Authors
Hirokazu Nakahara, Linda Howard, Erik W Thompson, Hiroshi Sato, Motoharu Seiki, Yunyun Yeh, Wen-Tien Chen
Publication date
1997/7/22
Journal
Proceedings of the National Academy of Sciences
Volume
94
Issue
15
Pages
7959-7964
Publisher
The National Academy of Sciences of the USA
Description
The invasion of human malignant melanoma cells into the extracellular matrix (ECM) involves the accumulation of proteases at sites of ECM degradation where activation of matrix metalloproteases (MMP) occurs. Here, we show that when membrane type 1 MMP (MT-MMP) was overexpressed in RPMI7951 human melanoma cells, the cells made contact with the ECM, activated soluble and ECM-bound MMP-2, and degraded and invaded the ECM. Further experiments demonstrated the importance of localization of the MT-MMP to invadopodia. Overexpression of MT-MMP without invadopodial localization caused activation of soluble MMP-2, but did not facilitate ECM degradation or cell invasiveness. Up-regulation of endogenous MT-MMP with concanavalin A caused activation of MMP-2. However, concanavalin A treatment prevented invadopodial localization of MT-MMP and ECM degradation. Neither a truncated …
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