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Detection of autoimmunity by pharmaceuticals.

机译:通过药物检测自身免疫。

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摘要

Despite the important health and economic impact of autoimmunogenicity or allergenicity by pharmaceuticals models to detect such adverse effects are not available yet. The most important reason for this is the related complex interplay of multiple factors, for which reason these adverse effects are also referred to as idiosyncratic in nature. Moreover, clinical effects are quite diverse, and involve both organ-specific and systemic effects, including a diversity of skin diseases. Because of its complexity on the one hand and the fundamental knowledge on certain particular mechanistic effects it may be more relevant to design a rationalistic toolbox of test models from which a predictive strategy can be composed. Since one mechanistic aspect centers around T cell sensitization a straightforward lymph node assay such as the reporter antigen-popliteal lymph node assay (RA-PLNA) would fit in such a toolbox. This RA-PLNA holds a strong promise to distinguish sensitizing and/or neoantigen-forming capacity oflow molecular weight pharmaceuticals. In addition, from the pharmacokinetic point of view a rationalistic toolbox should also contain oral exposure models with immunological read out parameters in normal or in genetically predisposed animal strains. This review focuses on these two categories of candidate test methods, PLNA and oral exposure models, and proposes to use these in tandem in order to predict the hazard of induction of allergy or autoimmune phenomena by new pharmaceutical candidates.
机译:尽管药物自身免疫原性或致敏性对健康和经济产生了重要影响,但尚无用于检测此类不良反应的模型。最重要的原因是多个因素相关的复杂相互作用,因此这些不利影响在本质上也被称为特质。此外,临床效果十分多样,涉及器官特异性和全身性影响,包括多种皮肤疾病。一方面,由于其复杂性以及对某些特定机械作用的基础知识,因此设计测试模型的合理性工具箱(从中可以构成预测策略)可能更为相关。由于一个机械方面集中于T细胞致敏,因此一种简单的淋巴结测定法(例如报道分子抗原-lite细胞淋巴结测定法(RA-PLNA))将适合这种工具箱。该RA-PLNA有望区分低分子量药物的敏化和/或新抗原形成能力。此外,从药代动力学的角度来看,理性工具箱还应包含正常或遗传易感动物品系中具有免疫学读出参数的口服暴露模型。这篇综述着重于这两种候选测试方法,即PLNA和口服暴露模型,并建议将它们串联使用,以预测新的候选药物诱发过敏或自身免疫现象的危险。

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