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多药耐药的分子细胞遗传学

Molecular cytogenetics of multiple drug resistance.

作者信息

Schoenlein P V

机构信息

Department of Cellular Biology and Anatomy, Medical College of Georgia, Augusta 30912.

出版信息

Cytotechnology. 1993;12(1-3):63-89. doi: 10.1007/BF00744658.

Abstract

The refractory nature of many human cancers to multi-agent chemotherapy is termed multidrug resistance (MDR). In the past several decades, a major focus of clinical and basic research has been to characterize the genetic and biochemical mechanisms mediating this phenomenon. To provide model systems in which to study mechanisms of multidrug resistance, in vitro studies have established MDR cultured cell lines expressing resistance to a broad spectrum of unrelated drugs. In many of these cell lines, the expression of high levels of multidrug resistance developed in parallel to the appearance of cytogenetically-detectable chromosomal anomalies resulting from gene amplification. This review describes cytogenetic and molecular-based studies that have characterized DNA amplification structures in MDR cell lines and describes the important role gene amplification played in the cloning and characterization of the mammalian multidrug resistance genes (mdr). In addition, this review discusses the genetic selection generally used to establish the MDR cell lines, and how drug selections performed in transformed cell lines generally favor the genetic process of gene amplification, which is still exploited to identify drug resistance genes that may play an important role in clinical MDR.

摘要

许多人类癌症对多药化疗具有难治性,这种现象被称为多药耐药(MDR)。在过去几十年中,临床和基础研究的一个主要重点是确定介导这种现象的遗传和生化机制。为了提供研究多药耐药机制的模型系统,体外研究建立了对多种不相关药物具有抗性的MDR培养细胞系。在许多这些细胞系中,高水平多药耐药的表达与基因扩增导致的细胞遗传学可检测染色体异常的出现同时发生。本综述描述了对MDR细胞系中DNA扩增结构进行表征的细胞遗传学和基于分子的研究,并描述了基因扩增在哺乳动物多药耐药基因(mdr)的克隆和表征中所起的重要作用。此外,本综述讨论了通常用于建立MDR细胞系的遗传选择,以及在转化细胞系中进行的药物选择如何通常有利于基因扩增的遗传过程,而这一过程仍被用于鉴定可能在临床MDR中起重要作用的耐药基因。

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