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Monoclonal versus polyclonal anti-D in the treatment of ITP

机译:单克隆抗多抗D治疗ITP

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摘要

Immune thrombocytopenia (ITP) is an autoimmune bleeding disorder caused by low numbers of platelets generally due to the production of anti-platelet antibodies. One effective treatment for ITP patients who express the RhD antigen on their red blood cells has been the use of blood donor-derived pooled polyclonal anti-D. Although anti-D has served us well, it needs to be replaced with a recombinant product. While the mechanism of action of anti-D in ITP remains highly speculative, this has not thwarted attempts to replace anti-D with a monoclonal product. Although a single attempt at a monoclonal antibody was not successful in the 1990s for the treatment of ITP, more recent efforts in mouse models of ITP and ITP patients now show that monoclonal antibodies can be successful in ITP. These studies also finally help substantiate the concept that it is unlikely that contaminants in the original donor-derived preparations mediate the major ameliorative activity of anti-D in ITP.
机译:免疫性血小板减少症(ITP)是一种自身免疫性出血性疾病,通常是由于产生抗血小板抗体而导致血小板数量少所致。对于在红细胞上表达RhD抗原的ITP患者,一种有效的治疗方法是使用血液供体来源的合并多克隆抗D抗体。尽管anti-D对我们有用,但仍需要用重组产品代替。尽管ITP中抗D的作用机制仍具有高度推测性,但这并未阻止用单克隆产品替代抗D的尝试。尽管在1990年代单次尝试使用单克隆抗体未能成功治疗ITP,但最近在ITP和ITP患者的小鼠模型中进行的最新研究表明,单克隆抗体可以在ITP中成功。这些研究最终也有助于证实这一概念,即原始供体来源的制剂中的污染物不太可能介导ITP中抗D的主要改善作用。

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