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

Abstract: Purpose: DNA-dependent 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 (PCa), and is associated with poor outcomes. DNA-PK was previously nominated as a therapeutic target and DNA-PK inhibitors are currently undergoing clinical investigation. While DNA-PK is well studied in DNA repair and transcriptional regulation, much remains to be understood about the way by which DN… Show more

“…Interestingly, upstream stimulatory factor (USF) 1/2 heterodimer has been shown to be phosphorylated by DNA-PKcs resulting in fatty acid synthase (FASN) promoter activation ( Wong et al, 2009 ). Consistent with this, Dylgjeri et al (2022) have also found FASN as one of the novel DNA-PK partners, indicating an essential role of DNA-PKcs in regulating the cellular metabolism.…”

“…While we have long been appreciating the role of DNA-PKcs in DNA DSB repair mechanism, recent evidence highlighting a significant amount of DNA-PKcs being present in the cytoplasm ( Dylgjeri et al, 2022 ) suggests the novel role of DNA-PKcs in cells. By performing DNA-PK protein interactome, Dylgjeri et al (2022) have reported novel interacting partners of DNA-PK, including those involved in ribonucleic acid metabolism (DOT1L [histone methyltransferase], RPLs [L ribosomal proteins], HNRPs [heterogeneous nuclear ribonucleoprotein Ks], eEFs [eukaryotic elongation factors]), energy metabolism (PGK1, PKM2, FASN, VDAC-2 [voltage-dependent anion channel-2]), heat shock proteins (HSPs), zinc finger proteins (ZNFs), and inflammation (MIF [macrophage migration inhibitory factor]). This suggests that inhibition of DNA-PK is likely to inhibit multi-substrates at multiple locations (nucleus and cytoplasm), which may yield a complex outcome.…”

“…Despite the role of DNA-PKcs in the nucleus, recent evidence suggests that approximately 20% of the total DNA-PKcs protein levels have been detected in the cytoplasm of castration-resistant prostate cancer cells ( Dylgjeri et al, 2022 ). Furthermore, this study has demonstrated that DNA-PKcs promotes Warburg effect through phosphorylation of various enzymes involved in the glycolytic pathway including glyceraldehyde 3 phosphate dehydrogenase (GAPDH), phosphoglycerate kinase 1 (PGK1), enolase 1, and pyruvate kinase M2 (PKM2), hence suggesting that inhibition of DNA-PK in conjunction with aerobic glycolysis would increase antitumor efficacy ( Dylgjeri et al, 2022 ) ( Fig. 1 ).…”

DNA-Dependent Protein Kinase Catalytic Subunit (DNA-PKcs): Beyond the DNA Double-Strand Break Repair

“…Interestingly, upstream stimulatory factor (USF) 1/2 heterodimer has been shown to be phosphorylated by DNA-PKcs resulting in fatty acid synthase (FASN) promoter activation ( Wong et al, 2009 ). Consistent with this, Dylgjeri et al (2022) have also found FASN as one of the novel DNA-PK partners, indicating an essential role of DNA-PKcs in regulating the cellular metabolism.…”

“…While we have long been appreciating the role of DNA-PKcs in DNA DSB repair mechanism, recent evidence highlighting a significant amount of DNA-PKcs being present in the cytoplasm ( Dylgjeri et al, 2022 ) suggests the novel role of DNA-PKcs in cells. By performing DNA-PK protein interactome, Dylgjeri et al (2022) have reported novel interacting partners of DNA-PK, including those involved in ribonucleic acid metabolism (DOT1L [histone methyltransferase], RPLs [L ribosomal proteins], HNRPs [heterogeneous nuclear ribonucleoprotein Ks], eEFs [eukaryotic elongation factors]), energy metabolism (PGK1, PKM2, FASN, VDAC-2 [voltage-dependent anion channel-2]), heat shock proteins (HSPs), zinc finger proteins (ZNFs), and inflammation (MIF [macrophage migration inhibitory factor]). This suggests that inhibition of DNA-PK is likely to inhibit multi-substrates at multiple locations (nucleus and cytoplasm), which may yield a complex outcome.…”

“…Despite the role of DNA-PKcs in the nucleus, recent evidence suggests that approximately 20% of the total DNA-PKcs protein levels have been detected in the cytoplasm of castration-resistant prostate cancer cells ( Dylgjeri et al, 2022 ). Furthermore, this study has demonstrated that DNA-PKcs promotes Warburg effect through phosphorylation of various enzymes involved in the glycolytic pathway including glyceraldehyde 3 phosphate dehydrogenase (GAPDH), phosphoglycerate kinase 1 (PGK1), enolase 1, and pyruvate kinase M2 (PKM2), hence suggesting that inhibition of DNA-PK in conjunction with aerobic glycolysis would increase antitumor efficacy ( Dylgjeri et al, 2022 ) ( Fig. 1 ).…”

DNA-Dependent Protein Kinase Catalytic Subunit (DNA-PKcs): Beyond the DNA Double-Strand Break Repair

“…DNA-PKcs, when present in the nucleus contributes to repair and the regulation of transcription, but in the cytoplasm [63], it also has functions in energy metabolism [64], fatty acid synthesis [65] and aging [66]. Although the functions of DNA-PKcs continue to expand [67], its involvement in c-NHEJ has received the most attention and has been profoundly enriched by recent structural studies revealing intriguing aspects of its function in this repair pathway [68,69]. The work presented here helps to further develop and consolidate the functions of DNA-PKcs related to resection.…”

Increased Resection at DSBs in G2-Phase Is a Unique Phenotype Associated with DNA-PKcs Defects That Is Not Shared by Other Factors of c-NHEJ

“…Metabolically, PKM2 has reduced enzymatic activity and slows down pyruvate production, allowing more upstream biomolecules to be available for other biosynthetic processes [ 137 ]. A recent report suggests that deoxyribonucleic acid (DNA)-dependent protein kinase (DNA-PK) may play a role in regulating increased glycolytic flux by phosphorylating aldolase and PKM2 to increase their enzymatic activities [ 138 ]. Interestingly, PKM2 also possess non-metabolic kinase activity and can function as a transcription factor, thereby promoting metastasis and regulating responses to hypoxia in PCa [ 139 , 140 , 141 , 142 , 143 ].…”

Druggable Metabolic Vulnerabilities Are Exposed and Masked during Progression to Castration Resistant Prostate Cancer