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人肌联蛋白- obscurin 复合物的晶体结构揭示了一个保守而特异的肌节 M 带拉链模块。

The crystal structure of the human titin:obscurin complex reveals a conserved yet specific muscle M-band zipper module.

机构信息

Randall Division of Cell and Molecular Biophysics, King's College London, New Hunt's House, Guy's Campus, London SE1 1UL, UK.

Randall Division of Cell and Molecular Biophysics, King's College London, New Hunt's House, Guy's Campus, London SE1 1UL, UK; Cardiovascular Division, King's College London, New Hunt's House, Guy's Campus, London SE1 1UL, UK.

出版信息

J Mol Biol. 2015 Feb 27;427(4):718-736. doi: 10.1016/j.jmb.2014.11.019. Epub 2014 Dec 6.

DOI:10.1016/j.jmb.2014.11.019
PMID:25490259
Abstract

M10 is the most C-terminal immunoglobulin (Ig) domain of the giant protein titin and a frequent target of disease-linked mutations. Currently, it is the only known muscle Ig domain able to interact with two alternative ligands-obscurin and obscurin-like-1 (Obsl1)-in different sarcomeric subregions. Obscurin and Obsl1 use their homologous N-terminal Ig domain (O1 in obscurin and OL1 in Obsl1) to bind M10 in a mutually exclusive manner. We present here the X-ray structure of the human titin:obscurin M10:O1 complex extending our previous work on the M10:OL1 interaction. Similar to M10:OL1, the M10:O1 complex displays a chevron-shaped antiparallel Ig-Ig architecture held together by a conserved molecular interface, which we validated by isothermal titration calorimetry and sorting experiments in neonatal rat cardiomyocytes. O1, although structurally related to OL1 and M10, both members of the intermediate set (I-set) Ig family, presents an intriguing switch of its βA' strand. This leads to structural differences between the complexes, particularly for the "open side" of the chevron-shaped assembly. A bioinformatics analysis reveals that the βA'-switch observed for O1 is rare and that it is involved in mediating protein-protein interactions. Molecular dynamics simulations also suggest that this topological alteration substantially increases local flexibility compared to the conventional I-set Ig domains. The O1/OL1 Ig domains are candidate discriminatory structural modules potentially directing the binding of specific additional partners at the M-band. Cellular sorting experiments in neonatal rat cardiomyocytes are consistent with the view that the titin:obscurin/Obsl1 complexes might be a platform for higher-order interactions.

摘要

M10 是巨大蛋白肌联蛋白的最 C 端免疫球蛋白(Ig)结构域,也是疾病相关突变的常见靶点。目前,它是唯一已知的能够在不同肌节亚区与两种替代配体—— obscurin 和 obscurin-like-1(Obsl1)相互作用的肌肉 Ig 结构域。 obscurin 和 Obsl1 分别使用其同源的 N 端 Ig 结构域(obscurin 中的 O1 和 Obsl1 中的 OL1)以相互排斥的方式与 M10 结合。我们在此展示了人肌联蛋白: obscurin M10:O1 复合物的 X 射线结构,扩展了我们之前关于 M10:OL1 相互作用的工作。与 M10:OL1 类似,M10:O1 复合物呈现出一种 Chevron 形的反平行 Ig-Ig 结构,由保守的分子界面结合在一起,我们通过等温滴定量热法和新生大鼠心肌细胞的分选实验验证了这一点。尽管 O1 在结构上与 OL1 和 M10 相关,均属于中间集合(I-set)Ig 家族的成员,但它的βA'链发生了有趣的转换。这导致了复合物之间的结构差异,特别是 Chevron 形组装的“开口侧”。生物信息学分析表明,观察到的 O1 的βA'-转换很少见,并且它参与了蛋白质-蛋白质相互作用的介导。分子动力学模拟还表明,与传统的 I-set Ig 结构域相比,这种拓扑变化会大大增加局部灵活性。O1/OL1 Ig 结构域是潜在的有区别的结构模块,可能指导特定的附加配体在 M 带上的结合。新生大鼠心肌细胞的分选实验与肌联蛋白: obscurin/Obsl1 复合物可能是更高阶相互作用的平台的观点一致。

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