Crucial role for the VWF A1 domain in binding to type IV collagen

Flood, Veronica H.; Schlauderaff, Abraham; Haberichter, Sandra L.; Slobodianuk, Tricia L; Jacobi, Paula M.; Bellissimo, Daniel B.; Christopherson, Pamela A.; Friedman, Kenneth D.; Hoffmann, Raymond G.; Montgomery, Robert R.; Abshire, Thomas C.; Dunn, Amy L.; Bennett, Carolyn M.; Lusher, Jeanne M.; Rajpurkar, Madhvi; Brown, Deborah L; Shapiro, Amy D.; Lentz, Steven R.; Gill, Joan Cox; Leissinger, Cindy; Ragni, Margaret V.; Hord, Jeffrey D.; Manco‐Johnson, Marilyn J.; Strouse, John J.; Ma, Alice; Valentino, Leonard A.; Boggio, Lisa; Sharathkumar, Anjali; Gruppo, Ralph A.; Kerlin, Bryce A.; Journeycake, Janna M.; Kulkarni, Roshni; Green, D.; Mahoney, Donald H.; Mathias, Liesl; Bedros, Antranik A.; Diamond, Carol; Neff, Anne T.; Michele, D’Elia; Giardina, Patricia J.; Cohen, Alan; Paidas, Michael J.; Werner, Eric; Matsunaga, Atsuko; Tarantino, Michael D.; Shafer, Frank; Konkle, Barbara A.; Cuker, Adam; Kouides, Peter A.; Stein, Dagmar

doi:10.1182/blood-2014-11-610824

Cited by 83 publications

(87 citation statements)

References 35 publications

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“…Differences in collagen binding were observed as previously reported. 19 At the time of initiation of this study, type 2M did not routinely include collagen-binding variants, so these subjects remained in the type 1 cohort for this study.…”

Section: Resultsmentioning

confidence: 99%

“…Our data showed that subjects with laboratory findings otherwise consistent with type 1 VWD but with low VWF:CB4 had increased bleeding symptoms as measured by BS. 19 Although only 12 subjects were affected, this represented 4% of type 1 subjects. This raises the possibility that these subjects may be better classified as type 2M VWD on the basis of a functional defect in the VWF protein, even though the VWF:RCo/VWF:Ag ratio was normal.…”

Section: Discussionmentioning

confidence: 99%

“…19 The median BS for the subjects with low VWF:CB4 group was 10.5, as compared with a median BS of 5 for the remainder of the type 1 subjects with VWF:CB4/VWF:Ag .0.5 or median BS of 6 when comparison type 1 subjects were matched for comparable VWF:Ag, age, gender, race, and ethnicity. This difference was not statistically significant, but when subjects ,18 were excluded (due to having less time to generate significant bleeding symptoms), the median BS was 13.5 for those with low VWF:CB4/VWF:Ag ratios compared with 7 for those with normal ratios (P , .01).…”

Section: Org Frommentioning

confidence: 99%

“…17 Multimer distribution was assayed by quantitative gel electrophoresis. 18 Ligand binding assays were performed as previously described, including VWF binding to type III collagen (VWF:CB3), 16 VWF binding to type IV collagen (VWF:CB4), 19 and VWF binding to mutant platelet GPIb (VWF:GPIbM). 20,21 VWF propeptide (VWFpp) was measured to evaluate for VWF clearance defects.…”

Section: Laboratory Evaluationmentioning

confidence: 99%

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Clinical and laboratory variability in a cohort of patients diagnosed with type 1 VWD in the United States

Flood

Christopherson

Gill

et al. 2016

Blood

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Org Frommentioning

confidence: 99%

Section: Laboratory Evaluationmentioning

confidence: 99%

See 2 more Smart Citations

Clinical and laboratory variability in a cohort of patients diagnosed with type 1 VWD in the United States

Flood

Christopherson

Gill

et al. 2016

Blood

Self Cite

111

171

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“…In this case, the majority of mutations are located in the A3 domain, and exons 29-32 should be investigated. A small proportion of A1 domain mutations result from collagen types IV or VI binding defects [34].…”

Section: Molecular Characterization Of Type 1 and 3 Vwd Patientsmentioning

confidence: 99%

Molecular diagnosis of von Willebrand disease

2017

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word count: 212 Text word count: 3781Number of Tables and Figures: Tables 3, Figures 3 2 AbstractThe role of molecular characterization in the diagnosis of VWD is not essential if the patients have been extensively investigated using phenotypic analysis. On the other hand, if some of these phenotype assays are not available, the identification of the mutation causing the disease could be crucial for an accurate diagnosis. Nevertheless, there are several reasons for performing molecular analysis in patients phenotypically well characterized, e.g. to identify the mutation causing VWD can be useful for patients and their family members when prenatal diagnosis is required (type 3 or severe type 2).In this manuscript we report the techniques used for the molecular characterization of suspected VWD patients. We describe the use of online VWF database and online SNV (single nucleotide variation) databases, the former to verify whether a candidate mutation has been previously identified in other VWD patients and the latter to ascertain whether a putative mutation has been reported earlier in healthy individuals. We listed the available in silico analysis tools, to determine the predicted pathogenicity of a sequence variant and to establish its possible negative effect on the normal splicing process. We also report the strategy that can be used to identify VWD type 2 patients' mutations in subjects that have been fully characterized using the phenotype assays.

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