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粒细胞-巨噬细胞集落刺激因子、白细胞介素-3和白细胞介素-5受体共同β链细胞因子结合域的溶液结构。

The solution structure of the cytokine-binding domain of the common beta-chain of the receptors for granulocyte-macrophage colony-stimulating factor, interleukin-3 and interleukin-5.

作者信息

Mulhern T D, Lopez A F, D'Andrea R J, Gaunt C, Vandeleur L, Vadas M A, Booker G W, Bagley C J

机构信息

Department of Biochemistry, University of Adelaide, Adelaide, 5005, Australia.

出版信息

J Mol Biol. 2000 Apr 7;297(4):989-1001. doi: 10.1006/jmbi.2000.3610.

DOI:10.1006/jmbi.2000.3610
PMID:10736232
Abstract

The haemopoietic cytokines, granulocyte-macrophage colony-stimulating factor, interleukin-3 and interleukin-5 bind to cell-surface receptors comprising ligand-specific alpha-chains and a shared beta-chain. The beta-chain is the critical signalling subunit of the receptor and its fourth domain not only plays a critical role in interactions with ligands, hence in receptor activation, but also contains residues whose mutation can lead to ligand-independent activation of the receptor. We have determined the NMR solution structure of the isolated human fourth domain of the beta-chain. The protein has a fibronectin type III fold with a well-defined hydrophobic core and is stabilised by an extensive network of pi-cation interactions involving Trp and Arg side-chains, including two Trp residues outside the highly conserved Trp-Ser-Xaa-Trp-Ser motif (where Xaa is any amino acid) that is found in many cytokine receptors. Most of the residues implicated in factor-independent mutants localise to the rigid core of the domain or the pi-cation stack. The loops between the B and C, and the F and G strands, that contain residues important for interactions with cytokines, lie adjacent at the membrane-distal end of the domain, consistent with their being involved cooperatively in binding cytokines. The elucidation of the structure of the cytokine-binding domain of the beta-chain provides insight into the cytokine-dependent and factor-independent activation of the receptor.

摘要

造血细胞因子、粒细胞-巨噬细胞集落刺激因子、白细胞介素-3和白细胞介素-5与由配体特异性α链和共享β链组成的细胞表面受体结合。β链是受体的关键信号亚基,其第四结构域不仅在与配体的相互作用中起关键作用,从而在受体激活中起关键作用,而且还包含一些残基,其突变可导致受体的配体非依赖性激活。我们已经确定了β链分离的人第四结构域的核磁共振溶液结构。该蛋白质具有纤连蛋白III型折叠,具有明确的疏水核心,并通过涉及色氨酸和精氨酸侧链的广泛π-阳离子相互作用网络得以稳定,包括在许多细胞因子受体中发现的高度保守的色氨酸-丝氨酸-Xaa-色氨酸-丝氨酸基序(其中Xaa是任何氨基酸)之外的两个色氨酸残基。与因子非依赖性突变体相关的大多数残基定位于该结构域的刚性核心或π-阳离子堆积处。B和C以及F和G链之间的环,包含与细胞因子相互作用重要的残基,位于该结构域膜远端的相邻位置,这与其协同参与结合细胞因子一致。β链细胞因子结合结构域结构的阐明为受体的细胞因子依赖性和因子非依赖性激活提供了深入了解。

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