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首页> 外文期刊>Human Immunology: Official Journal of the American Society for Histocompatibility and Immunogenetics >Structurally based epitope analysis of major histocompatibility complex class I-related chain A (MICA) antibody specificity patterns.
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Structurally based epitope analysis of major histocompatibility complex class I-related chain A (MICA) antibody specificity patterns.

机译:主要组织相容性复杂的I类相关链A(MICA)抗体特异性模式的基于结构的表位分析。

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摘要

Recent studies have suggested a clinical significance to the detection of anti-major histocompatibility complex class I-related chain A (MICA) antibodies in transplantation. We have developed an eplet-based version of the HLAMatchmaker algorithm to assess the epitope specificity of these antibodies. Molecular viewing of the MICA structure and the determination of amino acid sequence differences between MICA alleles has yielded a repertoire of 38 potentially immunogenic MICA eplets. These eplets are based on the functional epitope structure that considers a configuration of amino acids within a 3-Angstrom radius of an antibody-accessible polymorphic residue on the molecular surface. In this study MICA-reactive sera were screened in Luminex assays with single MICA allele panels and analyzed with HLAMatchmaker. We identified reactivity patterns that correspond to eplet-specific antibodies to identify of unacceptable MICA mismatches including those alleles that have not been tested with the serum. In conclusion, HLAMatchmaker is a useful algorithm to analyze the reactivity patterns of anti-MICA antibodies and the determination of MICA mismatch acceptability at the structural level.
机译:最近的研究表明,在移植中检测抗主要组织相容性复杂的I类相关链A(MICA)抗体具有临床意义。我们已经开发了基于小片段的HLAMatchmaker算法,以评估这些抗体的表位特异性。对MICA结构进行分子观察并确定MICA等位基因之间的氨基酸序列差异,已产生了38种具有潜在免疫原性的MICA小片段。这些小片段基于功能性表位结构,该功能性表位结构考虑了分子表面上抗体可及的多态性残基的3埃半径内的氨基酸构型。在这项研究中,在单个MICA等位基因组的Luminex分析中筛选了MICA反应性血清,并使用HLAMatchmaker进行了分析。我们鉴定了对应于eplet特异性抗体的反应模式,以鉴定不可接受的MICA错配,包括未经血清检测的那些等位基因。总之,HLAMatchmaker是一种有用的算法,可以在结构水平上分析抗MICA抗体的反应模式以及确定MICA错配的可接受性。

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