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通过应用体外MHC结合数据以及免疫表位数据库和分析资源来评估蛋白质药物的免疫原性。

Evaluating the immunogenicity of protein drugs by applying in vitro MHC binding data and the immune epitope database and analysis resource.

作者信息

Paul Sinu, Kolla Ravi V, Sidney John, Weiskopf Daniela, Fleri Ward, Kim Yohan, Peters Bjoern, Sette Alessandro

机构信息

La Jolla Institute for Allergy and Immunology, 9420 Athena Circle, La Jolla, San Diego, CA 92037, USA.

出版信息

Clin Dev Immunol. 2013;2013:467852. doi: 10.1155/2013/467852. Epub 2013 Oct 8.

Abstract

The immune system has evolved to become highly specialized in recognizing and responding to pathogens and foreign molecules. Specifically, the function of HLA class II is to ensure that a sufficient sample of peptides derived from foreign molecules is presented to T cells. This leads to an important concern in human drug development as the possible immunogenicity of biopharmaceuticals, especially those intended for chronic administration, can lead to reduced efficacy and an undesired safety profile for biological therapeutics. As part of this review, we will highlight the molecular basis of antigen presentation as a key step in the induction of T cell responses, emphasizing the events associated with peptide binding to polymorphic and polygenic HLA class II molecules. We will further review methodologies that predict HLA class II binding peptides and candidate epitopes. We will focus on tools provided by the Immune Epitope Database and Analysis Resource, discussing the basic features of different prediction methods, the objective evaluation of prediction quality, and general guidelines for practical use of these tools. Finally the use, advantages, and limitations of the methodology will be demonstrated in a review of two previous studies investigating the immunogenicity of erythropoietin and timothy grass pollen.

摘要

免疫系统已经进化到能够高度特异地识别病原体和外来分子并做出反应。具体而言,HLA II类分子的功能是确保将来自外来分子的足够数量的肽样本呈递给T细胞。这在人类药物研发中引发了一个重要问题,因为生物药物,尤其是那些用于长期给药的药物,可能具有的免疫原性会导致生物治疗药物的疗效降低以及出现不良的安全性状况。作为本综述的一部分,我们将强调抗原呈递的分子基础作为诱导T细胞反应的关键步骤,着重阐述与肽结合到多态性和多基因HLA II类分子相关的事件。我们还将回顾预测HLA II类结合肽和候选表位的方法。我们将聚焦于免疫表位数据库和分析资源提供的工具,讨论不同预测方法的基本特征、预测质量的客观评估以及这些工具实际应用的一般指南。最后,通过回顾之前两项分别研究促红细胞生成素和梯牧草花粉免疫原性的研究,将展示该方法的用途、优势和局限性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/fc20/3816028/94b046d65651/CDI2013-467852.001.jpg

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