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首页> 外文期刊>Anticancer Research: International Journal of Cancer Research and Treatment >Oncoprotein coexpression in human aberrant crypt foci and minute polypoid lesions of the large bowel.
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Oncoprotein coexpression in human aberrant crypt foci and minute polypoid lesions of the large bowel.

机译:人异常隐窝灶和大肠微小息肉样病灶中的癌蛋白共表达。

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摘要

BACKGROUND: Genetic aberrations observed in the large bowel during the neoplastic progression have a cumulative effect and are responsible for the propagation of the multistep malignant process. In the present study we evaluated the immunoreactivity of c-fos, ras, bcl-2 and p53 in aberrant crypt foci (ACF) and minute polyps of the large bowel obtained from patients with colorectal cancer. METHODS: ACF and minute polyps were collected from macroscopically normal colonic mucosa. Protein immunoreactivity was detected on parafin sections utilizing the biotin-streptavidin method on 25 hyperplastic, 10 dysplastic ACF, 5 hyperplastic and 10 dysplastic adenomas. RESULTS: 41% of the lesions displayed positive ras immunoreactivity. bcl-2 immunoreactivity was positive in six minute polyps of which five were neoplastic. fos immunoreactivity was detected in five ACF and seven minute polyps, mainly in dysplastic lesions. Two neoplastic polyps were positive for p53 immunoreactivity. Coexpression of two or more oncoproteins was found with increasing frequency in dysplastic versus hyperplastic lesions and in polypoid lesions versus ACF. CONCLUSION: Abnormal expression and coexpression in oncoproteins can be identified in the earliest stages of colorectal tumorigenesis and may contribute to the progression of selected lesions during ACF-adenoma-carcinoma sequence.
机译:背景:在大肠癌变过程中观察到的遗传畸变具有累积效应,并负责多步恶性过程的传播。在本研究中,我们评估了结直肠癌患者大肠隐窝病灶(ACF)和微小息肉中c-fos,ras,bcl-2和p53的免疫反应性。方法:从宏观上正常的结肠粘膜收集ACF和微小息肉。使用生物素-链霉亲和素方法在25个增生性,10个增生性ACF,5个增生性和10个增生性腺瘤上检测石蜡切片上的蛋白免疫反应性。结果:41%的病灶显示ras免疫反应阳性。 6分钟息肉中bcl-2免疫反应阳性,其中5个为肿瘤性息肉。在五个ACF和七个分钟的息肉中检测到fos免疫反应性,主要在增生性病变中。两名肿瘤性息肉p53免疫反应阳性。在增生性病变与增生性病变以及息肉状病变与ACF中,发现两种或多种癌蛋白的共表达频率增加。结论:癌蛋白的表达和共表达可在大肠癌发生的最早阶段被鉴定出来,并可能有助于ACF-腺瘤-癌序列中某些病变的进展。

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