首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Functionality of major histocompatibility complex class II molecules in mice doubly deficient for invariant chain and H-2M complexes
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Functionality of major histocompatibility complex class II molecules in mice doubly deficient for invariant chain and H-2M complexes

机译:主要组织相容性复合物II类分子在小鼠中恒定链和H-2M复合物双重缺乏的功能

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摘要

By combining two previously generated null mutations, Ii° and M°, we produced mice lacking the invariant chain and H-2M complexes, both required for normal cell-surface expression of major histocompatibility complex class II molecules loaded with the usual diverse array of peptides. As expected, the maturation and transport of class II molecules, their expression at the cell surface, and their capacity to present antigens were quite similar for cells from Ii°M° double-mutant mice and from animals carrying just the Ii° mutation. More surprising were certain features of the CD4+ T cell repertoire selected in Ii°M° mice: many fewer cells were selected than in Ii+M° animals, and these had been purged of self-reactive specificities, unlike their counterparts in Ii+M° animals. These findings suggest (i) that the peptides carried by class II molecules on stromal cells lacking H-2M complexes may almost all derive from invariant chain and (ii) that H-2M complexes edit the peptide array displayed on thymic stromal cells in the absence of invariant chain, showing that it can edit, in vivo, peptides other than CLIP.
机译:通过组合两个先前产生的无效突变Ii°和M°,我们产生了缺少恒定链和H-2M复合体的小鼠,这两个结构都是主要的组织相容性复合体II类分子的正常细胞表面表达所必需的,这些分子装载了通常的各种肽阵列。正如预期的那样,II型分子的成熟和运输,它们在细胞表面的表达以及它们呈递抗原的能力对于来自IiM双重突变小鼠和仅携带Ii°突变的动物的细胞非常相似。在Ii°M°小鼠中选择的CD4 + T细胞库的某些特征更加令人惊讶:与Ii + M°动物相比,选择的细胞要少得多,与Ii + M°动物中的同类动物不同,它被清除了自我反应性特异性。这些发现表明:(i)II类分子在缺乏H-2M复合物的基质细胞上携带的肽可能几乎全部来自不变链;(ii)在没有胸腺基质细胞的情况下,H-2M复合物可编辑肽阵列恒定链的结构,表明它可以在体内编辑CLIP以外的其他肽。

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