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Interaction of MHC class II molecules with the invariant chain: role of the invariant chain (81-90) region.

机译:MHC II类分子与不变链的相互作用:不变链(81-90)区的作用。

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摘要

Association of the invariant chain (Ii) with MHC class II alpha and beta chains is central for their functionality and involves the Ii CLIP(81-104) region. Ii mutants with an antigenic peptide sequence in place of the CLIP region are shown to form alphabetaIi complexes resistant to dissociation by SDS at 25 degrees C. This reflects class II peptide binding site occupancy, since substitution of the major anchor residue within the antigenic peptide sequence of one of these Ii mutants abolishes its capacity to form SDS-stable heterotrimers. Therefore, CLIP location within Ii is compatible with CLIP access to the class II binding groove. However, in wild-type Ii this access does not lead to a tight association, which seems to be affected by the Ii 81-90 region. This region, together with a region C-terminal of CLIP, is shown to contribute to Ii association with HLA-DR1 molecules. Thus, Ii mutants with non-HLA-DR1 binding sequences in place of the CLIP(87-102) region can still associate with HLA-DR1 molecules and inhibit peptide binding.
机译:恒定链(Ii)与II类MHCα和β链的关联对于它们的功能至关重要,并且涉及Ii CLIP(81-104)区域。显示具有抗原肽序列代替CLIP区的IIi突变体形成了对25°C的SDS分解具有抗性的字母复合物。这反映了II类肽结合位点的占有,因为抗原肽序列中主要锚定残基的取代这些IIi突变体之一的突变消除了其形成SDS稳定的异源三聚体的能力。因此,Ii中的CLIP位置与对II类绑定槽的CLIP访问兼容。但是,在野生型Ii中,这种接触不会导致紧密的关联,这似乎受到Ii 81-90区域的影响。该区域以及CLIP的C末端区域一起显示出与HLA-DR1分子的Ii缔合。因此,具有非HLA-DR1结合序列代替CLIP(87-102)区的IIi突变体仍可与HLA-DR1分子缔合并抑制肽结合。

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