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ERCC1 和 RRM1:准备好首秀了吗?

ERCC1 and RRM1: ready for prime time?

机构信息

Université Paris Sud, Kremlin-Bicêtre, France.

出版信息

J Clin Oncol. 2013 Mar 10;31(8):1050-60. doi: 10.1200/JCO.2012.43.0900. Epub 2013 Feb 11.

Abstract

The quest for markers of sensitivity to cytotoxic agents has been ongoing for decades. In non-small-cell lung cancer, platinum compounds represent the cornerstone of systemic therapy. They target DNA and induce damage that cancer cells struggle to overcome. Somatic excision repair cross-complementing rodent repair deficiency, complementation group 1 (ERCC1), and ribonucleotide reductase M1 (RRM1) expression levels have been extensively explored as markers of DNA repair capacity in tumor cells. Although low ERCC1 and/or RRM1 expression is generally associated with sensitivity to platinum, the results published in retrospective and prospective studies are not always consistent. Against this background, we will examine in this review the function of these two biomarkers as well as the tools available for their assessment and the associated technical issues. Their prognostic and predictive values will be summarized and considered in terms of customizing systemic therapy according to biomarker (ERCC1 and RRM1) expression levels. We will also discuss why the use of both markers should at this point be restricted to clinical research and underline that functional readouts of DNA repair will help boost future strategies for biomarker discovery in the field.

摘要

几十年来,人们一直在寻找对细胞毒性药物敏感的标志物。在非小细胞肺癌中,铂类化合物是系统治疗的基石。它们靶向 DNA 并诱导癌细胞难以克服的损伤。体细胞切除修复交叉互补鼠修复缺陷,互补组 1(ERCC1)和核昔酸还原酶 M1(RRM1)的表达水平已被广泛探索作为肿瘤细胞 DNA 修复能力的标志物。尽管低 ERCC1 和/或 RRM1 表达通常与铂类药物的敏感性相关,但回顾性和前瞻性研究的结果并不总是一致。在此背景下,我们将在这篇综述中检查这两个生物标志物的功能以及用于评估它们的工具和相关技术问题。将总结它们的预后和预测价值,并根据生物标志物(ERCC1 和 RRM1)表达水平来考虑对系统治疗进行定制。我们还将讨论为什么目前应该将这两个标志物的使用仅限于临床研究,并强调 DNA 修复的功能读数将有助于推动该领域生物标志物发现的未来策略。

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