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Data from A Novel Role for DNA-PK in Metabolism by Regulating Glycolysis in Castration-Resistant Prostate Cancer

Authors :
Karen E. Knudsen
William K. Kelly
Jeff Holst
Lisa M. Butler
Jason S. Carroll
Erin L. Seifert
Leonard G. Gomella
Peter A. McCue
Costas D. Lallas
Matthew J. Schiewer
Irina Vasilevskaya
Christopher M. McNair
Saswati Chand
Amy C. Mandigo
Jennifer J. McCann
Swati Irani
Jonathan F. Goodwin
Angel Pang
Yi F. Guan
Peter T. Gallagher
Galina Semenova
Ayesha A. Shafi
Vishal Kothari
Emanuela Dylgjeri
Publication Year :
2023
Publisher :
American Association for Cancer Research (AACR), 2023.

Abstract

Purpose:DNA-dependent protein kinase catalytic subunit (DNA-PKcs, herein referred as DNA-PK) is a multifunctional kinase of high cancer relevance. DNA-PK is deregulated in multiple tumor types, including prostate cancer, and is associated with poor outcomes. DNA-PK was previously nominated as a therapeutic target and DNA-PK inhibitors are currently undergoing clinical investigation. Although DNA-PK is well studied in DNA repair and transcriptional regulation, much remains to be understood about the way by which DNA-PK drives aggressive disease phenotypes.Experimental Design:Here, unbiased proteomic and metabolomic approaches in clinically relevant tumor models uncovered a novel role of DNA-PK in metabolic regulation of cancer progression. DNA-PK regulation of metabolism was interrogated using pharmacologic and genetic perturbation using in vitro cell models, in vivo xenografts, and ex vivo in patient-derived explants (PDE).Results:Key findings reveal: (i) the first-in-field DNA-PK protein interactome; (ii) numerous DNA-PK novel partners involved in glycolysis; (iii) DNA-PK interacts with, phosphorylates (in vitro), and increases the enzymatic activity of glycolytic enzymes ALDOA and PKM2; (iv) DNA-PK drives synthesis of glucose-derived pyruvate and lactate; (v) DNA-PK regulates glycolysis in vitro, in vivo, and ex vivo; and (vi) combination of DNA-PK inhibitor with glycolytic inhibitor 2-deoxyglucose leads to additive anti-proliferative effects in aggressive disease.Conclusions:Findings herein unveil novel DNA-PK partners, substrates, and function in prostate cancer. DNA-PK impacts glycolysis through direct interaction with glycolytic enzymes and modulation of enzymatic activity. These events support energy production that may contribute to generation and/or maintenance of DNA-PKā€“mediated aggressive disease phenotypes.

Details

Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....be2b7964efd7d533fa2a0b6b1fd5226a
Full Text :
https://doi.org/10.1158/1078-0432.c.6531392