个性化胰腺癌治疗:当组织成为问题时。
Personalising pancreas cancer treatment: When tissue is the issue.
作者信息
Sjoquist Katrin M, Chin Venessa T, Chantrill Lorraine A, O'Connor Chelsie, Hemmings Chris, Chang David K, Chou Angela, Pajic Marina, Johns Amber L, Nagrial Adnan M, Biankin Andrew V, Yip Desmond
机构信息
Katrin M Sjoquist, NHMRC Clinical Trials Centre, University of Sydney, Sydney NSW 1450, Australia.
出版信息
World J Gastroenterol. 2014 Jun 28;20(24):7849-63. doi: 10.3748/wjg.v20.i24.7849.
Abstract
The treatment of advanced pancreatic cancer has not moved much beyond single agent gemcitabine until recently when protocols such as FOLFIRINOX (fluorouracil, leucovorin, irinotecan and oxaliplatin) and nab-paclitaxel-gemcitabine have demonstrated some improved outcomes. Advances in technology especially in massively parallel genome sequencing has progressed our understanding of the biology of pancreatic cancer especially the candidate signalling pathways that are involved in tumourogenesis and disease course. This has allowed identification of potentially actionable mutations that may be targeted by new biological agents. The heterogeneity of pancreatic cancer makes tumour tissue collection important with the aim of being able to personalise therapies for the individual as opposed to a one size fits all approach to treatment of the condition. This paper reviews the developments in this area of translational research and the ongoing clinical studies that will attempt to move this into the everyday oncology practice.
摘要
直到最近,如FOLFIRINOX(氟尿嘧啶、亚叶酸钙、伊立替康和奥沙利铂)和纳米白蛋白结合型紫杉醇-吉西他滨等方案显示出一些改善的结果之前,晚期胰腺癌的治疗一直没有太多超越单药吉西他滨的进展。技术的进步,特别是大规模平行基因组测序技术的进步,加深了我们对胰腺癌生物学的理解,尤其是对参与肿瘤发生和疾病进程的候选信号通路的理解。这使得识别可能被新型生物制剂靶向的潜在可操作突变成为可能。胰腺癌的异质性使得肿瘤组织采集变得重要,目的是能够为个体量身定制治疗方案,而不是采用一刀切的方法来治疗这种疾病。本文综述了这一转化研究领域的进展以及正在进行的临床研究,这些研究将试图把这一领域的成果应用到日常肿瘤学实践中。
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