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首页> 外文期刊>The journal of immunology >Tapasin Is a Facilitator, Not an Editor, of Class I MHC Peptide Binding
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Tapasin Is a Facilitator, Not an Editor, of Class I MHC Peptide Binding

机译:Tapasin是I类MHC肽结合的促进者,而不是编辑者

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Tapasin has been proposed to function as a peptide editor to displace lower affinity peptides and/or to favor the binding of high affinity peptides. Consistent with this, cell surface HLA-B8 molecules in tapasin-deficient cells were less stable and the peptide repertoire was substantially altered. However, the binding affinities of peptides expressed in the absence of tapasin were unexpectedly higher, not lower. The peptide repertoire from cells expressing soluble tapasin was similar in both appearance and affinity to that presented in the presence of full-length tapasin, but the HLA-B8 molecules showed altered cell surface stability characteristics. Similarly, the binding affinities of HLA-A*0201-associated peptides from tapasin+ and tapasin? cells were equivalent, although steady state HLA-A*0201 cell surface expression was decreased and the molecules demonstrated reduced cell surface stability on tapasin? cells. These data are inconsistent with a role for tapasin as a peptide editor. Instead, we propose that tapasin acts as a peptide facilitator. In this role, it stabilizes the peptide-free conformation of class I MHC molecules in the endoplasmic reticulum and thus increases the number and variety of peptides bound to class I MHC. Full-length tapasin then confers additional stability on class I MHC molecules that are already associated with peptides.
机译:已经提出Tapasin用作肽编辑器以取代较低亲和力的肽和/或有助于结合高亲和力的肽。与此相符的是,在缺乏胰蛋白酶的细胞中,细胞表面HLA-B8分子的稳定性较差,肽库也发生了实质性变化。然而,在没有塔帕森蛋白酶的情况下表达的肽的结合亲和力出乎意料地更高而不是更低。表达可溶性木瓜蛋白酶的细胞的肽库在外观和亲和力上均与存在全长木瓜蛋白酶的肽库相似,但是HLA-B8分子显示出改变的细胞表面稳定性特征。同样,来自塔帕森+和塔帕森β的HLA-A * 0201相关肽的结合亲和力。尽管稳态HLA-A * 0201细胞表面表达降低并且分子在塔帕森蛋白酶上显示出降低的细胞表面稳定性,但这些细胞是等效的。细胞。这些数据与Tapasin作为肽编辑器的作用不一致。取而代之的是,我们建议使用塔帕森蛋白酶作为肽的促进剂。在这种作用下,它稳定了内质网中I类MHC分子的无肽构象,从而增加了与I类MHC结合的肽的数量和种类。全长木薯蛋白酶然后赋予已经与肽结合的I类MHC分子额外的稳定性。

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