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J Thromb Haemost. 2018 Sep;16(9):1779-1788. doi: 10.1111/jth.14233. Epub 2018 Aug 13.
6
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7
High-affinity, noninhibitory pathogenic C1 domain antibodies are present in patients with hemophilia A and inhibitors.高亲和力、非抑制性致病性C1结构域抗体存在于甲型血友病和有抑制剂的患者中。
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本文引用的文献

1
Mitral valve repair in a Jehovah's witness with haemophilia A with high-titre inhibitor.
Haemophilia. 2015 Nov;21(6):e523-5. doi: 10.1111/hae.12789. Epub 2015 Aug 17.
2
The diversity of the immune response to the A2 domain of human factor VIII.人凝血因子 VIII A2 结构域的免疫应答多样性。
Blood. 2013 Apr 4;121(14):2785-95. doi: 10.1182/blood-2012-09-456582. Epub 2013 Jan 24.
3
Potentiation of thrombin generation in hemophilia A plasma by coagulation factor VIII and characterization of antibody-specific inhibition.凝血因子VIII对甲型血友病血浆中凝血酶生成的增强作用及抗体特异性抑制的特征分析
PLoS One. 2012;7(10):e48172. doi: 10.1371/journal.pone.0048172. Epub 2012 Oct 29.
4
Discrepancy between one-stage and chromogenic factor VIII activity assay results can lead to misdiagnosis of haemophilia A phenotype.一期法和显色因子 VIII 活性测定结果之间的差异可能导致血友病 A 表型的误诊。
Hamostaseologie. 2010 Nov;30(4):207-11.
5
Non-classical anti-factor VIII C2 domain antibodies are pathogenic in a murine in vivo bleeding model.非经典抗凝血因子VIII C2结构域抗体在小鼠体内出血模型中具有致病性。
J Thromb Haemost. 2009 Apr;7(4):658-64. doi: 10.1111/j.1538-7836.2009.03299.x. Epub 2009 Jan 24.
6
Kinetics of factor VIII:C inhibitors and treatment response in severe hemophilia A patients.因子 VIII:C 抑制剂的动力学及其对严重血友病 A 患者的治疗反应。
Int J Lab Hematol. 2009 Dec;31(6):673-82. doi: 10.1111/j.1751-553X.2008.01099.x. Epub 2008 Sep 1.
7
One-stage and chromogenic FVIII:C assay discrepancy in mild haemophilia A and the relationship with the mutation and bleeding phenotype.轻度甲型血友病中一步法与显色法FVIII:C检测结果的差异及其与突变和出血表型的关系。
Haemophilia. 2008 Sep;14(5):1049-54. doi: 10.1111/j.1365-2516.2008.01781.x. Epub 2008 Jun 5.
8
Nonclassical anti-C2 domain antibodies are present in patients with factor VIII inhibitors.非典型抗C2结构域抗体存在于患有VIII因子抑制剂的患者体内。
Blood. 2008 Aug 15;112(4):1151-3. doi: 10.1182/blood-2008-01-132639. Epub 2008 May 21.
9
Antihuman factor VIII C2 domain antibodies in hemophilia A mice recognize a functionally complex continuous spectrum of epitopes dominated by inhibitors of factor VIII activation.血友病A小鼠中的抗人因子VIII C2结构域抗体识别出一个功能复杂的连续表位谱,该表位谱以因子VIII激活抑制剂为主导。
Blood. 2007 Dec 15;110(13):4234-42. doi: 10.1182/blood-2007-06-096842. Epub 2007 Sep 11.
10
The humoral response to human factor VIII in hemophilia A mice.血友病A小鼠对人凝血因子VIII的体液免疫反应。
J Thromb Haemost. 2007 Mar;5(3):512-9. doi: 10.1111/j.1538-7836.2007.02373.x. Epub 2006 Dec 20.

高滴度抗凝血因子VIII A2结构域抗体的一个亚群对凝血因子VIII治疗有反应。

A subset of high-titer anti-factor VIII A2 domain antibodies is responsive to treatment with factor VIII.

作者信息

Eubanks Joshua, Baldwin W Hunter, Markovitz Rebecca, Parker Ernest T, Cox Courtney, Kempton Christine L, Meeks Shannon L

机构信息

School of Medicine, Emory University, Atlanta, GA;

Aflac Cancer and Blood Disorders Center, Children's Healthcare of Atlanta/Emory University, Atlanta, GA; and.

出版信息

Blood. 2016 Apr 21;127(16):2028-34. doi: 10.1182/blood-2015-09-670034. Epub 2016 Jan 29.

DOI:10.1182/blood-2015-09-670034
PMID:26825708
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4841042/
Abstract

The primary B-cell epitopes of factor VIII (fVIII) are in the A2 and C2 domains. Within the C2 domain, antibody epitope and kinetics are more important than inhibitor titer in predicting pathogenicity in a murine bleeding model. To investigate this within the A2 domain, the pathogenicity of a diverse panel of antihuman fVIII A2 domain monoclonal antibodies (MAbs) was tested in the murine model. MAbs were injected into hemophilia A mice, followed by injection of human B domain-deleted fVIII. Blood loss after a 4-mm tail snip was measured. The following anti-A2 MAbs were tested: high-titer type 1 inhibitors 4A4, 2-76, and 1D4; 2-54, a high-titer type 2 inhibitor; B94, a type 2 inhibitor; and noninhibitory MAbs GMA-012, 4C7, and B25. All high-titer type 1 MAbs produced blood loss that was significantly greater than control mice, whereas all non-inhibitory MAbs produced blood loss that was similar to control. The type 2 MAbs were not pathogenic despite 2-54 having an inhibitor titer of 34 000 BU/mg immunoglobulin G. In addition, a patient with a high-titer type 2 anti-A2 inhibitor who is responsive to fVIII is reported. The discrepancy between inhibitor titer and bleeding phenotype combined with similar findings in the C2 domain stress the importance of inhibitor properties not detected in the standard Bethesda assay in predicting response to fVIII therapy.

摘要

凝血因子VIII(fVIII)的主要B细胞表位位于A2和C2结构域。在C2结构域内,在预测小鼠出血模型的致病性方面,抗体表位和动力学比抑制剂滴度更重要。为了在A2结构域内研究这一点,在小鼠模型中测试了多种抗人fVIII A2结构域单克隆抗体(MAb)的致病性。将MAb注射到甲型血友病小鼠体内,随后注射人B结构域缺失的fVIII。测量4毫米剪尾后的失血量。测试了以下抗A2 MAb:高滴度1型抑制剂4A4、2-76和1D4;2-54,一种高滴度2型抑制剂;B94,一种2型抑制剂;以及非抑制性MAb GMA-012、4C7和B25。所有高滴度1型MAb导致的失血量均显著高于对照小鼠,而所有非抑制性MAb导致的失血量与对照相似。尽管2-54的抑制剂滴度为34000 BU/mg免疫球蛋白G,但2型MAb无致病性。此外,还报告了一名对fVIII有反应的高滴度2型抗A2抑制剂患者。抑制剂滴度与出血表型之间的差异以及C2结构域中的类似发现强调了在标准贝塞斯达试验中未检测到的抑制剂特性在预测对fVIII治疗反应方面的重要性。