Abstract
Antithrombin is a key inhibitor of the coagulation cascade, but it may also function as an anti-inflammatory, anti-angiogenic, anti-viral and anti-apoptotic protein. Here, we report a novel function of antithrombin as a modulator of tumor cell migration and invasion. Antithrombin inhibited enteropeptidase on the membrane surface of HT-29, A549 and U-87 MG cells. The inhibitory process required the activation of antithrombin by heparin, and the reactive center loop and the heparin binding domain were essential. Surprisingly, antithrombin non-covalently inhibited enteropeptidase, revealing a novel mechanism of inhibition for this serpin. Moreover, as a consequence of this inhibition, antithrombin was cleaved, resulting in a molecule with anti-angiogenic properties that reduced vessel-like formation of endothelial cells. The addition of antithrombin and heparin to U-87 MG and A549 cells reduced motility in wound healing assays, inhibited the invasion in transwell assays and the degradation of a gelatin matrix mediated by invadopodia. These processes were controlled by enteropeptidase, as demonstrated by RNA interference experiments. Carcinoma cell xenografts in nude mice showed in vivo co-localization of enteropeptidase and antithrombin. Finally, treatment with heparin reduced experimental metastasis induced by HT29 cells in vivo. In conclusion, the inhibition of enteropeptidase by antithrombin may have a double anti-tumor effect through inhibiting a protease involved in metastasis and generating an anti-angiogenic molecule.
Highlights
– low molecular weight heparins (LMWH) AT AT +LMWH AT London +LMWH AT Toyama +LMWH of serine proteases known as type II transmembrane serine proteases (TTSPs) are among the enzymes deregulated during tumor growth and progression
Enteropeptidase is a serine protease that belongs to the type II transmembrane serine protease superfamily
It has been reported that the members of this superfamily are involved in the progression of some tumors[21,22,23], the physiological function of enteropeptidase is the conversion of zymogens into active proteases for food digestion[24]
Summary
– LMWH AT AT +LMWH AT London +LMWH AT Toyama +LMWH of serine proteases known as type II transmembrane serine proteases (TTSPs) are among the enzymes deregulated during tumor growth and progression. These TTSPs include TMPRSS2, corin, hepsin, enteropeptidase or TMPRSS15, matriptase, TMPRSS3, TMPRSS4, matriptase-2 and differentially expressed in squamous cell carcinoma gene 1 (DESC1)[11]. PCI does not inhibit enteropeptidase in vivo[12]. We characterized the antithrombin-mediated inhibition of enteropeptidase and investigated the effects of antithrombin on tumor cell migration, invasion and angiogenesis. We assessed the effect of heparin treatment in metastasis in an in vivo mouse model
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