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Immunological mechanism underlying the immune response to recombinant human protein therapeutics.

机译:对重组人蛋白质治疗剂免疫应答的潜在免疫学机制。

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摘要

Recombinant human (rhu) protein therapeutics are powerful tools to treat several severe diseases such as multiple sclerosis and diabetes mellitus, among others. A major drawback of these proteins is the production of anti-drug antibodies (ADAs). In some cases, these ADAs have neutralizing capacity and can interfere with the efficacy and safety of the drug. Little is known about the immunological mechanisms underlying the unwanted immune response against human homolog protein therapeutics. This article aims to provide current insights into recent immunological developments and to link this with regard to production of ADAs. A particular focus is given to aggregates being present in a rhu protein formulation and their impact on the immune system, subsequently leading to breakage of tolerance and formation of ADAs. Aggregation is one of the key factors in immunogenicity and by reducing aggregation one can reduce immunogenicity and make drugs safer and more efficient.
机译:重组人(rhu)蛋白疗法是治疗多种严重疾病(如多发性硬化症和糖尿病等)的强大工具。这些蛋白质的主要缺点是产生抗药物抗体(ADAs)。在某些情况下,这些ADA具有中和能力,并且会干扰药物的功效和安全性。关于针对人类同源蛋白治疗剂的有害免疫反应的潜在免疫机制知之甚少。本文旨在提供对最新免疫学发展的最新见解,并将其与ADA的产生联系起来。特别关注rhu蛋白配方中存在的聚集体及其对免疫系统的影响,随后导致耐受性破坏和ADAs的形成。聚集是免疫原性的关键因素之一,通过减少聚集可以降低免疫原性并使药物更安全,更有效。

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