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人类早期结直肠癌中形态学与血管生成之间的相互作用。

Interaction between morphology and angiogenesis in human early colorectal cancers.

作者信息

Okada Keiichiro, Satoh Toshimi, Fujimoto Kazuma, Tokunaga Osamu

机构信息

Department of Pathology and Biodefense, Saga Medical School, Saga, Japan.

出版信息

Pathol Int. 2004 Jul;54(7):490-7. doi: 10.1111/j.1440-1827.2004.01650.x.

Abstract

Morphologically, early colorectal cancers are divided into two types: polypoid cancers and non-polypoid cancers. They vary in growth pattern, progression, and genetic alteration. Angiogenesis between polypoid and non-polypoid cancers may also be different. Therefore, the present study aims to evaluate angiogenesis in the early stages of colorectal malignancy, with particular attention to the morphological differences. The serial slides of all materials (48 polypoid cancers, 10 non-polypoid cancers, 20 adenomas and 10 normal tissues) were immunohistochemically stained for three endothelial cell markers (CD31, von Willebrand factor and CD105), counted for the number of microvessels in the same hot spots, and the angiogenic status was estimated. Polypoid cancers had higher microvessel counts and were more predominantly supplied by activated (CD105-positive, newly forming) microvessels than non-polypoid cancers. The present study indicated the possibility that the difference in growth pattern might be explained by the difference in angiogenesis between polypoid and non-polypoid cancers.

摘要

从形态学上看,早期结直肠癌分为两种类型:息肉样癌和非息肉样癌。它们在生长模式、进展和基因改变方面存在差异。息肉样癌和非息肉样癌之间的血管生成情况也可能不同。因此,本研究旨在评估结直肠恶性肿瘤早期的血管生成情况,特别关注形态学差异。对所有材料(48例息肉样癌、10例非息肉样癌、20例腺瘤和10例正常组织)的连续切片进行免疫组织化学染色,检测三种内皮细胞标志物(CD31、血管性血友病因子和CD105),计数相同热点区域的微血管数量,并评估血管生成状态。与非息肉样癌相比,息肉样癌的微血管计数更高,且主要由活化的(CD105阳性,新形成的)微血管供血。本研究表明,息肉样癌和非息肉样癌之间血管生成的差异可能解释了它们生长模式的不同。

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