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人异常隐窝病灶中细胞黏附蛋白和异常糖蛋白的表达

Expression of cellular adhesion proteins and abnormal glycoproteins in human aberrant crypt foci.

作者信息

Wargovich Michael J, Chang Phyllis, Velasco Marco, Sinicrope Frank, Eisenbrodt Edward, Sellin Joseph

机构信息

Division of Basic Research, South Carolina Cancer Center, University of South Carolina School of Medicine, Columbia, SC, USA.

出版信息

Appl Immunohistochem Mol Morphol. 2004 Dec;12(4):350-5. doi: 10.1097/00129039-200412000-00011.

Abstract

Aberrant crypt foci (ACFs) may be the earliest recognizable histologic precursor lesion for colon cancer. ACF may develop from a complex of events, including the development of cryptal hyperproliferation, defects in the rate of apoptosis, and abnormalities in cellular adhesion. In this study, we hypothesized that human ACF would exhibit discrete differences in cell adhesion proteins compared with normal mucosa of biologic markers associated with colon cancer. ACFs were isolated from resected colon mucosa from 45 patients undergoing surgery for colon cancer. We evaluated the protein expression of 3 biologic markers that may be related to the progression of aberrant crypt foci to tumors: carcinoembryonic antigen, E-cadherin, and sialyl Tn antigen. In general, ACFs located near cancers in the right colon were more often hyperplastic than dysplastic; this was more noticeable in the left colon. Carcinoembryonic antigen expression was found to be more intense in apical portions of ACF crypts, with sialyl Tn antigen moderately increased, whereas E-cadherin diffusely stained throughout crypts within ACFs. There are significant biologic changes in potential tumor markers that accompany the early transformation of the normal glandular epithelium, some of which are expressed very early in the colon at the stage of appearance of ACF.

摘要

异常隐窝灶(ACFs)可能是结肠癌最早可识别的组织学前驱病变。ACF可能由一系列复杂事件发展而来,包括隐窝过度增殖、凋亡率缺陷以及细胞黏附异常。在本研究中,我们假设与结肠癌相关的生物标志物相比,人类ACF在细胞黏附蛋白方面会表现出明显差异。从45例接受结肠癌手术的患者切除的结肠黏膜中分离出ACFs。我们评估了3种可能与异常隐窝灶进展为肿瘤相关的生物标志物的蛋白表达:癌胚抗原、E-钙黏蛋白和唾液酸化Tn抗原。一般来说,右半结肠靠近癌灶的ACFs增生性多于发育异常性;在左半结肠这种情况更明显。发现癌胚抗原在ACF隐窝顶部表达更强烈,唾液酸化Tn抗原中度增加,而E-钙黏蛋白在ACFs内的隐窝中呈弥漫性染色。在正常腺上皮早期转化过程中,潜在肿瘤标志物存在显著的生物学变化,其中一些在结肠ACF出现阶段就很早表达。

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