grant

Identifying regulatory uORFs as a targetable axis for hereditary disease

Organization UNIVERSITY OF PENNSYLVANIALocation PHILADELPHIA, UNITED STATESPosted 23 Sept 2022Deadline 31 May 2027
NIHUS FederalResearch GrantFY20255' Untranslated Regions5'UTRAffectAssayBMPR-IIBMPR2BMPR2 geneBRK-3 proteinBackBioassayBiological AssayBiologyBone Morphogenetic Protein Receptor, Type II (Serine/Threonine Kinase) GeneCell BodyCellsCodeCoding SystemCommunitiesComputer ModelsComputerized ModelsCoupledDNA Molecular BiologyDataData BasesData SetDatabasesDiseaseDisorderDorsumEvolutionExhibitsFutureGene ProteinsGene variantGenesGeneticGenetic Data BanksGenetic Data BasesGenetic DatabanksGenetic DatabasesGenetic DiseasesGenetic Information DatabasesGenomicsGoalsGrantHealthHereditary DiseaseHeritabilityHumanInborn Genetic DiseasesInherited disorderInitiation CodonInitiator CodonLinkLuciferase ImmunologicLuciferasesMapsMessenger RNAModern ManMolecular BiologyMutateNon-Polyadenylated RNAORFsOpen Reading FramesOutputPathway interactionsPatientsPeptidesPhenotypeProtein Coding RegionProtein Gene ProductsProteinsPublishingRNARNA Gene ProductsRNA ProcessingRegulatory ElementReporterResearch ResourcesResourcesRestRibo-seqRibonucleic AcidRoleSignal PathwayStart CodonStop CodonTermination CodonTerminator CodonTestingTherapeuticTherapeutic InterventionTranslation Stop SignalTranslationsValidationVariantVariationWorkallelic variantbiobankbiorepositorybone morphogenetic protein receptor IIbone morphogenetic protein receptor type IIclinical relevanceclinically relevantcomputational modelingcomputational modelscomputational pipelinescomputer based modelscomputerized modelingdata basedesigndesigningdisease phenotypedosageexperimentexperimental researchexperimental studyexperimentsgenetic conditiongenetic disordergenetic variantgenomic varianthereditary disorderheritable disorderimprovedinborn errorinherited diseasesinherited genetic diseaseinherited genetic disorderintervention therapymRNAmRNA Leader Sequencesnovelpathwaypreservationprotein expressionpulmonary arterial hypertensionpulmonary artery hypertensionribosome footprint profilingribosome profilingsocial roletranslationtranslation strategytranslational approachtranslational strategytype II BMP receptoruser-friendlyvalidationsweb toolweb-based tool
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Full Description

Abstract The aim of this grant is to identify and validate for therapeutic intervention, regulatory elements within the 5’ untranslated regions (UTR) of protein coding genes, known as upstream open reading frames (uORFs). In so doing, we aim to modulate the protein output from selected genes, offering a novel, translational approach with broad potential. To achieve the goals of our integrative MultiPI R01, we will leverage the expertise of both our labs spanning computational modeling, genomics, genetics, RNA biology and molecular biology. In Aim 1 we will combine large genomic and genetic datasets including gnomAD, the PennMedicine BioBank, and the UKBioBank to systematically identify functional uORFs and prioritize those for validation.

The resulting database of human uORFs will be made publicly available and widely accessible as a user-friendly web-tool. Predicted regulatory uORFs suggested by the Aim 1 pipeline will be fed into the experimental Aim 2. In Aim 2 we will validate the high-priority uORF targets using luciferase assays. The results of Aims 2 will be fed back to the pipeline of Aim1 to improve prioritization of future uORFs.

Overall, we expect the resources and discoveries made by this grant to shed light on the functional role of uORFs and offer therapeutic avenues for several hereditary diseases.

Grant Number: 5R01GM147739-04
NIH Institute/Center: NIH

Principal Investigator: Yoseph Barash

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