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中国河南高危人群早期食管前病变和癌组织中p53抑癌基因突变情况

p53 tumor suppressor gene mutation in early esophageal precancerous lesions and carcinoma among high-risk populations in Henan, China.

作者信息

Gao H, Wang L D, Zhou Q, Hong J Y, Huang T Y, Yang C S

机构信息

Laboratory for Cancer Research, College of Pharmacy, Rutgers University, Piscataway, New Jersey 08855.

出版信息

Cancer Res. 1994 Aug 15;54(16):4342-6.

PMID:8044781
Abstract

To understand whether p53 gene mutation is an early or late event in esophageal carcinogenesis, biopsy samples of esophageal epithelium from symptom-free subjects in a high incidence area, Huixian county of Henan Province, China, were analyzed. Mutations in exons 5, 6, 7, and 8 of p53 were analyzed by single-strand conformation polymorphism analysis and DNA sequencing. Among the 37 biopsy samples showing accumulation of p53 protein in immunohistochemical staining, missense mutations of p53 gene were detected in 1 of 3 samples with normal epithelia, 3 of 23 samples with basal cell hyperplasia, and 4 of 11 samples with dysplasia. All mutations occurred at exon 5 with 3 at codon 175, 2 at codon 176, and 1 each at codons 159, 135, and codon 132. Of the 8 mutations, there were 3 G to A transitions and 3 G to T transversions. To understand the mutation spectrum and possible causative factors of esophageal cancer in this area, surgically resected human primary esophageal carcinomas from Linxian county were analyzed for p53 gene mutations in exons 5, 6, 7, and 8. Mutations were detected in 16 of 29 samples (55%). Twelve samples contained different missense point mutations, with 75% transitions (7 G to A and 2 A to G) and 25% transversions (2 G to T and 1 G to C). Most of the mutations were located at either exon 5 or exon 7. A deletion and an insertion of nucleotides leading to frame-shift mutations were detected in each of two other samples. The results demonstrate that p53 protein accumulation and gene mutation may occur at very early stages of esophageal carcinogenesis. In carcinomas, there was a higher frequency of p53 gene mutations, which accounts for most of the cases with p53 protein accumulation.

摘要

为了解p53基因突变是食管癌发生过程中的早期还是晚期事件,我们分析了中国河南省辉县(食管癌高发区)无症状受试者的食管上皮活检样本。通过单链构象多态性分析和DNA测序分析p53基因第5、6、7和8外显子的突变情况。在免疫组织化学染色显示p53蛋白积累的37个活检样本中,正常上皮的3个样本中有1个检测到p53基因错义突变,基底细胞增生的23个样本中有3个,发育异常的11个样本中有4个。所有突变均发生在第5外显子,密码子175处有3个突变,密码子176处有2个突变,密码子159、135和132处各有1个突变。在这8个突变中,有3个G到A的转换和3个G到T的颠换。为了解该地区食管癌的突变谱和可能的致病因素,我们分析了林县手术切除的人原发性食管癌第5、6、7和8外显子的p53基因突变情况。29个样本中有16个(55%)检测到突变。12个样本含有不同的错义点突变,75%为转换(7个G到A和2个A到G),25%为颠换(2个G到T和1个G到C)。大多数突变位于第5外显子或第7外显子。另外两个样本中分别检测到导致移码突变的核苷酸缺失和插入。结果表明,p53蛋白积累和基因突变可能发生在食管癌发生的非常早期阶段。在癌组织中,p53基因突变频率较高,这是大多数p53蛋白积累病例的原因。

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