Fibrinogen and fibrin polymerization: appraisal of the binding events that accompany fibrin generation and fibrin clot assembly.

Blood Coagul Fibrinolysis

University of Wisconsin Medical School, Milwaukee Clinical Campus, Sinai Samaritan Medical Center, 53233, USA.

Published: July 1997

Fibrinogen is a complex multifunctional protein comprised of three major domains (two outer D and one central E) which contains constitutive binding sites (e.g. Da, Db, gammaXL, D:D, gamma', thrombin substrate, platelet receptor) as well as binding sites that become exposed or expressed as a result of fibrinogen proteolysis by thrombin and/or that are exposed as a consequence of the polymerization process itself (tPA binding sites). Fibrin-dependent tPA-mediated activation of plasminogen is associated with exposure of polymerization-dependent epitopes (Aalpha148-160, gamma312-324) that are expressed in assembled fibrin and in crosslinked (polymerized) fibrinogen but not in unpolymerized fibrinogen or fibrin. Fibrin polymerization is initiated by thrombin cleavage of fibrinopeptide A from fibrinogen Aalpha chains, exposing two E domain E(A) sites. Cleavage of fibrinopeptide B from fibrinogen Bbeta chains exposes other E domain polymerization sites, termed E(B), that also interact with platelets, fibroblasts and endothelial cells. Fibrin generation is followed by an assembly process of intermolecular end-to-middle D to E associations to form linear and branched double-stranded fibrin fibrils, lateral fibril-fibril associations to form fibers and a branched fiber network. Binding sites in fibrinogen play their roles in fibrin assembly by self-association (gammaXL to gammaXL and D:D to D:D) or by complementary association with exposed sites in fibrin (Da to E(A) and Db to E[B]). Other binding sites in fibrinogen include thrombin substrate recognition sites in each E domain and a non-substrate high affinity thrombin binding site in the carboxy-terminal region of each gamma' chain, which also binds plasma factor XIII. Fibrin possesses low affinity thrombin binding sites in each E domain and retains the gamma' chain nonsubstrate thrombin-binding site.

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