| Literature DB >> 30874300 |
Amit Subedi1, Makoto Muroi1, Yushi Futamura1, Tatsuro Kawamura2, Harumi Aono1, Mayuko Nishi3, Akihide Ryo3, Nobumoto Watanabe2,4, Hiroyuki Osada1,2.
Abstract
Differences in the metabolism of cancer cells or cancer stem cells (CSCs) as compared to normal cells have provided avenues to safely target cancers. To discover metabolic inhibitors of CSCs, we performed alkaline phosphatase- and tumoursphere-based drug screening using induced cancer stem cell-like cells. From the screening of a RIKEN NPDepo chemical library, we discovered NPD2381 as a novel and selective cancer-stemness inhibitor that targets mitochondrial metabolism. Using our ChemProteoBase profiling, we found that NPD2381 increases the expression of enzymes within the serine biosynthesis pathway. We also found a role for serine in protecting cancer cells from mitochondrial inhibitors. Our results suggest the existence of a compensatory mechanism to increase the level of intracellular serine in response to mitochondrial inhibitors.Entities:
Keywords: cancer metabolism; cancer stem cells; drug screen; mitochondrial inhibitors; serine biosynthesis; tumourspheres
Year: 2019 PMID: 30874300 DOI: 10.1002/1873-3468.13361
Source DB: PubMed Journal: FEBS Lett ISSN: 0014-5793 Impact factor: 4.124