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治疗性人免疫球蛋白制剂中载脂蛋白 H(β2-糖蛋白 I)的污染。

Contamination of therapeutic human immunoglobulin preparations with apolipoprotein H (β2-glycoprotein I).

机构信息

AGES Medizinmarktaufsicht, Vienna, Austria.

出版信息

Electrophoresis. 2014 Feb;35(4):515-21. doi: 10.1002/elps.201300319. Epub 2013 Nov 24.

Abstract

Polyclonal immunoglobulin (Ig) concentrates are important biological medicinal products and the assurance of their quality and safety is crucial. In our present approach we used proteomic methods to check the purity of commercial Ig products of different origin. The experimental setup included nonreducing 2DE or DIGE combined with MALDI-TOF and the thrombin generation assay, a routine safety test for pharmaceutical Ig preparations, and was complemented by a specific immunoassay. 2DE patterns displayed contaminations with trace amounts of human apolipoprotein H (Apo-H), transferrin, albumin, and its fragments. In contrast to the latter, Apo-H is a protein that is active in the coagulation cascade, and thus a potential involvement in thromboembolic events in vivo cannot be excluded. It was found by 2DE and MALDI-TOF to be a contaminant of several Ig preparations. Spiking experiments of Ig preparations with pure Apo-H demonstrated an Apo-H concentration dependent increase in thrombin generation assay values. Traces of Apo-H are possibly also contributing to unwanted side effects, as already known for factor XIa. The significance of Apo-H contaminations for these side effects might be verified by detailed analyses of pharmacovigilance data.

摘要

多克隆免疫球蛋白 (Ig) 浓缩物是重要的生物药物,确保其质量和安全性至关重要。在我们目前的方法中,我们使用蛋白质组学方法来检查不同来源的商业 Ig 产品的纯度。实验方案包括非还原 2-DE 或 DIGE 与 MALDI-TOF 结合,以及凝血酶生成试验,这是一种用于药物 Ig 制剂的常规安全性测试,并通过特定的免疫测定法进行补充。2-DE 图谱显示痕量的人载脂蛋白 H (Apo-H)、转铁蛋白、白蛋白及其片段的污染。与后者不同的是,Apo-H 是一种在凝血级联中具有活性的蛋白质,因此不能排除其在体内血栓栓塞事件中的潜在作用。通过 2-DE 和 MALDI-TOF 发现,它是几种 Ig 制剂的污染物。用纯 Apo-H 对 Ig 制剂进行的加标实验表明,凝血酶生成试验值随 Apo-H 浓度的增加而增加。Apo-H 的痕迹也可能导致不需要的副作用,正如已经知道的因子 XIa 一样。通过详细分析药物警戒数据,可以验证 Apo-H 污染对这些副作用的意义。

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