gp130细胞因子结合区域的晶体结构
Crystal structure of a cytokine-binding region of gp130.
作者信息
Bravo J, Staunton D, Heath J K, Jones E Y
机构信息
Laboratory of Molecular Biophysics, The Rex Richards Building, South Parks Road, Oxford OX1 3QU.
出版信息
EMBO J. 1998 Mar 16;17(6):1665-74. doi: 10.1093/emboj/17.6.1665.
Abstract
The structure of the cytokine-binding homology region of the cell surface receptor gp130 has been determined by X-ray crystallography at 2.0 A resolution. The beta sandwich structure of the two domains conforms to the topology of the cytokine receptor superfamily. This first structure of an uncomplexed receptor exhibits a similar L-shaped quaternary structure to that of ligand-bound family members and suggests a limited flexibility in relative domain orientation of some 3 degrees. The putative ligand-binding loops are relatively rigid, with a phenylalanine side chain similarly positioned to exposed aromatic residues implicated in ligand binding for other such receptors. The positioning and structure of the N-terminal portion of the polypeptide chain have implications for the structure and function of cytokine receptors, such as gp130, which contain an additional N-terminal immunoglobulin-like domain.
摘要
细胞表面受体gp130的细胞因子结合同源区结构已通过X射线晶体学在2.0埃分辨率下确定。两个结构域的β折叠结构符合细胞因子受体超家族的拓扑结构。这种未结合配体的受体的首个结构展现出与结合配体的家族成员相似的L形四级结构,并表明相对结构域取向存在约3度的有限灵活性。推定的配体结合环相对刚性,苯丙氨酸侧链的位置类似于其他此类受体中与配体结合有关的暴露芳香族残基。多肽链N端部分的定位和结构对细胞因子受体(如含有额外N端免疫球蛋白样结构域的gp130)的结构和功能具有影响。
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