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肾细胞癌的突变。

Mutations in renal cell carcinoma.

机构信息

Department of Hematology/Oncology, Fox Chase Cancer Center, Philadelphia, PA.

Molecular Therapeutics, Fox Chase Cancer Center, Temple Health, Philadelphia, PA; Department of Urology, Einstein Medical Center, Philadelphia, PA.

出版信息

Urol Oncol. 2020 Oct;38(10):763-773. doi: 10.1016/j.urolonc.2018.10.027. Epub 2018 Nov 23.

DOI:10.1016/j.urolonc.2018.10.027
PMID:30478013
Abstract

Renal cell carcinoma (RCC) is a commonly diagnosed and histologically diverse urologic malignancy. Clear cell RCC (ccRCC) is by far the most common, followed by the papillary and chromophobe subtypes. Sarcomatoid differentiation is a morphologic change that can be seen in all subtypes that typically portends a poor prognosis. In the past, treatment options for RCC were limited to cytokine-based therapy with a high-toxicity profile and low response rate. An increased understanding of the molecular basis of RCC has led to substantial improvement in treatment options in the form of targeted therapy and immunotherapy. A significant early discovery in RCC was frequent inactivation of the Von Hippel Lindau gene in ccRCC, which ultimately led to the development of vascular endothelial growth factor and mammalian target of rapamycin inhibitors. Further genomic sequencing of ccRCC tumors has identified other common mutations including BAP-1, PBRM1, SETD2, and PIK3CA. Many recent studies have explored how these mutations can affect prognosis and response to treatment. Likewise, papillary RCC has also been studied at the molecular level, which has shown a high level of mutations in the MET gene; early clinical data suggest the utility of MET targeted therapy. Finally, regarding the rarer sarcomatoid tumors, mutations in TP53 and NF2 may be important to their development. As we continue to learn more about what drives RCC at the molecular level, treatment options for RCC patients are diversifying.

摘要

肾细胞癌(RCC)是一种常见的诊断和组织学多样化的泌尿系统恶性肿瘤。透明细胞 RCC(ccRCC)是迄今为止最常见的,其次是乳头状和嫌色细胞亚型。肉瘤样分化是一种形态学改变,可在所有亚型中看到,通常预示着预后不良。过去,RCC 的治疗选择仅限于细胞因子为基础的治疗,具有高毒性和低反应率。对 RCC 的分子基础的认识增加,导致了靶向治疗和免疫治疗等治疗选择的显著改善。RCC 的一个重要早期发现是 ccRCC 中 Von Hippel Lindau 基因的频繁失活,这最终导致了血管内皮生长因子和哺乳动物雷帕霉素靶蛋白抑制剂的开发。对 ccRCC 肿瘤的进一步基因组测序已经确定了其他常见的突变,包括 BAP-1、PBRM1、SETD2 和 PIK3CA。许多最近的研究都探讨了这些突变如何影响预后和对治疗的反应。同样,在分子水平上也对乳头状 RCC 进行了研究,这表明 MET 基因的突变水平很高;早期的临床数据表明 MET 靶向治疗的有效性。最后,对于更罕见的肉瘤样肿瘤,TP53 和 NF2 的突变可能对其发展很重要。随着我们对 RCC 在分子水平上的驱动因素了解得越来越多,RCC 患者的治疗选择也在多样化。

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