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基于核切除修复的非小细胞肺癌个性化治疗:从假设到现实

Nuclear excision repair-based personalized therapy for non-small cell lung cancer: from hypothesis to reality.

作者信息

Simon George R, Ismail-Khan Roohi, Bepler Gerold

机构信息

H. Lee Moffitt Cancer Center and Research Institute, Tampa, FL, USA.

出版信息

Int J Biochem Cell Biol. 2007;39(7-8):1318-28. doi: 10.1016/j.biocel.2007.05.006. Epub 2007 Jun 12.

DOI:10.1016/j.biocel.2007.05.006
PMID:17600754
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3167070/
Abstract

The crucial 'flaw' in the existing treatment paradigm for non-small cell lung cancer (NSCLC) is the 'one size fits all approach'. Consequently, adjuvant chemotherapy is given to all patients to benefit a minority and, in the metastatic setting doublet chemotherapy only provides modest improvements in response rates and survival. A personalized approach of treatment selection is therefore desperately needed. Genetic information is stored in the chemical structure of DNA. To maintain the structural integrity of DNA, an intricate network of DNA repair systems have evolved. One of these is the nucleotide excision repair (NER), a highly versatile and sophisticated DNA damage removal pathway. We show here that this DNA repair mechanism is instrumental in defining prognosis and response to treatment. ERCC1, one of the proteins in this pathway, is measured to assess its functional status of the NER pathway. In patients with early stage NSCLC, low ERCC1 predicts for relapse and selects for patients who will benefit from adjuvant cisplatin-based chemotherapy. Conversely, ERCC1-positive resected patients have a better intrinsic prognosis and are not likely to benefit from platinum based chemotherapy. In a phase II trial in metastatic disease, we show that by tailoring chemotherapy using ERCC1 and RRM1 we can obtain 1-year survival of 60% (versus approximately 36% in historical controls) and response rates of 42% (versus 25% in historical controls). This approach is currently being validated in a prospective phase III trial. In the future, assessment of NER function may play a central role in NSCLC treatment decision making.

摘要

非小细胞肺癌(NSCLC)现有治疗模式的关键“缺陷”是“一刀切的方法”。因此,对所有患者进行辅助化疗,受益的只是少数患者;而在转移性疾病中,双联化疗仅能适度提高缓解率和生存率。因此,迫切需要一种个性化的治疗选择方法。遗传信息存储在DNA的化学结构中。为维持DNA的结构完整性,一个复杂的DNA修复系统网络已经进化形成。其中之一是核苷酸切除修复(NER),这是一条高度通用且复杂的DNA损伤清除途径。我们在此表明,这种DNA修复机制有助于确定预后和对治疗的反应。该途径中的一种蛋白质ERCC1被检测以评估NER途径的功能状态。在早期NSCLC患者中,低ERCC1预示复发,并筛选出将从基于顺铂的辅助化疗中受益的患者。相反,ERCC1阳性的切除患者有较好的内在预后,不太可能从铂类化疗中受益。在一项转移性疾病的II期试验中,我们表明通过使用ERCC1和RRM1定制化疗,我们可以获得60%的1年生存率(相比历史对照约为36%)和42%的缓解率(相比历史对照为25%)。这种方法目前正在一项前瞻性III期试验中得到验证。未来,NER功能评估可能在NSCLC治疗决策中发挥核心作用。

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本文引用的文献

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Genetic polymorphisms and haplotypes of ERCC1 and ERCC2 associated with quality of life, depression, and anxiety status among patients with lung cancer.肺癌患者 ERCC1 和 ERCC2 基因多态性与生活质量、抑郁和焦虑状态的关联。
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Impact of ERCC2 Gene Polymorphisms on OSCC Susceptibility and Clinical Characteristics.ERCC2基因多态性对口腔鳞状细胞癌易感性及临床特征的影响
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