Inhibition of Calpain Blocks Platelet Secretion, Aggregation, and Spreading

Previous studies have indicated that the Ca 2+ -dependent protease, calpain, is activated in platelets within 30–60 s of thrombin stimulation, but specific roles of calpain in platelets remain to be identified. To directly test the functions of calpain during platelet activation, a novel strategy...

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Bibliographic Details
Published in:The Journal of biological chemistry 1999-12, Vol.274 (51), p.36321-36327
Main Authors: Croce, K, Flaumenhaft, R, Rivers, M, Furie, B, Furie, B C, Herman, I M, Potter, D A
Format: Article
Language:English
Subjects:
Amino Acid Sequence
Blood Platelets - cytology
Blood Platelets - physiology
Calcium-Binding Proteins
Calpain - physiology
Humans
Molecular Sequence Data
Mutation
Peptide Fragments
Platelet Adhesiveness - physiology
Platelet Aggregation
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Summary:Previous studies have indicated that the Ca 2+ -dependent protease, calpain, is activated in platelets within 30–60 s of thrombin stimulation, but specific roles of calpain in platelets remain to be identified. To directly test the functions of calpain during platelet activation, a novel strategy was developed for introducing calpain's specific biological inhibitor, calpastatin, into platelets prior to activation. This method involves treatment of platelets with a fusion peptide, calpastat, consisting of the cell-penetrating signal sequence from Kaposi's fibroblast growth factor connected to a calpain-inhibiting consensus sequence derived from calpastatin. Calpastat specifically inhibits thrombin peptide (SFLLR)-induced α-granule secretion (IC 50 = 20 μ m ) during the first 30 s of activation, thrombin-induced platelet aggregation (IC 50 = 50 μ m ), and platelet spreading on glass surfaces (IC 50 = 34 μ m ). Calpastat-Ala, a mutant peptide in which alanine is substituted at conserved calpastatin residues, lacks calpain inhibitory activity and fails to inhibit secretion, aggregation, or spreading. The peptidyl calpain inhibitors calpeptin, MDL 28,170 (MDL) and E64d also inhibit secretion, aggregation and spreading, but require 3–10-fold higher concentrations than calpastat for biological activity. Together, these findings demonstrate that calpain regulates platelet secretion, aggregation, and spreading and indicate that calpain plays an earlier role in platelet activation following thrombin receptor stimulation than had been previously detected.
ISSN:0021-9258
1083-351X
DOI:10.1074/jbc.274.51.36321