Effects of anti-factor VIII inhibitor antibodies on factor VIIa/tissue factor-catalysed activation and inactivation of factor VIII

被引:6
|
作者
Yada, Koji [1 ]
Nogami, Keiji [1 ]
Ogiwara, Kenichi [1 ]
Shibata, Masaru [1 ]
Shima, Midori [1 ]
机构
[1] Nara Med Univ, Dept Pediat, Nara 6348522, Japan
关键词
FVIII; FVIII inhibitor antibodies; FVIIa/TF; activation/inactivation; cleavage; A2; DOMAIN; FACTOR XA; INTERACTIVE SITE; HEAVY-CHAIN; COAGULANT ACTIVITY; TISSUE FACTOR; LIGHT-CHAIN; C2; FACTOR-IX; BINDING;
D O I
10.1160/TH10-12-0781
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Factor (F)VIIa/tissue factor (IF) rapidly activates FVIII activity by proteolysis at Arg(372) and Arg(740), and subsequently inactivates FVIIIa activity by proteolysis at Arg(336), although this activation is weaker than that by thrombin. The effects of anti-FVIII inhibitor antibodies on these reactions remain unknown, however. In this study, 13 of anti-FVIII inhibitor antibodies recognising the A2 or C2 domain were prepared. None of them, irrespective of epitope specificity, significantly affected FVIIa/TF-catalysed FVIII activation in one-stage clotting assays. Anti-A2 and anti-C2 type 2 antibodies had little effect on the inactivation phase. Anti-C2 type 1 antibodies, however, modulated inactivation by 40-60% of that seen with control IgG, suggesting that the activity of FVIIIa generated by FVIIa/TF persisted in the presence of this specific type of inhibitor. SDS-PAGE analysis demonstrated that all antibodies had little effect on FVIIa/TF-catalyzed proteolysis at Arg(372) and Arg(740). Anti-C2 type 1, however, significantly delayed cleavage at Arg(336) in dose-dependent manners. Neither anti-A2 nor anti-C2 type 2 affected this reaction, and the findings were consistent with the results of the functional assays. In addition, anti-C2 monoclonal antibodies with type 1 and 2 demonstrated similar patterns of reaction as the anti-C2 polyclonal antibodies in FVIIa/TF-mediated FVIII mechanisms. We demonstrated that FVIIa/TF activated FVIII even in the presence of anti-FVIII antibodies, but inactivation patterns appeared to depend on inhibitor type. It could be important to determine the characteristic of these inhibitor antibodies for prediction of their effects on FVIIa-related FVIII reactions, and the results could have significant therapeutic implications.
引用
收藏
页码:989 / 998
页数:10
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