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Hepsin activates pro-hepatocyte growth factor and is inhibited by hepatocyte growth factor activator inhibitor-1B (HAI-1B) and HAI-2 |
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| Authors: | Kirchhofer Daniel Peek Mark Lipari Michael T Billeci Karen Fan Bin Moran Paul |
| Institution: | Department of Physiology, Genentech, Inc., 1 DNA Way, South San Francisco, CA 94080, USA. dak@gne.com |
| Abstract: | Hepsin, a type II transmembrane serine protease, is highly upregulated in prostate cancer and promotes tumor progression and metastasis. We generated a soluble form of hepsin comprising the entire extracellular domain to show that it efficiently converts single-chain hepatocyte growth factor (pro-HGF) into biologically active two-chain HGF. Hepsin activity was potently inhibited by soluble forms of the bi-Kunitz domain inhibitors HAI-1B (IC(50) 21.1+/-2.7 nM) and HAI-2 (IC(50) 1.3+/-0.3 nM). Enzymatic assays with HAI-1B Kunitz domain mutants (R260A and K401A) further demonstrated that inhibition was due to Kunitz domain-1. The results suggest a functional link between hepsin and the HGF/Met pathway, which may contribute to tumor progression. |
| Keywords: | HGF hepatocyte growth factor HGFA HGF activator HAI-1 HAI-1B splice variants of HGFA inhibitor-1 HAI-2 HGFA inhibitor-2 KD1 and KD2 N- and C-terminal Kunitz domain of HAI-1B u-PA urokinase-type plasminogen activator t-PA tissue-type plasminogen activator TTSP type II transmembrane serine protease |
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