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p53蛋白在胃腺瘤和癌中的过度表达。

Over-expression of p53 protein in gastric adenoma and cancer.

作者信息

Yonemura Y, Fushida S, Fonseca L, Tsugawa K, Ninomiya I, Yamaguchi A, Miyazaki I

出版信息

Int J Oncol. 1993 Sep;3(3):497-501.

Abstract

Recently, alterations of p53 gene in gastric cancer have been reported by several authors, but the role of p53-gene alterations in early step of carcinogenesis of gastric cancer remains unclear. To assess whether p53 expression is an early event in the carcinogenesis of gastric cancer, 402 gastric tumors (14 hyperplastic polyps, 48 gastric adenomas, 340 gastric cancers) were analyzed by immunohistochemistry using the specific antibody, PAb1801, against p53 oncoprotein. Five (15%) of 34 adenomas and 110 (32%) of 340 gastric cancers showed a definite positive nuclear staning for p53 protein. In contrast, the anti-p53 MAb did not show any specific staining in normal gastric epithelial cells, intestinal metaplasia or hyperplastic polyps. Out of nine adenomas showing mild dysplasia, only one tumor (11%) showed p53 expression. In contrast, 4 (16%) of 25 adenomas showing moderate dysplasia revealed positive p53 expression. In addition, positive p53 staining was not found in adenomas less than 1 cm in diameter, but five (25%) of 20 adenomas 1 cm or more in diameter showed definite p53-staining. In this way, the positive-p53 tissue status in adenomas was correlated with the dysplastic grade and size of adenomas. The incidence of positive-p53 immunoreaction in the differentiated type of cancers was 35% and showed no relation to wall invasion. On the contrary, p53 expression in the undifferentiated type of m-cancers, in which tumor invasion was limited to the mucosal layers, was detected in only one (5%) of 21 cases. Among undifferentiated type of gastric cancer, however, deeply invasive cancers showed higher p53-positive rate, as compared with m-cancer. These results may suggest p53 gene activation at a relatively early stage of the adenoma-carcinoma sequence, leading to the development of some differentiated adenocarcinomas in the stomach.

摘要

最近,几位作者报道了胃癌中p53基因的改变,但p53基因改变在胃癌癌变早期阶段中的作用仍不清楚。为了评估p53表达是否为胃癌癌变过程中的早期事件,我们使用针对p53癌蛋白的特异性抗体PAb1801,通过免疫组织化学分析了402例胃肿瘤(14例增生性息肉、48例胃腺瘤、340例胃癌)。34例腺瘤中有5例(15%)以及340例胃癌中有110例(32%)显示p53蛋白有明确的阳性核染色。相比之下,抗p53单克隆抗体在正常胃上皮细胞、肠化生或增生性息肉中未显示任何特异性染色。在9例显示轻度发育异常的腺瘤中,只有1例肿瘤(11%)显示p53表达。相比之下,25例显示中度发育异常的腺瘤中有4例(16%)显示p53表达呈阳性。此外,直径小于1 cm的腺瘤中未发现p53染色阳性,但直径1 cm或更大的20例腺瘤中有5例(25%)显示明确的p53染色。这样,腺瘤中p53阳性组织状态与腺瘤的发育异常程度和大小相关。分化型癌中p53免疫反应阳性的发生率为35%,且与壁浸润无关。相反,在肿瘤浸润仅限于黏膜层的未分化型微小癌中,21例中仅1例(5%)检测到p53表达。然而,在未分化型胃癌中,与微小癌相比,深部浸润癌显示出更高的p53阳性率。这些结果可能提示在腺瘤 - 癌序列的相对早期阶段p53基因被激活,从而导致胃内一些分化型腺癌的发生。

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