Abstract
Annual Review of Pharmacology and Toxicology
Vol. 48:
495-535
(Volume publication date February 2008)
(doi:10.1146/annurev.pharmtox.48.080907.180426)
First published online as a Review in Advance on October 15, 2007The Role of Cellular Accumulation in Determining Sensitivity to Platinum-Based Chemotherapy * Matthew D. Hall, Mitsunori Okabe, Ding-Wu Shen, Xing-Jie Liang, and Michael M. GottesmanLaboratory of Cell Biology, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892-4255; email: mgottesman@nih.gov The platinum (Pt) drugs cisplatin and carboplatin are heavily employed in chemotherapy regimens; however, similar to other classes of drugs, a number of intrinsic and acquired resistance mechanisms hamper their effectiveness. The method by which Pt drugs enter cells has traditionally been attributed to simple passive diffusion. However, recent evidence suggests a number of active uptake and efflux mechanisms are at play, and altered regulation of these transporters is responsible for the reduced accumulation of drug in resistant cells. This review suggests a model that helps reconcile the disparate literature by describing multiple pathways for Pt-containing drugs into and out of the cell. Platinum Anticancer Coordination Compounds: Study of DNA Binding Inspires New Drug Design European Journal of Inorganic Chemistry 2009(10):1303-1312 (2009) Expression of Na,K-ATPase-β1 subunit increases uptake and sensitizes carcinoma cells to oxaliplatin Cancer Chemotherapy and Pharmacology (2009) Glucose-regulated protein 78 antagonizes cisplatin and adriamycin in human melanoma cells Carcinogenesis 30(2):197-204 (2008)
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