首页> 美国卫生研究院文献>Proceedings of the National Academy of Sciences of the United States of America >Conformational variants of class II MHC/peptide complexes induced by N- and C-terminal extensions of minimal peptide epitopes
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Conformational variants of class II MHC/peptide complexes induced by N- and C-terminal extensions of minimal peptide epitopes

机译:II型MHC /肽复合物的构象变体,由最小肽表位的N-和C-末端延伸诱导

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摘要

Class II MHC molecules are known to exist in conformational variants. “Floppy” and “compact” forms of murine MHC molecules, for example, are discriminated by their migration behavior on SDS/PAGE and represent empty and ligand-loaded forms. Here we show that formation of distinctly faster-migrating ligand complexes (F-forms) rather than the normal compact (C-) forms of HLA-DR1 or -DR4 results from extensions of minimal peptide epitopes (such as HA306-318 or IC106-120) by ≈10 amino acids at either the N or the C terminus. Two similar but distinct F-forms (FI and FII) were detected, depending on the site of the extension. Both F-forms were characterized by increased surface hydrophobicity and reduced SDS-stability. Native gel separations and size exclusion chromatography indicated that the F-forms had increased hydrodynamic radii compared with the C-form and an apparent size similar to that of empty MHC molecules. The regions on the ligand overhangs responsible for the effect began at a distance of ≈5 amino acids on either side of the epitopes, comprised 4–8 amino acids (i.e., a total overhang of 9–14), and did not have a particular sequence preference. The possible functional significance of these forms is discussed.
机译:已知II类MHC分子以构象变体存在。例如,鼠类MHC分子的“松散”和“紧凑”形式通过它们在SDS / PAGE上的迁移行为来区分,代表空载和配体装载形式。在这里,我们显示了HLA-DR1或-DR4的明显较快迁移的配体复合物(F-形式)而不是正常紧致(C-)形式的形成是由于最小肽表位(如HA306-318或IC106- 120)在N或C末端加上≈10个氨基酸。根据扩展位点,检测到两个相似但截然不同的F形式(FI和FII)。两种F-形式的特征均在于增加的表面疏水性和降低的SDS稳定性。天然凝胶分离和尺寸排阻色谱法表明,与C型相比,F型具有增加的流体动力学半径,其表观大小与空MHC分子相似。配体突出端负责该作用的区域始于表位两侧约5个氨基酸的距离,包含4-8个氨基酸(即总突出9-14个),并且没有特定的顺序偏好。讨论了这些形式的可能的功能意义。

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