Catipović B, Talluri G, Oh J, Wei T, Su X M, Johansen T E, Edidin M, Schneck J P
Department of Medicine, Johns Hopkins School of Medicine, Baltimore, Maryland 21224.
J Exp Med. 1994 Nov 1;180(5):1753-61. doi: 10.1084/jem.180.5.1753.
We compared the conformation of empty and peptide-loaded class I major histocompatibility complex (MHC) molecules at the cell surface. Molecular conformations were analyzed by fluorescence resonance energy transfer (FRET) between fluorescent-labeled Fab fragments bound to the alpha 2 domain of the MHC heavy chain and fluorescent-labeled Fab fragments bound to beta 2-microglobulin. No FRET was found between Fab fragments bound to empty H-2Kb, but FRET was detected when empty H-2Kb molecules were loaded with peptide. The magnitude of FRET depended on the sequence of the peptide used. The results imply that empty H-2Kb molecules are in a relatively extended conformation, and that this conformation becomes more compact when peptide is bound. These changes, which are reflected in peptide-dependent binding of monoclonal antibodies, affect the surfaces of MHC molecules available for contact with T cell receptors and hence may influence T cell-receptor recognition of MHC molecules.
我们比较了细胞表面空载和负载肽的I类主要组织相容性复合体(MHC)分子的构象。通过荧光共振能量转移(FRET)分析分子构象,该能量转移发生在与MHC重链α2结构域结合的荧光标记Fab片段和与β2-微球蛋白结合的荧光标记Fab片段之间。在与空载H-2Kb结合的Fab片段之间未发现FRET,但当空载H-2Kb分子负载肽时检测到了FRET。FRET的大小取决于所用肽的序列。结果表明,空载H-2Kb分子处于相对伸展的构象,当结合肽时,这种构象会变得更加紧凑。这些变化反映在单克隆抗体的肽依赖性结合中,影响了MHC分子可与T细胞受体接触的表面,因此可能影响T细胞受体对MHC分子的识别。
