Tsilimigras Diamantis I, Ntanasis-Stathopoulos Ioannis, Bagante Fabio, Moris Demetrios, Cloyd Jordan, Spartalis Eleftherios, Pawlik Timothy M
School of Medicine, National and Kapodistrian University of Athens, Athens, Greece; Laboratory of Experimental Surgery and Surgical Research, School of Medicine, National and Kapodistrian University of Athens, Athens, Greece.
School of Medicine, National and Kapodistrian University of Athens, Athens, Greece.
Surg Oncol. 2018 Jun;27(2):280-288. doi: 10.1016/j.suronc.2018.05.012. Epub 2018 May 8.
Hepatic resection is considered the optimal potentially curative treatment for colorectal liver metastases (CRLM). Following resection, up to two-thirds of patients will develop recurrence within 5-years. Genetic mutation analysis of CRLM, especially KRAS status, has been proposed as a means to guide treatment, as well as identifying patients who can derive the most survival benefit from hepatic resection.
A systematic review of the literature was conducted the PubMed, Embase and Cochrane library through February 8th, 2018. The following algorithm was applied: "(colorectal OR rectal OR colon OR colonic) AND (liver OR hepatic) AND (metastasis OR metastases) AND (gene OR mutation OR KRAS OR BRAF OR SMAD4 OR RAS OR TP53 OR P53 OR APC OR PI3K OR MSI OR EGFR OR MACC1 OR microsatellite)."
From the 2404 records retrieved, 78 studies were finally deemed eligible; 47 studies reported mutational data on patients with resectable CRLM, whereas 31 studies reported on patients with unresectable CRLM. Mutational analyses were mostly performed on the CRLM specimen rather than the primary CRC. The vast majority of studies reported on the KRAS mutational status (88.5%, n = 69/78). Prevalence of KRAS mutations ranged from 25% to 52%. Most studies reported that RAS mutation was a negative prognostic factor for overall (OS) (n = 24) and recurrence-free (RFS) (n = 9) survival; a few reports noted no effect of RAS mutational status on OS (n = 4) or RFS (n = 6). Twelve studies reported on BRAF mutations with a prevalence of BRAF mutation ranging from 0 to 9.1% in resected CRLM specimens. BRAF mutation was strongly associated with a worse prognosis. TP53 and PIK3CA gene mutations did not affect long-term outcomes.
The biological status of each tumor provides the basis for individualized cancer therapeutics. Data on the mutational status on CRLM should be a part of multidisciplinary discussions to help inform the therapeutic approach, type of chemotherapy, as well as timing and approach of surgical resection.
肝切除术被认为是治疗结直肠癌肝转移(CRLM)的最佳潜在治愈性方法。切除术后,高达三分之二的患者会在5年内复发。CRLM的基因突变分析,尤其是KRAS状态,已被提议作为指导治疗的一种手段,同时也用于识别能从肝切除术中获得最大生存益处的患者。
通过检索PubMed、Embase和Cochrane图书馆,对截至2018年2月8日的文献进行系统综述。应用以下检索策略:“(结直肠癌或直肠癌或结肠癌或结肠)AND(肝脏或肝)AND(转移或转移灶)AND(基因或突变或KRAS或BRAF或SMAD4或RAS或TP53或P53或APC或PI3K或MSI或EGFR或MACC1或微卫星)”。
从检索到的2404条记录中,最终确定78项研究符合要求;47项研究报告了可切除CRLM患者的突变数据,而31项研究报告了不可切除CRLM患者的情况。突变分析大多在CRLM标本而非原发性结直肠癌上进行。绝大多数研究报告了KRAS突变状态(88.5%,n = 69/78)。KRAS突变的发生率在25%至52%之间。大多数研究报告RAS突变是总生存期(OS)(n = 24)和无复发生存期(RFS)(n = 9)的不良预后因素;少数报告指出RAS突变状态对OS(n = 4)或RFS(n = 6)无影响。12项研究报告了BRAF突变,在切除的CRLM标本中BRAF突变的发生率为0至9.1%。BRAF突变与更差的预后密切相关。TP53和PIK3CA基因突变不影响长期预后。
每个肿瘤的生物学状态为个体化癌症治疗提供了依据。CRLM突变状态的数据应成为多学科讨论的一部分,以帮助确定治疗方法、化疗类型以及手术切除的时机和方式。
