Linkage analysis in von Willebrand disease |
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| Authors: | M. S. Verp R. M. Radvany D. Green P. M. Conneally V. A. Patel A. O. Martin J. L. Simpson |
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| Affiliation: | Departments of Obstetrics and Gynecology, Chicago, Illinois;Departments of Surgery, Chicago, Illinois;Departments of Atherosclerosis-Medicine, Northwestern University Medical School and Rehabilitation Institute of Chicago, Chicago, Illinois;Department of Medical Genetics, Indiana University School of Medicine, Indianapolis, Ind., U.S.A |
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| Abstract: | ![]()
We studied a 3-generation kindred to determine whether the gene responsible for one form of von Willebrand disease (vWD) is linked to 1) the HLA locus, or 2) a polymorphic locus for a serum enzyme or red cell antigen. HLA haplotypes were determined in 12 affected family members, in 10 cases by direct analysis and in 2 cases by deduction. Seven of 12 affected individuals were A2, B7, as compared to 0 of 9 unaffected. However, the maximum lod score was only 0.41 at a recombination frequency of 0.2. Of the 17 serum red cell and plasma protein markers studied, 5 (Kell, ADA, AK1, BF, GC) did not segregate, and 12 (ABO, Rh, JK, Fy, P, PGM1, ACPI, ESD, GLOl, MN, HP, GPT) gave lod scores less than +1.0. We conclude that there is no strong evidence for linkage between the locus for vWD and any of the markers studied. |
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| Keywords: | HLA linkage analysis von Willebrand disease |
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