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Modulation of Multidrug Resistance in Cancer by P-Glycoprotein

원문정보

Changdev G. Gadhe, Seung Joo Cho

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초록

영어

Multidrug resistance (MDR) is one of the main obstacles in the chemotherapy of cancer. MDR is associated with the over expression of P-glycoprotein (P-gp), resulting in increased efflux of chemotherapy from cancer cells. Inhibiting Pgp as a method to reverse MDR in cancer patients has been studied extensively, but the results have generally been disappointing. First-generation agents were limited by unacceptable toxicity, whereas second-generation agents had better tolerability but were confounded by unpredictable pharmacokinetic interactions and interactions with other transporter proteins. Third-generation inhibitors have high potency and specificity for P-gp. Furthermore, pharmacokinetic studies to date have shown no appreciable impact on drug metabolism and no clinically significant drug interactions with common chemotherapy agents. Third-generation P-gp inhibitors have shown promise in clinical trials. The continued development of these agents may establish the true therapeutic potential of P-gp-mediated MDR reversal.

목차

Abstract
 1. Introduction
 2. Experimental Section
  2.1. Domain Organization
  2.2. Drug Binding and Transport
  2.3. Polyspecificity of Drug Binding Pocket
  2.4. P-gp Modulators
 3. Result and Discussion
 References

저자정보

  • Changdev G. Gadhe Department of Bio-New Drug Development, College of Medicine, Chosun University
  • Seung Joo Cho Department of Bio-New Drug Development, College of Medicine, Chosun University, Department of Cellular·Molecular Medicine and Research Center for Resistant Cells, College of Medicine, Chosun University

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