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人膀胱尿路上皮癌中膜型1、2和3基质金属蛋白酶的表达及组织定位

Expression and tissue localization of membrane-types 1, 2, and 3 matrix metalloproteinases in human urothelial carcinomas.

作者信息

Kitagawa Y, Kunimi K, Ito H, Sato H, Uchibayashi T, Okada Y, Seiki M, Namiki M

机构信息

Department of Urology, Kanazawa University School of Medicine, Japan.

出版信息

J Urol. 1998 Oct;160(4):1540-5.

PMID:9751409
Abstract

PURPOSE

Three different membrane-type matrix metalloproteinases (MT1, 2, 3-MMP) which can activate proMMP-2 (progelatinase A) are thought to have an important role in various human carcinoma invasions and metastases. We examined the mRNA expression of MT-MMPs and the tissue immunolocalization of MT1-MMP in human urothelial carcinomas.

MATERIALS AND METHODS

mRNA was extracted from 27 clinical urothelial carcinomas and 10 normal urothelial mucosa tissues remote from the tumor. RT-PCR using specific primers was performed, and PCR products were hybridized to 32P-labeled internal probes and analyzed by a bioimage analyzer. Immunolocalization was studied using a monoclonal antibody against MT1-MMP (114-6G6).

RESULTS

MT1-MMP and MT2-MMP mRNA expressions in urothelial carcinomas were significantly higher than those in the normal mucosa. In contrast, MT3-MMP mRNA was little expressed in both tissues, and the amount of MT3-MMP mRNA appeared to be much lower than MT1-MMP and MT2-MMP in the tissue samples. In terms of the tumor multiplicity, MT1-MMP and MT2-MMP mRNA expressions in the group of multiple tumors were significantly higher than those in the solitary tumor group. The carcinoma cells were immunostained for MT1-MMP predominantly in invasive and superficial carcinoma cells. The immunoreactivity was more intense in the invasive type than in the superficial type.

CONCLUSIONS

It is suggested that MT1-MMP and MT2-MMP play an important role in the development of human urothelial carcinomas and reflect some aspects of the pathogenesis of multifocal occurrence. In spite of the possible contribution to the invasive and metastatic phenotype, MT1-MMP mRNA and its product are thought to be expressed already in the clinical superficial stage in some cases of this tumor type.

摘要

目的

三种不同的膜型基质金属蛋白酶(MT1、2、3 - MMP)可激活前MMP - 2(前明胶酶A),被认为在多种人类癌侵袭和转移中起重要作用。我们检测了人尿路上皮癌中MT - MMPs的mRNA表达及MT1 - MMP的组织免疫定位。

材料与方法

从27例临床尿路上皮癌及远离肿瘤的10例正常尿路上皮黏膜组织中提取mRNA。使用特异性引物进行逆转录聚合酶链反应(RT - PCR),PCR产物与32P标记的内部探针杂交,并用生物图像分析仪进行分析。使用抗MT1 - MMP的单克隆抗体(114 - 6G6)研究免疫定位。

结果

尿路上皮癌中MT1 - MMP和MT2 - MMP的mRNA表达显著高于正常黏膜。相反,MT3 - MMP mRNA在两种组织中均很少表达,且在组织样本中MT3 - MMP mRNA的量似乎远低于MT1 - MMP和MT2 - MMP。就肿瘤多灶性而言,多灶性肿瘤组中MT1 - MMP和MT2 - MMP的mRNA表达显著高于单灶性肿瘤组。癌细胞主要在浸润性和浅表癌细胞中对MT1 - MMP进行免疫染色。浸润型的免疫反应性比浅表型更强。

结论

提示MT1 - MMP和MT2 - MMP在人尿路上皮癌的发生发展中起重要作用,并反映了多灶性发生的发病机制的某些方面。尽管可能对侵袭性和转移表型有贡献,但在该肿瘤类型的某些病例中,MT1 - MMP mRNA及其产物被认为在临床浅表阶段就已表达。

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