| Literature DB >> 33615182 |
Verena Apfel1, Damien Begue2, Valentina Cordo'1, Laura Holzer1, Laetitia Martinuzzi1, Alexandra Buhles1, Grainne Kerr1, Ines Barbosa1, Ulrike Naumann2, Michelle Piquet3, David Ruddy3, Andreas Weiss1, Stephane Ferretti1, Reinaldo Almeida4, Debora Bonenfant2, Luca Tordella1, Giorgio G Galli1.
Abstract
Asparagine deprivation by l-asparaginase (L-ASNase) is an effective therapeutic strategy in acute lymphoblastic leukemia, with resistance occurring due to upregulation of ASNS, the only human enzyme synthetizing asparagine (Annu. Rev. Biochem. 2006, 75 (1), 629-654). l-Asparaginase efficacy in solid tumors is limited by dose-related toxicities (OncoTargets and Therapy 2017, pp 1413-1422). Large-scale loss of function genetic in vitro screens identified ASNS as a cancer dependency in several solid malignancies (Cell 2017, 170 (3), 564-576.e16. Cell 2017, 170 (3), 577-592.e10). Here we evaluate the therapeutic potential of targeting ASNS in melanoma cells. While we confirm in vitro dependency on ASNS silencing, this is largely dispensable for in vivo tumor growth, even in the face of asparagine deprivation, prompting us to characterize such a resistance mechanism to devise novel therapeutic strategies. Using ex vivo quantitative proteome and transcriptome profiling, we characterize the compensatory mechanism elicited by ASNS knockout melanoma cells allowing their survival. Mechanistically, a genome-wide CRISPR screen revealed that such a resistance mechanism is elicited by a dual axis: GCN2-ATF4 aimed at restoring amino acid levels and MAPK-BCLXL to promote survival. Importantly, pharmacological inhibition of such nodes synergizes with l-asparaginase-mediated asparagine deprivation in ASNS deficient cells suggesting novel potential therapeutic combinations in melanoma.Entities:
Year: 2021 PMID: 33615182 PMCID: PMC7887857 DOI: 10.1021/acsptsci.0c00196
Source DB: PubMed Journal: ACS Pharmacol Transl Sci ISSN: 2575-9108