Structural and Functional Characterization of EMF10, a Heterodimeric Disintegrin from Eristocophis macmahoni Venom That Selectively Inhibits α5β1 Integrin,

Abstract

α5β1, a major fibronectin receptor, is a widely distributed integrin that is essential for cell growth and organ development. Here, we describe a novel heterodimeric disintegrin named EMF10, isolated from the Eristocophis macmahoni venom, that is an extremely potent and selective inhibitor of α5β1. EMF10 inhibited adhesion of cells expressing α5β1 to fibronectin (IC₅₀ = 1−4 nM) and caused expression of a ligand-induced binding site (LIBS) on the β1 subunit of α5β1 integrin. It partially inhibited adhesion of cells expressing αIIbβ3, αvβ3, and α4β1 to appropriate ligands only at concentration higher than 500 nM. Guinea pig megakaryocytes expressing α5β1 adhered to immobilized EMF10 and showed extensive spreading and cytoskeletal mobilization. As determined by electrospray mass spectrometry, EMF10 is composed of two species with molecular masses of 14 575 and 14 949 Da, respectively. EMF10 is a heterodimer containing two subunits: EMF10A (M_r 7544 Da) and EMF10B (M_r 7405 and 7032 Da) linked covalently by S−S bonds. Subunit B showed heterogeneity and may be present as EMF10B1 (M_r 7032) and EMF10B2 (M_r 7405). In putative hairpin loops, EMF10A and EMF10B contained CKKGRGDNLNDYC and CWPAMGDWNDDYC motifs, respectively. The reduced and alkylated subunit B of EMF10 inhibited adhesion of K562 cells to fibronectin in a dose-dependent, saturable manner with IC₅₀ of 3 μM. The synthetic, cyclic CKKGRGDNLNDYC and CWPAMGDWNDDYC peptides expressed their inhibitory activity in the same system with IC₅₀ of 100 μM. We propose that α5β1 recognition of EMF10 is associated with the MGDW motif located in a putative hairpin loop of the B subunit and that the expression of activity may also depend on the RGDN motif in the subunit A and on the C-termini of both subunits.