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Accurate pan-specific prediction of peptide-MHC class II binding affinity with improved binding core identification

机译:肽-MHC II类结合亲和力的精确泛特异性预测,结合核心鉴定得到改善

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摘要

A key event in the generation of a cellular response against malicious organisms through the endocytic pathway is binding of peptidic antigens by major histocompatibility complex class II (MHC class II) molecules. The bound peptide is then presented on the cell surface where it can be recognized by T helper lymphocytes. NetMHCIIpan is a state-of-the-art method for the quantitative prediction of peptide binding to any human or mouse MHC class II molecule of known sequence. In this paper, we describe an updated version of the method with improved peptide binding register identification. Binding register prediction is concerned with determining the minimal core region of nine residues directly in contact with the MHC binding cleft, a crucial piece of information both for the identification and design of CD4(+) T cell antigens. When applied to a set of 51 crystal structures of peptide-MHC complexes with known binding registers, the new method NetMHCIIpan-3.1 significantly outperformed the earlier 3.0 version. We illustrate the impact of accurate binding core identification for the interpretation of T cell cross-reactivity using tetramer double staining with a CMV epitope and its variants mapped to the epitope binding core. NetMHCIIpan is publicly available at http://www.cbs.dtu.dk/services/NetMHCIIpan-3.1.
机译:通过内吞途径产生针对恶意生物的细胞反应的关键事件是主要组织相容性复合物II类(MHC II类)分子与肽类抗原的结合。然后将结合的肽呈递到细胞表面,在那里可以被T辅助淋巴细胞识别。 NetMHCIIpan是用于定量预测与已知序列的任何人或小鼠II类MHC分子结合的肽的最新方法。在本文中,我们描述了具有改进的肽结合寄存器识别的方法的更新版本。结合寄存器预测与确定直接与MHC结合裂口接触的9个残基的最小核心区域有关,这是鉴定和设计CD4(+)T细胞抗原的重要信息。当将NetMHCIIpan-3.1应用于一组具有已知结合寄存器的51种肽-MHC复合物的晶体结构时,新方法NetMHCIIpan-3.1明显优于早期的3.0版本。我们举例说明了准确的结合核心鉴定对T细胞交叉反应性的解释,该结果使用CMV表位及其变体映射到表位结合核心的四聚体双重染色来解释。 NetMHCIIpan可在http://www.cbs.dtu.dk/services/NetMHCIIpan-3.1上公开获得。

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