Abstract

Functions domains of factor IX will be defined by four overlapping approaches. Congenital defects provide dozens of distinct mutants, the structural bases of which can be correlated to clinical severity and specific levels of functional, in vitro interactions. Specific antisera,including monoclonal antibodies and polycolonal fractions, assist in localizing defects or functions. Synthetic peptides can be used to prepare specific antisera and to directly inhibit functional interactions. Finally, for regions in which synthetic peptides inadequately reflect surface structure, synthetic fragments can be produced by expression of mutated cDNAs in an appropriate vector which has been transfected into a cultured cell line. This proposal focuses upon distinct functional domains of factor IX. These are presented from the N to the C terminus. First, we will define the defect in a hemophilic IX which as abnormal calcium-binding properties. A synthetic leader peptide will be tested further for both stimulation of Gla formation in cell expression systems and with Dr. Suttie, for its structural requirements for interaction with the carboxylase system in vitro. Secondly, hemophilic defects involving the fourth exon will be characterized by analyses of their DNA and isolated proteins. A major effort will mounted to produce recombinant factor IX fragments containing the growth factor-like regions(s) in order to probe its role in hemostasis. Both locally with Dr. Heimark and with Dr. Stern in New York, peptides, antibodies and isolated abnormal IXs will be studied for IX binding to endothelial cells. Other potential roles of this region will be assessed by in vitro clotting and binding studies and animal survival measurements of the recombinant fragments. We will confirm that a specific antibody fraction to an exon IV eptiope recognizes a non-Gla, calcium binding sire. The use of a monoclonal a-IX recognizing an exonic polymorphism will be extended from IX to VIII and von Willebrand factor to develop rapid immunoassays for carrier testing in hemophilia A and von Willebrand disease. Attempts will be made to prepare antibodies specific for factor IXa. Peptides to sequences in the variable portion of IXa's heavy chain will be studied and new reagents developed to probe the function of the active enzyme. Binding antibodies in patients with severe defects will be characterized to develop strategies for localization of their defects. A heavy chain defect due to a point mutation in a Taq1 cleavage site will be defined by oligonucleotide probes, to compare with functional data of the hemophilic mutation.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL031193-05
Application #
3342238
Study Section
Hematology Subcommittee 2 (HEM)
Project Start
1988-12-01
Project End
1993-11-30
Budget Start
1989-12-01
Budget End
1990-11-30
Support Year
5
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Puget Sound Blood Center
Department
Type
DUNS #
City
Seattle
State
WA
Country
United States
Zip Code
98104

  Publications

Weinmann, A F; Schoof, J M; Thompson, A R (1996) Clinical correlates among 49 families with hemophilia A and factor VIII gene inversions. Am J Hematol 51:192-9
Kim, D J; Thompson, A R; Nash, D R et al. (1995) Factors XWenatchee I and II: compound heterozygosity involving two variant proteins. Biochim Biophys Acta 1271:327-34
Kim, D J; Thompson, A R; James, H L (1995) Factor XKetchikan: a variant molecule in which Gly replaces a Gla residue at position 14 in the light chain. Hum Genet 95:212-4
Chen, S H; Schoof, J M; Weinmann, A F et al. (1995) Heteroduplex screening for molecular defects in factor IX genes from haemophilia B families. Br J Haematol 89:409-12
Thompson, A R; Chen, S H (1994) Germ line origins of de novo mutations in hemophilia B families. Hum Genet 94:299-302
Chen, S H; Schoof, J M; Scott, C R et al. (1993) Five novel factor IX mutations in unrelated hemophilia B families. Hum Mol Genet 2:599-600
Thompson, A R; Chen, S H (1993) Characterization of factor IX defects in hemophilia B patients. Methods Enzymol 222:143-69
Weinmann, A F; Reiner, A P; Thompson, A R (1993) A polymorphic MseI site 5' to the factor IX gene varies among ethnic groups. Hum Mol Genet 2:486
Reiner, A P; Thompson, A R (1992) Screening for nonsense mutations in patients with severe hemophilia A can provide rapid, direct carrier detection. Hum Genet 89:88-94
Reiner, A P; Stray, S M; Thompson, A R (1992) Three missense mutations in Arg codons of the factor VIII genes of mild to moderately severe hemophilia A patients. Thromb Res 66:93-9

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