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Developmental Therapeutics Research Program

$53,112P30FY2021CANIH

Case Western Reserve University, Cleveland OH

Investigators

Linked publications, trials & patents

Trial NCT05340673Trial NCT05198830Trial NCT02590107Trial NCT02535325Trial NCT02451124Trial NCT02419846Trial NCT02417948Trial NCT02392377Trial NCT02388932Trial NCT02383433Trial NCT02375477Trial NCT02354326Trial NCT02345460Trial NCT02342730Trial NCT02337465Trial NCT02327390Trial NCT02319889Trial NCT02307474Trial NCT02287636Trial NCT02252393Trial NCT02181478Trial NCT02179762Trial NCT02163317Trial NCT02158767Trial NCT02153450Trial NCT02135562Trial NCT02131207Trial NCT02129582Trial NCT02129569Trial NCT02129517Trial NCT02129218Trial NCT02128373Trial NCT02108587Trial NCT02100423Trial NCT02084147Trial NCT02082405Trial NCT02081794Trial NCT02079155Trial NCT02073097Trial NCT02073045Trial NCT02071901Trial NCT02070458Trial NCT02070419Trial NCT02055586Trial NCT02037048Trial NCT01973062Trial NCT01959490Trial NCT01959477Trial NCT01954784Trial NCT01954732Trial NCT01951885Trial NCT01939028Trial NCT01928485Trial NCT01894061Trial NCT01408043Trial NCT00991991Trial NCT00970684Trial NCT00961220Trial NCT00956475Trial NCT00952939Trial NCT00949247Trial NCT00945061Trial NCT00941720Trial NCT00941070Trial NCT00939510Trial NCT00918892Trial NCT00918788Trial NCT00918658Trial NCT00918216Trial NCT00910039Trial NCT00909662Trial NCT00908739Trial NCT00908141Trial NCT00907699Trial NCT00905086Trial NCT00900133Trial NCT00899158Trial NCT00899132Trial NCT00898573Trial NCT00898274Trial NCT00897143Trial NCT00892385Trial NCT00873600Trial NCT00873002Trial NCT00866320Trial NCT00856115Trial NCT00853021Trial NCT00842452Trial NCT00809185Trial NCT00796978Trial NCT00795678Trial NCT00769951Trial NCT00769249Trial NCT00752323Trial NCT00740961Trial NCT00736216Trial NCT00735514Trial NCT00733252Trial NCT00732745Trial NCT00732173

Abstract

DEVELOPMENTAL THERAPEUTICS (DT) RESEARCH PROGRAM PROJECT SUMMARY/ABSTRACT The Developmental Therapeutics (DT) Research Program develops and evaluates novel therapeutics and combinations that: 1) overcome drug resistance of cancer cells mediated by a spectrum of genetic and epigenetic mechanisms; 2) inhibit growth and drug-resistant pathways of cancer; and 3) utilize novel immune checkpoint therapeutics to increase the proportion of cancer patients who benefit. The overall approach of the DT Program is to leverage the creativity and expertise of basic scientists in the Case Comprehensive Cancer Center (Case CCC) Programs by analyzing new agents for specific validated molecular targets and new therapeutic compounds for preclinical and clinical validation in early-phase clinical trials. DT members guide their development, and convey clinical samples back to laboratory investigators to drive further discovery. This bidirectional interchange enables DT's continued role as a major convener of new therapeutic concepts for the Center?s Programs. The program is organized around 3 scientific aims: (1) Interrogate cancer pathways to develop new efficacious therapeutics; (2) Implement early-phase clinical trials around novel pathway targets, new agents and combinatorial approaches; and (3) Implement early-phase trials around novel approaches to cancer immunotherapies, to widen their activity spectra. These aims reflect major working groups and initiatives that coalesces program members with other cancer center investigators through inter-programmatic collaborations that result in preclinical and clinical research efforts, grants, and trial protocols. Extensive use of an array of shared resources, in particular Translational, Cytometry, Imaging, Proteomics, and Drug Discovery facilitate all aspects of member discoveries. Under the leadership of Yogen Saunthararajah (Co-Leader) and John Letterio (Co-Leader) the DT Program has 52 members including 18 full, 5 associate and 29 clinical members representing 21 different departments across the consortium. Members are funded by a total of $12.5M in research grant funding (annual direct costs), of which $5.1M is peer-reviewed and $2.9M is NCI-funded. Between 2012 and 2016, DT program members published 1,012 publications. Cancer and program related publications included 35% inter- programmatic, 25% intra-programmatic, 14% inter- and intra-programmatic and 10% that involved collaborations with another Cancer Center. This highly effective Program has made major practice-changing contributions benefiting cancer patients. Examples include: discoveries of first-in-class compounds (SMARCA5 inhibitor, PP2A activator, malate dehydrogenase inhibitor, base excision repair target with methoxyamine); discoveries targeting EGFR resistance, inhibition of uracil glycosylase and the inhibition of the BH4 domain of Bcl-2; analysis into the genetic markers of resistance to radiation; and identification of several small cell lung cancer genetic subsets. !

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