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体细胞突变筛查:利用血浆DNA鉴定携带K-ras突变的个体。

Somatic mutation screening: identification of individuals harboring K-ras mutations with the use of plasma DNA.

作者信息

Kopreski M S, Benko F A, Borys D J, Khan A, McGarrity T J, Gocke C D

机构信息

M. S. Kopreski, OncoMEDx, Inc., Columbia, MD, USA.

出版信息

J Natl Cancer Inst. 2000 Jun 7;92(11):918-23. doi: 10.1093/jnci/92.11.918.

DOI:10.1093/jnci/92.11.918
PMID:10841827
Abstract

BACKGROUND

Many cancers are attributed to somatic mutation of DNA. We investigated whether it is feasible to detect cancer-associated somatic mutations in patients with neoplasms by using plasma DNA.

METHODS

Plasma samples were prospectively collected from 240 patients undergoing colonoscopy. Colorectal biopsies were performed as clinically indicated in 135 patients, and risk factor information was available from 232 patients. DNA was extracted from plasma and colorectal tissue and was amplified by use of a polymerase chain reaction method that enriches for mutations in codon 12 of the K-ras oncogene. Molecular, histologic, and clinical data were compared by use of two-sided Fisher's exact test.

RESULTS

Mutations in the K-ras gene detected in the plasma of 64 (28%) of 232 patients were statistically significantly associated with colorectal cancer risk factors (P =.0002). Of those patients having tissue available for comparison (n = 135), mutations in the K-ras gene were found in the tissues of 35 patients, and 29 (83%) of these 35 showed mutations in plasma samples. In contrast, the plasma assay was negative in 93 of the 100 patients whose tissue K-ras was wild-type. Among patients without biopsies (n = 105), 28 had mutated K-ras in their plasma DNA, despite the absence of remarkable colonoscopy findings; 24 of these 28 patients had risk factors for colorectal cancer. Overall, 25 (39%) of 64 patients showing mutations in plasma DNA had colorectal neoplasms with K-ras mutations compared with five (3%) of 176 patients without K-ras mutations in plasma DNA.

CONCLUSION

Plasma DNA assays for the detection of mutations in K-ras codon 12 may provide a feasible method to screen populations for somatic mutations frequently found in neoplasms. The clinical utility of using this test in screening populations requires further study.

摘要

背景

许多癌症归因于DNA的体细胞突变。我们研究了通过使用血浆DNA检测肿瘤患者中与癌症相关的体细胞突变是否可行。

方法

前瞻性收集了240例接受结肠镜检查患者的血浆样本。135例患者根据临床指征进行了结肠活检,232例患者可获得危险因素信息。从血浆和结肠组织中提取DNA,并使用聚合酶链反应方法进行扩增,该方法可富集K-ras癌基因第12密码子的突变。使用双侧Fisher精确检验比较分子、组织学和临床数据。

结果

在232例患者中的64例(28%)血浆中检测到的K-ras基因突变与结直肠癌危险因素在统计学上显著相关(P = 0.0002)。在有组织可供比较的患者(n = 135)中,3

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