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来自. 的脱落酸受体和共受体的组合相互作用网络。

Combinatorial interaction network of abscisic acid receptors and coreceptors from .

机构信息

Chair of Botany, TUM School of Life Sciences Weihenstephan, Technical University of Munich, D-85354 Freising, Germany.

Bavarian Center for Biomolecular Mass Spectrometry, TUM School of Life Sciences Weihenstephan, Technical University of Munich, D-85354 Freising, Germany.

出版信息

Proc Natl Acad Sci U S A. 2017 Sep 19;114(38):10280-10285. doi: 10.1073/pnas.1706593114. Epub 2017 Sep 5.

Abstract

The phytohormone abscisic acid (ABA) is induced in response to abiotic stress to mediate plant acclimation to environmental challenge. Key players of the ABA-signaling pathway are the ABA-binding receptors (RCAR/PYR1/PYL), which, together with a plant-specific subclade of protein phosphatase 2C (PP2C), form functional holoreceptors. The genome encodes nine PP2C coreceptors and 14 different RCARs, which can be divided into three subfamilies. The presence of these gene families in higher plants points to the existence of an intriguing regulatory network and poses questions as to the functional compatibility and specificity of receptor-coreceptor interactions. Here, we analyzed all RCAR-PP2C combinations for their capacity to regulate ABA signaling by transient expression in protoplasts. Of 126 possible RCAR-PP2C pairings, 113 were found to be functional. The three subfamilies within the RCAR family showed different sensitivities to regulating the ABA response at basal ABA levels when efficiently expressed. At exogenous high ABA levels, the RCARs regulated most PP2Cs and activated the ABA response to a similar extent. The PP2C AHG1 was regulated only by RCAR1/PYL9, RCAR2/PYL7, and RCAR3/PYL8, which are characterized by a unique tyrosine residue. Site-directed mutagenesis of RCAR1 showed that its tyrosine residue is critical for AHG1 interaction and regulation. Furthermore, the PP2Cs HAI1 to HAI3 were regulated by all RCARs, and the ABA receptor RCAR4/PYL10 showed ABA-dependent PP2C regulation. The findings unravel the interaction network of possible RCAR-PP2C pairings and their different potentials to serve a rheostat function for integrating fluctuating hormone levels into the ABA-response pathway.

摘要

植物激素脱落酸(ABA)在非生物胁迫下被诱导,以调节植物对环境挑战的适应。ABA 信号通路的关键参与者是 ABA 结合受体(RCAR/PYR1/PYL),它与植物特异性蛋白磷酸酶 2C (PP2C)的一个亚家族一起,形成功能完整的受体。基因组编码了九个 PP2C 核心受体和 14 种不同的 RCAR,可以分为三个亚家族。这些基因家族在高等植物中的存在表明存在一个引人入胜的调控网络,并提出了受体-核心受体相互作用的功能兼容性和特异性问题。在这里,我们通过原生质体瞬时表达分析了所有 RCAR-PP2C 组合调控 ABA 信号的能力。在 126 种可能的 RCAR-PP2C 配对中,发现 113 种具有功能。RCAR 家族中的三个亚家族在有效表达时,在基础 ABA 水平下对调节 ABA 反应的敏感性不同。在外源高 ABA 水平下,RCAR 调节大多数 PP2C 并以相似的程度激活 ABA 反应。RCAR1/PYL9、RCAR2/PYL7 和 RCAR3/PYL8 仅调节 PP2C AHG1,它们的特征是具有独特的酪氨酸残基。RCAR1 的定点突变表明,其酪氨酸残基对 AHG1 相互作用和调节至关重要。此外,所有 RCAR 都调节 PP2Cs HAI1 到 HAI3,ABA 受体 RCAR4/PYL10 显示出 ABA 依赖性的 PP2C 调节。这些发现揭示了可能的 RCAR-PP2C 配对的相互作用网络及其不同的潜力,以将波动的激素水平整合到 ABA 反应途径中。

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