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HistoCheck: rating of HLA class I and II mismatches by an internet-based software tool.

机译:HistoCheck:通过基于Internet的软件工具对HLA I级和II级不匹配进行评级。

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摘要

HLA polymorphism is a major barrier for hematopoietic stem cell and solid organ transplantation. To estimate the allogeneic potential between HLA-mismatched stem cell donor/recipient pairs, we recently proposed a matching score (dissimilarity index) that is based on the structural data of HLA class I molecules, and on the functional similarity of amino acids (AA). This first approach revealed new features about presumptive subtype allogenicities within the HLA-A*23 and A*24 groups. We have now developed an internet-based software tool ("HistoCheck") that is capable to assess the allogenicity (matching score) between any pair of clinically relevant HLA class I, and also class II, alleles. Newly described HLA sequences will be regularly integrated into the database according to the nomenclature for factors of the HLA system updates. The software is intended to be a first step for estimating the allogenicity of HLA mismatches in peculiar clinical settings, as long as there are no reliable in vitro or clinical studies available. The algorithm can later be modified according to functional data, for example, peptide-binding specificities. With the extension of the sequence similarity concept to all clinically relevant HLA class I and II loci, HistoCheck may contribute to prevent HLA mismatching being a matter of chance.
机译:HLA多态性是造血干细胞和实体器官移植的主要障碍。为了估计HLA不匹配的干细胞供体/受体对之间的同种异体潜力,我们最近提出了一个匹配分数(相异指数),该分数基于HLA I类分子的结构数据以及氨基酸(AA)的功能相似性。第一种方法揭示了HLA-A * 23和A * 24组中有关亚型同种异体性的新特征。现在,我们已经开发了一种基于互联网的软件工具(“ HistoCheck”),该工具能够评估任何一对临床相关的HLA I类和II类等位基因之间的同种异体性(匹配评分)。新描述的HLA序列将根据HLA系统更新因素的命名规则地定期集成到数据库中。只要没有可靠的体外或临床研究,该软件即可用作估算HLA错配在特定临床环境中异基因性的第一步。以后可以根据功能数据(例如肽结合特异性)修改算法。随着将序列相似性概念扩展到所有临床相关的I类和II类HLA基因座,HistoCheck可能有助于防止HLA错配。

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