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人肾细胞癌中尿激酶及尿激酶受体基因表达的调控

Modulation of urokinase and urokinase receptor gene expression in human renal cell carcinoma.

作者信息

Wagner S N, Atkinson M J, Thanner S, Wagner C, Schmitt M, Wilhelm O, Rotter M, Höfler H

机构信息

Institut für Pathologie, GSF-Forschungszentrum für Umwelt und Gesundheit, Oberschleissim, Germany.

出版信息

Am J Pathol. 1995 Jul;147(1):183-92.

Abstract

In vivo and in vitro experimental models have suggested a major role for the urokinase-type plasminogen activator (uPA) in tumor cell invasion and metastasis. The uPA proteolytic activity of tumor cells has been shown to be largely determined by the extent of the expression and saturation of the uPA receptor. We have analyzed the expression and cellular localization of both uPA and uPA receptor at the protein and mRNA levels in 33 paired samples of renal cell carcinoma (RCC) and non-tumorous kidney tissue. In comparison with adjacent normal non-tumorous kidney tissues RCC tumor cells modestly overexpressed uPA-receptor mRNA and showed significantly decreased uPA mRNA expression. However, the immunoreactive uPA content of tumor cells was comparable to that of the surrounding normal non-tumorous kidney tissue. Assuming constancy of the uPA-receptor affinity for uPA this indicates that a proportion of the RCC-associated uPA may be derived from an exogenous source and subsequently concentrated at the tumor cell surface via uPA receptor expression. The modest increase in uPA receptor expression may lead to a normalization of uPA antigen content in RCC; however, it is not sufficient to substantially increase tumor tissue-uPA content over the level of normal non-tumorous kidney tissue.

摘要

体内和体外实验模型表明,尿激酶型纤溶酶原激活剂(uPA)在肿瘤细胞侵袭和转移中起主要作用。肿瘤细胞的uPA蛋白水解活性已被证明很大程度上取决于uPA受体的表达程度和饱和度。我们在33对肾细胞癌(RCC)和非肿瘤性肾组织样本中,从蛋白质和mRNA水平分析了uPA和uPA受体的表达及细胞定位。与相邻的正常非肿瘤性肾组织相比,RCC肿瘤细胞适度过表达uPA受体mRNA,且uPA mRNA表达显著降低。然而,肿瘤细胞的免疫反应性uPA含量与周围正常非肿瘤性肾组织相当。假设uPA受体对uPA的亲和力恒定,这表明一部分与RCC相关的uPA可能来源于外源性,随后通过uPA受体表达集中在肿瘤细胞表面。uPA受体表达的适度增加可能导致RCC中uPA抗原含量正常化;然而,这不足以使肿瘤组织中的uPA含量大幅超过正常非肿瘤性肾组织的水平。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/234d/1869882/ad1c478eb94a/amjpathol00043-0192-a.jpg

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