Von Willebrand factor Ristocetin co-factor activity to von Willebrand factor antigen level ratio for diagnosis of acquired von Willebrand syndrome caused by aortic stenosis

Noriyuki Okubo,Hisanori Horiuchi,Tohru Fujiwara,Hiroshi Takiguchi,Koichi Kokame,Kenichi Tsujita,Masaki Hayakawa,Yoshimitsu Soga,Shin-Ichi Fujimaki,Ryutaro Shirakawa,Masaki Tateishi,Hiroaki Shimokawa,Shingo Sugawara,Yasunori Kawate,Kota Goto,Takeshi Kimura,Nobuhiro Yaoita,Tsuyoshi Doman,Mihoko Yamashita,Shin Watanabe,Hiroyuki Takahama,Yoshihiro Fukumoto,Yoshikatsu Saiki,Koichi Kaikita,Yoshio Arai,Toshihiro Tamura,Hiroshi Nakase,Misako Suzuki,Satoshi Yasuda,Masanori Matsumoto,Mizuki Miura,Takaharu Nakayoshi,Shinichi Shirai,Kenji Ando,Yuka Eura,Shinji Yoshii,Ko Sakatsume

doi:10.1016/j.rpth.2023.102284

Noriyuki Okubo, Hisanori Horiuchi + Show 35 more

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https://doi.org/10.1016/j.rpth.2023.102284

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Abstract

BackgroundSevere aortic stenosis (AS) causes acquired von Willebrand syndrome by the excessive shear stress–dependent cleavage of high molecular weight multimers of von Willebrand factor (VWF). While the current standard diagnostic method is so-called VWF multimer analysis that is western blotting under nonreducing conditions, it remains unclear whether a ratio of VWF Ristocetin co-factor activity (VWF:RCo) to VWF antigen levels (VWF:Ag) of <0.7, which can be measured with an automated coagulation analyzer in clinical laboratories and is used for the diagnosis of hereditary von Willebrand disease. ObjectivesTo evaluated whether the VWF:RCo/VWF:Ag is useful for the diagnosis of AS-induced acquired von Willebrand syndrome. MethodsVWF:RCo and VWF:Ag were evaluated with the VWF large multimer index as a reference, which represents the percentage of a patient’s VWF high molecular weight multimer ratio to that of standard plasma in the VWF multimer analysis. ResultsWe analyzed 382 patients with AS having transaortic valve maximal pressure gradients of >30 mmHg, 27 patients with peripheral artery disease, and 46 control patients free of cardiovascular disease with osteoarthritis, diabetes, and so on. We assumed a large multimer index of <80% as loss of VWF large multimers since 59.0% of patients with severe AS had the indices of <80%, while no control patients or patients with peripheral artery disease, except for 2 patients, exhibited the indices of <80%. The VWF:RCo/VWF:Ag ratios, measured using an automated blood coagulation analyzer, were correlated with the indices (rs = 0.470, P < .001). When the ratio of <0.7 was used as a cut-off point, the sensitivity and specificity to VWF large multimer indices of <80% were 0.437 and 0.826, respectively. ConclusionVWF:RCo/VWF:Ag ratios of <0.7 may indicate loss of VWF large multimers with high specificity, but low sensitivity. VWF:RCo/VWF:Ag ratios in patients with AS having a ratio of <0.7 may be useful for monitoring the loss of VWF large multimers during their clinical courses.

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