManModificationMolecularMolecular TargetMurineMusMyeloid CellsMφNatureNeoplasm MetastasisOncogenesisOxygen DeficiencyPathway interactionsPatientsPhasePhenotypePrevalenceProcessProductionPrognosisProteinsProteomicsPublishingRNA ExpressionRespirationRoleSecondary NeoplasmSecondary TumorStimulusT-Cell DepletionT-cell depletion therapyT-lymphocyte depletion therapyT8 CellsT8 LymphocytesTeff cellTestingTherapeuticTranscriptionTranslationsTumor ImmunityTumor PromotionTumor-associated macrophagesWorkadaptive immunityangiogenesisanti-canceranti-cancer therapeuticanti-cancer therapyanti-tumor immunityantitumor immunityattenuateattenuatescancer immunitycancer metastasiscancer microenvironmentcancer therapycancer-directed therapycytokinedevelopmentaleffector T cellepigeneticallyexperimentexperimental researchexperimental studyexperimentsgene functiongenetically engineered mouse modelgenetically engineered murine modelhistone acetyltransferase p300host responseimmune system responseimmunoresponseimprovedin vivoinsightlactate dehydrogenase Amalignancymitochondrialmonocyteneoplasm/cancernovelp300pathwaypromoterpromotorrespiratory mechanismsocial roletherapeutic targettranscriptomicstranslationtumortumor cell metastasistumor growthtumor microenvironmenttumorigenesis

Applications closed.

Description preview

ABSTRACT
Tumor-associated macrophages (TAMs) are the most prevalent immune cell in the tumor microenvironment.
TAMs adopt an M2-like phenotype that supports angiogenesis, attenuates anti-cancer immune responses, and
facilitates metastatic dissemination. Studies in humans and experimental animal models support targeting
TAMs for anti-cancer…

🔒

Full details available on the Agency plan

Unlock the complete grant description, eligibility criteria, contract value, evaluation details and apply link — plus alerts, pipeline tracking, and CSV export.

Start 7-day free trial — $29.99/mo →

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

More from UNIVERSITY OF CHICAGO

All grants from UNIVERSITY OF CHICAGO →