Platelet activation and signal transduction by convulxin, a C-type lectin from Crotalus durissus terrificus (tropical rattlesnake) venom via the p62/GPVI collagen receptor

  • J Biol Chem. 1997 May 23;272(21):13576-83. doi: 10.1074/jbc.272.21.13576.
J Polgár  1 J M Clemetson B E Kehrel M Wiedemann E M Magnenat T N Wells K J Clemetson
Affiliations
  • 1. Theodor Kocher Institute, University of Berne, Freiestrasse 1, CH-3012 Berne, Switzerland.
Abstract

Convulxin, a powerful platelet activator, was isolated from Crotalus durissus terrificus venom, and 20 amino acid N-terminal sequences of both subunits were determined. These indicated that convulxin belongs to the heterodimeric C-type lectin family. Neither antibodies against GPIb nor echicetin had any effect on convulxin-induced platelet aggregation showing that, in contrast to Other venom C-type lectins acting on platelets, GPIb is not involved in convulxin-induced platelet activation. In addition, partially reduced/denatured convulxin only affects collagen-induced platelet aggregation. The mechanism of convulxin-induced platelet activation was examined by platelet aggregation, detection of time-dependent tyrosine phosphorylation of platelet proteins, and binding studies with 125I-convulxin. Convulxin induces signal transduction in part like Collagen, involving the time-dependent tyrosine phosphorylation of Fc receptor gamma chain, Phospholipase Cgamma2, p72(Syk), c-Cbl, and p36-38. However, unlike Collagen, pp125(FAK) and some Other bands are not tyrosine-phosphorylated. Convulxin binds to a glycosylated 62-kDa membrane component in platelet lysate and to p62/GPVI immunoprecipitated by human anti-p62/GPVI antibodies. Convulxin subunits inhibit both aggregation and tyrosine phosphorylation in response to Collagen. Piceatannol, a tyrosine kinase inhibitor with some specificity for p72(Syk), showed differential effects on Collagen and convulxin-stimulated signaling. These results suggest that convulxin uses the p62/GPVI but not the alpha2beta1 part of the Collagen signaling pathways to activate platelets. Occupation and clustering of p62/GPVI may activate Src family kinases phosphorylating Fc receptor gamma chain and, by a mechanism previously described in T- and B-cells, activate p72(Syk) that is critical for downstream activation of platelets.

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