首页> 外文期刊>Thrombosis and Haemostasis: Journal of the International Society on Thrombosis and Haemostasis >Dominant C2 domain epitope specificity of inhibitor antibodies elicited by a heat pasteurized product, factor VIII CPS-P, in previously treated hemophilia A patients without inhibitors.
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Dominant C2 domain epitope specificity of inhibitor antibodies elicited by a heat pasteurized product, factor VIII CPS-P, in previously treated hemophilia A patients without inhibitors.

机译:在没有抑制剂的先前治疗过的血友病A患者中,由热巴氏灭菌产品VIII因子CPS-P引起的抑制剂抗体的主要C2域抗原决定簇特异性。

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摘要

From June, 1990, to November, 1991, in The Netherlands and Belgium, 16 previously treated severe hemophilia A patients (PTP) developed inhibitors after exposure to factor VIII CPS-P, a new heat pasteurized product. A previously untreated patient (PUP) also developed an inhibitor to CPS-P. In inhibitor neutralization assays with recombinant fVIII C2 and A2 domain polypeptides, plasmas from 14 PTPs were > or = 79% neutralized by C2 and < 10% by A2, but the PUP plasma was partially neutralized by C2 (48%) and A2 (28%). Immunoprecipitation assays of the PTP and PUP plasmas with the fVIII heavy chain and with recombinant C2 and A3-C1 polypeptides confirmed that the C2 dominant immune response to CPS-P was found only in the PTPs. Competition of the binding of 2 inhibitors to 125I-CPS-P by unlabeled CPS-P and another plasma fVIII was similar, demonstrating that the antibody response was not directed to epitopes only present in CPS-P. We propose that the immunogenicity of the CPS-P C2 domain was altered by heat pasteurization.
机译:从1990年6月到1991年11月,在荷兰和比利时,有16名先前接受过治疗的重度A型血友病患者(PTP)在暴露于一种新的热巴氏灭菌的因子VIII CPS-P后产生了抑制剂。先前未治疗的患者(PUP)也产生了CPS-P抑制剂。在使用重组fVIII C2和A2结构域多肽的抑制剂中和测定中,来自14个PTP的血浆被C2中和> 79%,被A2 <10%,但PUP血浆被C2(48%)和A2部分中和(28 %)。具有fVIII重链以及重组C2和A3-C1多肽的PTP和PUP血浆的免疫沉淀测定证实,仅在PTP中发现了对CPS-P的C2显性免疫应答。未标记的CPS-P与另一种血浆fVIII对2种抑制剂与125I-CPS-P结合的竞争是相似的,这表明抗体应答并不针对仅存在于CPS-P中的表位。我们建议通过热巴氏灭菌法改变CPS-P C2域的免疫原性。

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