The peptide LSARLAF causes platelet secretion and aggregation by directly activating the integrin αIIbβ3

Abstract

A novel peptide (designed to bind to α_IIbβ₃) caused platelet aggregation and aggregation-independent secretion of the contents of α-granules in an α_IIbβ₃-dependent fashion. The agonist peptide induced secretion in the presence of prostaglandin E₁. In cell-free assays, α_IIbβ₃ bound specifically to immobilized agonist peptide and the peptide enhanced the binding of fibrinogen to immobilized α_IIbβ₃. The agonist peptide apparently activates α_IIbβ₃ by directly inducing a conformational change in the receptor. This change activates the platelets and causes secretion in a manner independent of fibrinogen binding.