| Literature DB >> 28263311 |
Peter M Bruno1,2, Yunpeng Liu1,2, Ga Young Park3, Junko Murai4, Catherine E Koch1,2, Timothy J Eisen2,5, Justin R Pritchard1,2, Yves Pommier4, Stephen J Lippard1,3, Michael T Hemann1,2.
Abstract
Cisplatin and its platinum analogs, carboplatin and oxaliplatin, are some of the most widely used cancer chemotherapeutics. Although cisplatin and carboplatin are used primarily in germ cell, breast and lung malignancies, oxaliplatin is instead used almost exclusively to treat colorectal and other gastrointestinal cancers. Here we utilize a unique, multi-platform genetic approach to study the mechanism of action of these clinically established platinum anti-cancer agents, as well as more recently developed cisplatin analogs. We show that oxaliplatin, unlike cisplatin and carboplatin, does not kill cells through the DNA-damage response. Rather, oxaliplatin kills cells by inducing ribosome biogenesis stress. This difference in drug mechanism explains the distinct clinical implementation of oxaliplatin relative to cisplatin, and it might enable mechanistically informed selection of distinct platinum drugs for distinct malignancies. These data highlight the functional diversity of core components of front-line cancer therapy and the potential benefits of applying a mechanism-based rationale to the use of our current arsenal of anti-cancer drugs.Entities:
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Year: 2017 PMID: 28263311 PMCID: PMC5520548 DOI: 10.1038/nm.4291
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440