首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >A point mutation in the groove of HLA-DO allows egress from the endoplasmic reticulum independent of HLA-DM
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A point mutation in the groove of HLA-DO allows egress from the endoplasmic reticulum independent of HLA-DM

机译:HLA-DO凹槽中的点突变允许从内质网脱离HLA-DM

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摘要

B lymphocytes express the nonclassical class Ⅱ molecule HLA-DO, which modulates the peptide loading activity of HLA-DM in the endocytic pathway. Binding to HLA-DM is required for HLA-DO to egress from the endoplasmic reticulum (ER). To gain insights into the mode of action of DO and on the role of DM in ER release, we sought to identify DM-binding residues on DO. Our results show that DOα encompasses the binding site for HLA-DM. More specifically, mutation of residue DOα41 on an exposed lateral loop of the α1 domain affects the binding to DM, ER egress, and activity of DO. Using a series of chimeric DR/DO molecules, we confirmed the role of the α chain and established that a second DM-binding region is located C-terminal to the DOα80 residue, most probably in the α2 domain. Interestingly, after mutation of a buried proline (α11) on the floor of the putative peptide-binding groove, HLA-DO remained functional but became independent of HLA-DM for ER egress and intracellular trafficking. Collectively, these results suggest that the binding of HLA-DM to DOα allows the complex to egress from the ER by stabilizing intramolecular contacts between the N-terminal antiparallel β-strands of the DOαβ heterodimer.
机译:B淋巴细胞表达非经典的Ⅱ类分子HLA-DO,它调节内吞途径中HLA-DM的肽负载活性。 HLA-DO从内质网(ER)流出需要与HLA-DM结合。为了深入了解DO的作用方式以及DM在ER释放中的作用,我们寻求鉴定DO上的DM结合残基。我们的结果表明,DOα包含HLA-DM的结合位点。更具体地,在α1结构域的暴露的侧向环上的残基DOα41的突变影响与DM的结合,ER出口和DO的活性。使用一系列嵌合DR / DO分子,我们确认了α链的作用,并确定了第二个DM结合区位于DOα80残基的C端,最有可能在α2结构域中。有趣的是,在假定的肽结合槽底上的掩埋脯氨酸(α11)发生突变后,HLA-DO仍保持功能,但变得独立于HLA-DM用于内质网出口和细胞内运输。总的来说,这些结果表明HLA-DM与DOα的结合通过稳定DOαβ异二聚体的N端反平行β链之间的分子内接触而使复合物从ER中释放出来。

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