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通过配体与E3连接酶信号效应因子DWARF3的结合使独脚金内酯受体DWARF14不稳定。

Destabilization of strigolactone receptor DWARF14 by binding of ligand and E3-ligase signaling effector DWARF3.

作者信息

Zhao Li-Hua, Zhou X Edward, Yi Wei, Wu Zhongshan, Liu Yue, Kang Yanyong, Hou Li, de Waal Parker W, Li Suling, Jiang Yi, Scaffidi Adrian, Flematti Gavin R, Smith Steven M, Lam Vinh Q, Griffin Patrick R, Wang Yonghong, Li Jiayang, Melcher Karsten, Xu H Eric

机构信息

VARI-SIMM Center, Center for Structure and Function of Drug Targets, Key Laboratory of Receptor Research, Shanghai Institute of Materia Medica, Chinese Academy of Sciences, Shanghai 201203, China.

The Institute of Biomedical Sciences and School of Life Sciences, East China Normal University, Shanghai 200241, China.

出版信息

Cell Res. 2015 Nov;25(11):1219-36. doi: 10.1038/cr.2015.122. Epub 2015 Oct 16.

Abstract

Strigolactones (SLs) are endogenous hormones and exuded signaling molecules in plant responses to low levels of mineral nutrients. Key mediators of the SL signaling pathway in rice include the α/β-fold hydrolase DWARF 14 (D14) and the F-box component DWARF 3 (D3) of the ubiquitin ligase SCF(D3) that mediate ligand-dependent degradation of downstream signaling repressors. One perplexing feature is that D14 not only functions as the SL receptor but is also an active enzyme that slowly hydrolyzes diverse natural and synthetic SLs including GR24, preventing the crystallization of a binary complex of D14 with an intact SL as well as the ternary D14/SL/D3 complex. Here we overcome these barriers to derive a structural model of D14 bound to intact GR24 and identify the interface that is required for GR24-mediated D14-D3 interaction. The mode of GR24-mediated signaling, including ligand recognition, hydrolysis by D14, and ligand-mediated D14-D3 interaction, is conserved in structurally diverse SLs. More importantly, D14 is destabilized upon the binding of ligands and D3, thus revealing an unusual mechanism of SL recognition and signaling, in which the hormone, the receptor, and the downstream effectors are systematically destabilized during the signal transduction process.

摘要

独脚金内酯(SLs)是植物在应对低水平矿质营养时分泌的内源性激素和信号分子。水稻中SL信号通路的关键介质包括α/β折叠水解酶DWARF 14(D14)和泛素连接酶SCF(D3)的F-box组分DWARF 3(D3),它们介导下游信号抑制因子的配体依赖性降解。一个令人困惑的特征是,D14不仅作为SL受体发挥作用,还是一种活性酶,能缓慢水解包括GR24在内的多种天然和合成SLs,从而阻止D14与完整SL形成二元复合物以及D14/SL/D3三元复合物的结晶。在这里,我们克服了这些障碍,得出了与完整GR24结合的D14的结构模型,并确定了GR24介导的D14 - D3相互作用所需的界面。GR24介导的信号传导模式,包括配体识别、D14水解以及配体介导的D14 - D3相互作用,在结构多样的SLs中是保守的。更重要的是,D14在配体和D3结合后会变得不稳定,从而揭示了一种不同寻常的SL识别和信号传导机制,即在信号转导过程中,激素、受体和下游效应器会系统性地变得不稳定。

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