Abstract

Nascent fibrin that is formed on release of fibrinopeptide A by thrombin is carried in a soluble, monomeric form reversibly complexed with fibrinogen in blood. Rapid clearance of this fibrin from the circulation appears to depend on a recently identified receptor-mediated mechanism for endocytotic uptake by phagocytic cells. The clearance of fibrin prior to its incorporation into tightly bound aggregates is suggested to be of critical importance in reducing dependence on thrombolytic pathways for its removal. There are indications that specific uptake of fibrinogen monomer involves the aggregation site that is blocked by fibrinopeptide A in the parent fibrinogen molecule. Continued studies are proposed to characterize the fibrin-specific receptors in mouse J774A.1 and human U-937 macrophage/monocyte cell lines which bind monomer and NDSK preparations of fibrin with specificities identical to peritoneal macrophages. These studies will be aided by highly selective modifications of fibrin and fibrin derivatives for specific affinity labelling and isolation of the receptors. New interrelationships between dissociability of fibrin complexes and receptor mediated clearance provide insights into biologic significances of fibrinopeptide B release and the cross-linking that occur toward end stages of fibrin formation. Hypotheses pertaining to fibrin assembly and its metabolism will be detailed through direct analysis of equilibria in fibrin/fibrinogen interactions, coupled interactions with fibrinogen dimer and effects on fibrin clearance, and identification of critical epitopes functioning in fibrin assembly and cellular uptake. Cross-lined fibrin complexes and degradation products corresponding to pre-and post-thrombus products can be readily differentiated and subclassified from immunoelectrophoretic analysis of plasma and serum. Both families of derivatives have been found consistently elevated in patients with claudication from peripheral arterial thromboembolism, and the levels of these fibrinogen derivatives do not change substantially during or after catheter-directed thrombolysis with tissue-plasminogen activator. Their persistence without substantial change in course of treatment prompts a hypothesis that the localized arterial emboli were symptomatic of a more extensive, possibly systemic coagulopathic process. Similar fibrinogen derivatives have been found to be pathognomonic for departure from a benign to a malignant form of experimental hypertension in rats. The proposed studied address precise characterization of the derivatives by immunochemical and direct amino aid sequencing methods, analysis of their disparate clearance mechanisms, and a new approach to assessing fibrinogen turnover. Focused study of these patients will provide criteria for identifying subjects with a predisposition to intravascular coagulation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL016361-11
Application #
3335192
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1976-04-01
Project End
1991-06-30
Budget Start
1988-07-01
Budget End
1989-06-30
Support Year
11
Fiscal Year
1988
Total Cost
Indirect Cost

  Institution

Name
Cleveland Clinic Lerner
Department
Type
DUNS #
017730458
City
Cleveland
State
OH
Country
United States
Zip Code
44195

  Publications

Shainoff, John R; Smejkal, Gary B; DiBello, Patricia M et al. (2002) Allosteric effects potentiating the release of the second fibrinopeptide A from fibrinogen by thrombin. J Biol Chem 277:19367-73
Mitkevich, O V; Shainoff, J R; DiBello, P M et al. (1998) Coagulation factor XIIIa undergoes a conformational change evoked by glutamine substrate. Studies on kinetics of inhibition and binding of XIIIA by a cross-reacting antifibrinogen antibody. J Biol Chem 273:14387-91
Smejkal, G B; Shainoff, J R (1997) Enhanced digital imaging of diaminobenzidene-stained immunoblots. Biotechniques 22:462
Odrljin, T M; Shainoff, J R; Lawrence, S O et al. (1996) Thrombin cleavage enhances exposure of a heparin binding domain in the N-terminus of the fibrin beta chain. Blood 88:2050-61
Mitkevich, O V; Sobel, J H; Shainoff, J R et al. (1996) Monoclonal antibody directed to a fibrinogen A alpha #529-539 epitope inhibits alpha-chain crosslinking by transglutaminases. Blood Coagul Fibrinolysis 7:85-92
Shainoff, J R; Smejkal, G B; Mitkevich, O et al. (1996) Preparative electrophoresis on linear polyacrylamide-agarose composite gels. Electrophoresis 17:179-84
Shainoff, J R; Smejkal, G B; DiBello, P M et al. (1996) Isolation and characterization of the fibrin intermediate arising from cleavage of one fibrinopeptide A from fibrinogen. J Biol Chem 271:24129-37
Shainoff, J R; Estafanous, F G; Yared, J P et al. (1994) Low factor XIIIA levels are associated with increased blood loss after coronary artery bypass grafting. J Thorac Cardiovasc Surg 108:437-45
Shainoff, J R; Urbanic, D A; DiBello, P M et al. (1993) GPR-phoresis, a novel approach to determining fibrin monomer and other macromolecular derivatives of fibrinogen and fibrin in blood. Blood Coagul Fibrinolysis 4:87-92
Valenzuela, R; Shainoff, J R; DiBello, P M et al. (1992) Immunoelectrophoretic and immunohistochemical characterizations of fibrinogen derivatives in atherosclerotic aortic intimas and vascular prosthesis pseudo-intimas. Am J Pathol 141:861-80

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