Mutations and common polymorphisms in ADAMTS13 gene responsible for von Willebrand factor-cleaving protease activity
Koichi Kokame,Masanori Matsumoto,Kenji Soejima,Hideo Yagi,Hiromichi Ishizashi,Masahisa Funato,Hiroshi Tamai,Mutsuko Konno,Kei Kamide,Yuhei Kawano,Toshiyuki Miyata,Yoshihiro Fujimura +11 more
TL;DR: A single-nucleotide polymorphism associated with alterations in VWF-CP activity is reported and it will be important to assess this single- nucleotide SNP as a risk factor for thrombotic disorders.
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Abstract: von Willebrand factor (VWF) is synthesized primarily in vascular endothelial cells and secreted into the plasma as unusually large VWF multimers. Normally, these multimers are quickly degraded into smaller forms by a plasma metalloproteinase, VWF-cleaving protease (VWF-CP). Decreases in the activity of this enzyme result in congenital and acquired thrombotic thrombocytopenic purpura (TTP). The human VWF-CP has recently been purified. Cloning of the corresponding cDNA revealed that the 1,427-aa polypeptide is a member of the ADAMTS gene family, termed ADAMTS13. Twelve rare mutations in this gene have been identified in patients with congenital TTP. Here, we report missense and nonsense mutations in two Japanese families with Upshaw–Schulman syndrome, congenital TTP with neonatal onset and frequent relapses. The comparison of individual ADAMTS13 genotypes and plasma VWF-CP activities indicated that the R268P, Q449stop, and C508Y mutations abrogated activity of the enzyme, whereas the P475S mutant retained low but significant activity. The effects of these mutations were further confirmed by expression analysis in HeLa cells. Recombinant VWF-CP containing either the R268P or C508Y mutations was not secreted from cells. In contrast, Q449stop and P475S mutants were normally secreted but demonstrated minimal activity. Genotype analysis of 364 Japanese subjects revealed that P475S is heterozygous in 9.6% of individuals, suggesting that approximately 10% of the Japanese population possesses reduced VWF-CP activity. We report on a single-nucleotide polymorphism associated with alterations in VWF-CP activity; it will be important to assess this single-nucleotide polymorphism as a risk factor for thrombotic disorders.
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References
von Willebrand Factor—Cleaving Protease and Upshaw-Schulman Syndrome
Yoshihiro Fujimura,Masanori Matsumoto,Hideo Yagi,Akira Yoshioka,Taei Matsui,Koiti Titani +5 more
TL;DR: Successful purification of vWF-CPase revealed that this enzyme is composed of a single polypeptide with a molecular mass of approximately 190 kd, and its complementary DNA cloning unambiguously indicated that it is uniquely produced in the liver and its gene is located on chromosome 9q34.
Drug-associated thrombotic thrombocytopenic purpura-hemolytic uremic syndrome.
TL;DR: Five drugs that have been the subject of the most and the most recent reports of drug-associated TTP-HUS are discussed: mitomycin C, cyclosporine, quinine, ticlopidine, and clopidogrel.
Identification of a cleavage site directing the immunochemical detection of molecular abnormalities in type IIA von Willebrand factor.
TL;DR: Chemical evidence is obtained to locate the protease-sensitive bond between residues Tyr-842 and Met-843, a site that appears to reflect the specificity of calcium-dependent neutral proteases (calpains).
Localization of a collagen-interactive domain of human von Willebrand factor between amino acid residues Gly 911 and Glu 1,365
TL;DR: A collagen-binding domain of von Willebrand factor has been identified in the central part of the molecule by comparing the binding properties of vWF and Staphylococcus aureus V-8 protease-generated vWF fragments with collagen.
Hyaline thrombosis of the terminal arterioles and capillaries : a hitherto undescribed disease
Eli Moschcowitz
- 01 Jan 1924
TL;DR: For several years now, Answering T.T.P. Foundation has held an International TTP Day, to raise awareness of this rare disease and attention is also drawn to the stories of those affected or their family members.
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