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A Novel Family of Human Leukocyte Antigen Class II Receptors May Have Its Origin in Archaic Human Species

机译:人类白细胞抗原II类受体的新型家族可能起源于古老的人类物种

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摘要

HLA class II α and β chains form receptors for antigen presentation to CD4+ T cells. Numerous pairings of class II α and β subunits from the wide range of haplotypes and isotypes may form, but most of these combinations, in particular those produced by isotype mixing, yielded mismatched dimers. It is unclear how selection of functional receptors is achieved. At the atomic level, it is not known which interactions of class II residues regulate selection of matched αβ heterodimers and the evolutionary origin of matched isotype mixed dimer formation. In this study we investigated assembly of isotype-mixed HLA class II α and β heterodimers. Assembly and carbohydrate maturation of various HLA-class II isotype-mixed α and β subunits was dependent on the groove binding section of the invariant chain (Ii). By mutation of polymorphic DPβ sequences, we identified two motifs, Lys-69 and GGPM-(84–87), that are engaged in Ii-dependent assembly of DPβ with DRα. We identified five members of a family of DPβ chains containing Lys-69 and GGPM 84–87, which assemble with DRα. The Lys/GGPM motif is present in the DPβ sequence of the Neanderthal genome, and this ancient sequence is related to the human allele DPB1*0401. By site-directed mutagenesis, we inspected Neanderthal amino acid residues that differ from the DPB1*0401 allele and aimed to determine whether matched heterodimers are formed by assembly of DPβ mutants with DRα. Because the *0401 allele is rare in the sub-Saharan population but frequent in the European population, it may have arisen in modern humans by admixture with Neanderthals in Europe.
机译:HLA II类Hα和β链形成抗原呈递给CD4 + T细胞的受体。可以形成来自广泛单倍型和同种型的II类α和β亚基的许多配对,但是这些组合中的大多数,特别是通过同种型混合产生的那些,产生不匹配的二聚体。尚不清楚如何实现功能受体的选择。在原子水平上,尚不清楚II类残基的哪些相互作用调节匹配的αβ异二聚体的选择和匹配的同型混合二聚体形成的进化起源。在这项研究中,我们研究了同种型混合HLA II类α和β异二聚体的组装。各种HLA II类同型混合的α和β亚基的组装和碳水化合物成熟取决于不变链(Ii)的凹槽结合部分。通过多态DPβ序列的突变,我们确定了两个基序Lys-69和GGPM-(84-87),它们与DPα与DRα的Ii依赖组装有关。我们鉴定了包含Lys-69和GGPM 84-87的DPβ链家族的五个成员,它们与DRα组装在一起。 Lys / GGPM基序存在于尼安德特人基因组的DPβ序列中,该古老序列与人等位基因DPB1 * 0401相关。通过定点诱变,我们检查了与DPB1 * 0401等位基因不同的尼安德特人氨基酸残基,旨在确定是否通过将DPβ突变体与DRα组装而形成匹配的异二聚体。因为* 0401等位基因在撒哈拉以南地区很少见,但在欧洲人群中很常见,因此它可能是在欧洲通过与尼安德特人混合而在现代人类中出现的。

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