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胰蛋白酶-2与基质金属蛋白酶-9的细胞内共定位:胰蛋白酶-2、基质金属蛋白酶-9和肠激酶在癌中的可能蛋白水解级联反应

Intracellular co-localization of trypsin-2 and matrix metalloprotease-9: possible proteolytic cascade of trypsin-2, MMP-9 and enterokinase in carcinoma.

作者信息

Vilen Suvi-Tuuli, Nyberg Pia, Hukkanen Mika, Sutinen Meeri, Ylipalosaari Merja, Bjartell Anders, Paju Annukka, Haaparanta Virpi, Stenman Ulf-Håkan, Sorsa Timo, Salo Tuula

机构信息

Institute of Dentistry, University of Helsinki, Department of Oral and Maxillofacial Diseases, Helsinki University Hospital, Finland.

出版信息

Exp Cell Res. 2008 Feb 15;314(4):914-26. doi: 10.1016/j.yexcr.2007.10.025. Epub 2007 Nov 12.

DOI:10.1016/j.yexcr.2007.10.025
PMID:18062964
Abstract

Tumor-associated trypsin-2 and matrix metalloprotease-9 (MMP-9) are associated with cancer, particularly with invasive squamous cell carcinomas. They require activation for catalytical competence via proteolytic cascades. One cascade is formed by enterokinase, trypsin-2 and MMP-9; enterokinase activates trypsinogen-2 to trypsin-2, which is an efficient proMMP-9 activator. We describe here that oral squamous cell carcinomas express all members of this cascade: MMP-9, trypsin-2 and enterokinase. The expression of enterokinase in a carcinoma cell line not derived from the duodenum was shown here for the first time. Enterokinase directly cleaved proMMP-9 at the Lys65-Ser66 site, but failed to activate it in vitro. We demonstrated by confocal microscopy that MMP-9 and trypsin-2 co-localized in intracellular vesicles of the carcinoma cells. This co-localization of trypsin-2 and MMP-9 resulted in intracellular proMMP-9 processing that represented fully or partially activated MMP-9. However, although both proteases were present also in various bone tumor tissues, MMP-9 and trypsin-2 never co-localized at the cellular level in these tissues. This suggests that the intracellular vesicular co-localization, storage and possible activation of these proteases may be a unique feature for aggressive epithelial tumors, such as squamous cell carcinomas, but not for tumors of mesenchymal origin.

摘要

肿瘤相关胰蛋白酶-2和基质金属蛋白酶-9(MMP-9)与癌症相关,尤其是与浸润性鳞状细胞癌有关。它们需要通过蛋白水解级联反应激活才能具备催化活性。其中一个级联反应由肠激酶、胰蛋白酶-2和MMP-9组成;肠激酶将胰蛋白酶原-2激活为胰蛋白酶-2,而胰蛋白酶-2是一种有效的MMP-9前体激活剂。我们在此描述,口腔鳞状细胞癌表达该级联反应的所有成员:MMP-9、胰蛋白酶-2和肠激酶。本文首次展示了肠激酶在非十二指肠来源的癌细胞系中的表达。肠激酶在Lys65-Ser66位点直接切割MMP-9前体,但在体外未能激活它。我们通过共聚焦显微镜证明,MMP-9和胰蛋白酶-2在癌细胞的细胞内囊泡中共定位。胰蛋白酶-2和MMP-9的这种共定位导致细胞内MMP-9前体加工,产生完全或部分激活的MMP-9。然而,尽管这两种蛋白酶也存在于各种骨肿瘤组织中,但在这些组织中MMP-9和胰蛋白酶-2在细胞水平上从未共定位。这表明这些蛋白酶在细胞内囊泡中的共定位、储存和可能的激活可能是侵袭性上皮肿瘤(如鳞状细胞癌)的独特特征,而不是间充质起源肿瘤的特征。

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