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上消化道癌患者异时性肿瘤中的TP53和RAS突变

TP53 and RAS mutations in metachronous tumors from patients with cancer of the upper aerodigestive tract.

作者信息

Yang H K, Linnoila R I, Conrad N K, Krasna M J, Aisner S C, Johnson B E, Kelley M J

机构信息

Navy Medical Oncology Branch, National Cancer Institute, Bethesda, MD 20889, USA.

出版信息

Int J Cancer. 1995 Aug 22;64(4):229-33. doi: 10.1002/ijc.2910640403.

Abstract

Patients who initially develop an upper aerodigestive tract cancer have an increased risk of second primary cancers. We examined TP53 and RAS mutations and p53 protein in 21 tumors from 10 patients with upper aerodigestive tract cancer who developed a metachronous tumor, to assess the genetic changes that occur in multiple primary tumors from the same individual. Thirteen of 21 (62%) tumors were found to have mis-sense mutations of either TP53 or RAS. Six tumors had TP53 mutations in codons 5 to 8 and 10 tumors from 7 patients had mutations of codons 12 or 13 of K-RAS. Only one patient had concordance of a mutation in 2 tumors; this mutation occurred in K-RAS and was accompanied by discordance of TP53 mutation. Three patients had tumors discordant for both TP53 and RAS mutations. Smoking-related tumors had TP53 and RAS mutations which were transversions in 11 (9 G:C to T:A and 2 G:C to C:G) and transitions in 3 (2 G:C to A:T and 1 A:T to G:C). Tumors not associated with smoking contained only transitions (both G:C to A:T). p53 protein was detected by immunohistochemistry in 7 of 13 (54%) tumors and was concordant in the multiple tumors of 3 patients. Three of the 7 tumors staining for p53 also had TP53 mutations. Thus, genetic alterations are discordant in multiple primary cancers and the pattern of mutations is similar to that found in patients with a single primary tumor, supporting the concept that these cancers arise independently.

摘要

最初患上上呼吸消化道癌症的患者发生第二原发性癌症的风险会增加。我们检测了10例患上异时性肿瘤的上呼吸消化道癌症患者的21个肿瘤中的TP53和RAS突变以及p53蛋白,以评估同一个体多个原发性肿瘤中发生的基因变化。21个肿瘤中有13个(62%)被发现存在TP53或RAS的错义突变。6个肿瘤在密码子5至8处有TP53突变,7例患者的10个肿瘤有K-RAS密码子12或13的突变。只有1例患者的2个肿瘤存在一致的突变;该突变发生在K-RAS,且伴有TP53突变不一致。3例患者的肿瘤在TP53和RAS突变方面均不一致。与吸烟相关的肿瘤中,TP53和RAS突变有11个是颠换(9个G:C到T:A和2个G:C到C:G),3个是转换(2个G:C到A:T和1个A:T到G:C)。与吸烟无关的肿瘤仅含转换(均为G:C到A:T)。通过免疫组织化学在13个肿瘤中的7个(54%)检测到p53蛋白,且在3例患者的多个肿瘤中是一致的。7个p53染色阳性的肿瘤中有3个也有TP53突变。因此,多个原发性癌症中的基因改变不一致,且突变模式与单一原发性肿瘤患者中发现的相似,支持这些癌症是独立发生的这一概念。

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