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分子生物标志物能否取代可切除结直肠癌肝转移的临床风险评分?

Can molecular biomarkers replace a clinical risk score for resectable colorectal liver metastasis?

作者信息

Veen Torhild, Søreide Kjetil

机构信息

Torhild Veen, Kjetil Søreide, Department of Gastrointestinal Surgery, HPB Unit, Stavanger University Hospital, N-4068 Stavanger, Norway.

出版信息

World J Gastrointest Oncol. 2017 Mar 15;9(3):98-104. doi: 10.4251/wjgo.v9.i3.98.

Abstract

In resectable colorectal liver metastasis (CRLM) the role and use of molecular biomarkers is still controversial. Several biomarkers have been linked to clinical outcomes in CRLM, but none have so far become routine for clinical decision making. For several reasons, the clinical risk score appears to no longer hold the same predictive value. Some of the reasons include the ever expanding indications for liver resection, which now increasingly tend to involve extrahepatic disease, such as lung metastases (both resectable and non-resectable) and the shift in indication from "what is taken out" (., how much liver has to be resected) to "what is left behind" (that is, how much functional liver tissue the patient has after resection). The latter is amenable to modifications by using adjunct techniques of portal vein embolization and the associating liver partition and portal vein ligation for staged hepatectomy techniques to expand indications for liver resection. Added to this complexity is the increasing number of molecular markers, which appear to hold important prognostic and predictive information, for which some will be discussed here. Beyond characteristics of tissue-based genomic profiles will be liquid biopsies derived from circulating tumor cells and cell-free circulating tumor DNA in the blood. These markers are present in the peripheral circulation in the majority of patients with metastatic cancer disease. Circulating biomarkers may represent more readily available methods to monitor, characterize and predict cancer biology with future implications for cancer care.

摘要

在可切除的结直肠癌肝转移(CRLM)中,分子生物标志物的作用和应用仍存在争议。几种生物标志物已与CRLM的临床结局相关联,但迄今为止,尚无一种成为临床决策的常规指标。由于多种原因,临床风险评分似乎不再具有相同的预测价值。其中一些原因包括肝切除适应证的不断扩大,现在越来越多地涉及肝外疾病,如肺转移(包括可切除和不可切除的),以及适应证从“切除了什么”(即需要切除多少肝脏)向“剩下了什么”(即患者切除后剩余多少功能性肝组织)的转变。后者可通过使用门静脉栓塞辅助技术以及联合肝脏分隔和门静脉结扎分期肝切除技术进行调整,以扩大肝切除的适应证。分子标志物数量的不断增加也增加了这种复杂性,这些标志物似乎具有重要的预后和预测信息,本文将讨论其中一些。除了基于组织的基因组图谱特征外,还有源自循环肿瘤细胞和血液中游离循环肿瘤DNA的液体活检。这些标志物在大多数转移性癌症患者的外周循环中都存在。循环生物标志物可能代表更易于获得的方法,用于监测、表征和预测癌症生物学,对未来的癌症治疗具有重要意义。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/a1c6/5348630/91f3793d60e4/WJGO-9-98-g001.jpg

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