| Literature DB >> 30043751 |
Anneleen Daemen1, Bonnie Liu2, Kyung Song2, Mandy Kwong2, Min Gao2, Rebecca Hong2, Michelle Nannini2, David Peterson3, Bianca M Liederer4, Cecile de la Cruz2, Dewakar Sangaraju4, Allan Jaochico4, Xiaofeng Zhao4, Wendy Sandoval5, Thomas Hunsaker2, Ron Firestein6, Sheerin Latham4, Deepak Sampath2, Marie Evangelista3, Georgia Hatzivassiliou7.
Abstract
The enzyme glutaminase (GLS1) is currently in clinical trials for oncology, yet there are no clear diagnostic criteria to identify responders. The evaluation of 25 basal breast lines expressing GLS1, predominantly through its splice isoform GAC, demonstrated that only GLS1-dependent basal B lines required it for maintaining de novo glutathione synthesis in addition to mitochondrial bioenergetics. Drug sensitivity profiling of 407 tumor lines with GLS1 and gamma-glutamylcysteine synthetase (GCS) inhibitors revealed a high degree of co-dependency on both enzymes across indications, suggesting that redox balance is a key function of GLS1 in tumors. To leverage these findings, we derived a pan-cancer metabolic signature predictive of GLS1/GCS co-dependency and validated it in vivo using four lung patient-derived xenograft models, revealing the additional requirement for expression of GAC above a threshold (log2RPKM + 1 ≥ 4.5, where RPKM is reads per kilobase per million mapped reads). Analysis of the pan-TCGA dataset with our signature identified multiple indications, including mesenchymal tumors, as putative responders to GLS1 inhibitors.Entities:
Keywords: GLS1; breast cancer; glutaminase dependence; glutathione synthesis; lung cancer; mesenchymal state; pharmacodynamic biomarkers; predictive gene expression signature; redox stress; tumor metabolism
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Year: 2018 PMID: 30043751 DOI: 10.1016/j.cmet.2018.06.003
Source DB: PubMed Journal: Cell Metab ISSN: 1550-4131 Impact factor: 27.287