Matrilysin (MMP-7) induces homotypic adhesion of human colon cancer cells and enhances their metastatic potential in nude mouse model

被引:0
|
作者
Mitomu Kioi
Kazuhiro Yamamoto
Shouichi Higashi
Naohiko Koshikawa
Kiyohide Fujita
Kaoru Miyazaki
机构
[1] Kihara Institute for Biological Research,Division of Cell Biology
[2] Yokohama City University,Department of Oral Maxillofacial Surgery
[3] 641-12,undefined
[4] Maioka-cho,undefined
[5] Totsuka-ku,undefined
[6] Yokohama City University School of Medicine,undefined
[7] 3-9,undefined
[8] Fukuura,undefined
[9] Kanazawa-ku,undefined
来源
Oncogene | 2003年 / 22卷
关键词
matrilysin; matrix metalloproteinases; metastasis; colon carcinoma; E-cadherin;
D O I
暂无
中图分类号
学科分类号
摘要
Matrilysin (MMP-7) is thought to contribute to invasive growth and metastasis of colon carcinoma and many other human cancers. The present study demonstrates that treatment of human colon carcinoma cells with active matrilysin induces cell aggregation in vitro and promotes liver metastasis in nude mice. When two kinds of colon carcinoma cell lines were incubated with active matrilysin, this enzyme efficiently bound to the cell surface and induced loose cell aggregation, which led to E-cadherin-mediated tight cell aggregation. Synthetic MMP inhibitors inhibited both the membrane binding of matrilysin and matrilysin-induced cell aggregation, while TIMP-2 inhibited only the cell aggregation. Two other active MMPs, stromelysin and gelatinase A, neither bound to cell membrane nor induced cell aggregation. Tumor cells in loose cell aggregates could reaggregate even after they were freed from matrilysin and dispersed. When injected into the spleen of nude mice, the tumor cells in the stable aggregates produced much larger metastatic nodules in the livers than control cells and those in the loose aggregates. These results suggest that matrilysin may enhance metastatic potential of tumor cells by processing a cell surface protein(s) and thereby inducing loose and then tight aggregation of tumor cells.
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页码:8662 / 8670
页数:8
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