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原发性结肠癌中 K-ras 突变的异质性分布:对 EGFR 靶向治疗的影响。

Heterogeneous distribution of K-ras mutations in primary colon carcinomas: implications for EGFR-directed therapy.

机构信息

Laboratory for Molecular Biology, Stavanger University Hospital, PO Box 8100, 4068, Stavanger, Norway.

出版信息

Int J Colorectal Dis. 2011 Oct;26(10):1271-7. doi: 10.1007/s00384-011-1233-5. Epub 2011 May 15.

DOI:10.1007/s00384-011-1233-5
PMID:21573767
Abstract

PURPOSE

K-ras mutations predict resistance against epidermal growth factor receptor (EGFR)-directed therapy of metastatic colorectal cancer (CRC). The purpose of this study was to analyze the distribution of K-ras mutations in primary tumors and corresponding sentinel lymph nodes (SLNs) from colon cancer patients.

METHODS

Tumor biopsies and SLNs from 158 patients with non-metastatic colon cancer were analyzed for K-ras mutations in codons 12 and 13 by a sensitive and quantitative peptide nucleic acid clamp PCR assay.

RESULTS

Analyses of single fresh-frozen tumor biopsies revealed K-ras mutations in 67 (42%) of the patients. Apparently low levels of K-ras mutations in 13 of the mutated primary tumors and the presence of K-ras mutations in SLNs from seven patients with a wild-type primary tumor biopsy suggested possible intratumoral heterogeneity for 20 of the patients. To confirm this hypothesis, we analyzed tissue sections from all available formalin-fixed, paraffin-embedded (FFPE) tumor blocks from these 20 patients. Ten of the patients had a mixture of tissue sections positive and tissue sections negative for K-ras mutations, two patients had K-ras mutations in all sections, and eight patients had no detectable K-ras mutations in tumor FFPE tissue blocks. Among these eight patients, five had K-ras mutations detected in SLNs. Thus, evidence supporting a heterogeneous distribution of K-ras mutations was obtained for 15 patients.

CONCLUSIONS

Heterogeneous distribution of K-ras codon 12 and 13 mutations within primary tumor, or between primary tumor and lymph node metastases, was demonstrated for 15 (20%) of 74 colon cancer patients having K-ras mutations. This may have implications for tissue sampling routines with regard to EGFR-directed therapy of CRC, both in adjuvant and metastatic settings.

摘要

目的

K-ras 突变预测转移性结直肠癌(CRC)对表皮生长因子受体(EGFR)靶向治疗的耐药性。本研究的目的是分析结肠癌患者原发肿瘤和相应前哨淋巴结(SLN)中 K-ras 突变的分布。

方法

采用敏感定量肽核酸夹PCR 法检测 158 例非转移性结肠癌患者肿瘤活检和 SLN 中 K-ras 密码子 12 和 13 的突变。

结果

分析单个新鲜冷冻肿瘤活检显示,67 例(42%)患者存在 K-ras 突变。13 例突变原发肿瘤中明显低水平的 K-ras 突变和 7 例野生型原发肿瘤活检 SLN 中存在 K-ras 突变提示 20 例患者可能存在肿瘤内异质性。为了证实这一假设,我们分析了这 20 例患者所有可用的福尔马林固定、石蜡包埋(FFPE)肿瘤块的组织切片。10 例患者的组织切片 K-ras 突变阳性和组织切片 K-ras 突变阴性混合存在,2 例患者所有切片均存在 K-ras 突变,8 例患者在肿瘤 FFPE 组织块中未检测到 K-ras 突变。这 8 例患者中有 5 例在 SLN 中检测到 K-ras 突变。因此,有 15 例患者获得了支持 K-ras 突变异质性分布的证据。

结论

在 74 例存在 K-ras 密码子 12 和 13 突变的结肠癌患者中,15 例(20%)患者的原发肿瘤内或原发肿瘤与淋巴结转移之间存在 K-ras 突变的异质性分布。这可能对 CRC 的 EGFR 靶向治疗的组织取样常规产生影响,无论是在辅助治疗还是转移性治疗中。

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