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P-糖蛋白抑制作为克服癌症多药耐药性的治疗方法:现状和未来展望。

P-glycoprotein inhibition as a therapeutic approach for overcoming multidrug resistance in cancer: current status and future perspectives.

机构信息

Faculty of Pharmacy and Pharmaceutical Sciences, University of Alberta, Edmonton, Alberta T6G 2E1, Canada.

出版信息

Curr Cancer Drug Targets. 2013 Mar;13(3):326-46. doi: 10.2174/15680096113139990076.

Abstract

One of the major causes of failure in cancer chemotherapy is multidrug resistance (MDR), where cancer cells simultaneously become resistant to different anticancer drugs. Over-expression of membrane efflux pumps like P-glycoprotein (P-gp) that recognizes different chemotherapeutic agents and transports them out of the cell, plays a major role in MDR. The shortcoming of P-gp inhibitors in clinic has been attributed to their non-specific action on P-gp and/or non-selective distribution to non-target organs that leads to intolerable side effects by the P-gp inhibitor at doses required for P-gp inhibition upon systemic administration. Another major issue is the reduced elimination of P-gp substrates (e.g. anticancer drugs) and intolerable toxicities by anticancer drugs when co-administered with P-gp inhibitors. To overcome these shortcomings, new generation of P-gp inhibitors with improved specificity for P-gp have been developed. More recently, attention has been paid to the use of drug delivery systems primarily to restrict P-gp inhibition to tumor and reduce the non-selective inhibition of P-gp in non-target organs. This review will provide an overview and update on the status of P-gp inhibition approaches and the role of drug delivery systems in overcoming P-gp mediated MDR.

摘要

癌症化疗失败的一个主要原因是多药耐药性(MDR),其中癌细胞同时对不同的抗癌药物产生耐药性。膜外排泵(如 P-糖蛋白(P-gp))的过度表达在 MDR 中起着主要作用,它可以识别不同的化疗药物并将其运出细胞。P-gp 抑制剂在临床上的缺点归因于它们对 P-gp 的非特异性作用和/或非选择性分布到非靶器官,导致在全身给药时需要抑制 P-gp 的剂量下,P-gp 抑制剂产生不可耐受的副作用。另一个主要问题是当与 P-gp 抑制剂共同给药时,P-gp 底物(如抗癌药物)的消除减少和抗癌药物的不可耐受毒性。为了克服这些缺点,已经开发出了新一代对 P-gp 具有改善特异性的 P-gp 抑制剂。最近,人们越来越关注使用药物传递系统,主要是将 P-gp 抑制限制在肿瘤部位,并减少 P-gp 在非靶器官中的非选择性抑制。本文综述了 P-gp 抑制方法的现状和药物传递系统在克服 P-gp 介导的 MDR 中的作用。

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