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多重耐药性

[Multiple drug resistance].

作者信息

Svoboda-Beusan I

机构信息

Imunoloski zavod, Zagreb.

出版信息

Lijec Vjesn. 1994 Jan-Feb;116(1-2):41-5.

PMID:8028439
Abstract

The multidrug-resistance (MDR) phenotype expressed in mammalian cell lines is complex. A cell selected with a single agent can acquire cross-resistance to a remarkably wide range of compounds which have no structural or functional similarities. The basis for cross-resistance seems to be a decreased net cellular accumulation of the drugs involved, and has been attributed to alterations in plasma membrane. An over-expressed plasma membrane P glycoprotein of relative molecular mass of 170 kD (Pgp) is consistently found in different MDR human and animal cell lines, and in transplantable tumors. Consequently, it has been postulated that Pgp directly or indirectly mediates MDR. This paper reviews the current knowledge on etiology, pathogenesis, diagnosis and therapy of MDR.

摘要

哺乳动物细胞系中表达的多药耐药(MDR)表型很复杂。用单一药物筛选出的细胞可获得对大量无结构或功能相似性的化合物的交叉耐药性。交叉耐药的基础似乎是所涉及药物的细胞净积累减少,这归因于质膜的改变。在不同的MDR人和动物细胞系以及可移植肿瘤中一直发现相对分子质量为170 kD的质膜P糖蛋白(Pgp)过度表达。因此,有人推测Pgp直接或间接介导MDR。本文综述了关于MDR的病因、发病机制、诊断和治疗的当前知识。

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