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Differential CLE peptide perception by plant receptors implicated from structural and functional analyses of TDIF-TDR interactions

机译:TDIF-TDR相互作用的结构和功能分析牵连植物受体对CLE肽的感知差异

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摘要

Tracheary Element Differentiation Inhibitory Factor (TDIF) belongs to the family of post-translationally modified CLE (CLAVATA3/embryo surrounding region (ESR)-related) peptide hormones that control root growth and define the delicate balance between stem cell proliferation and differentiation in SAM (shoot apical meristem) or RAM (root apical meristem). In Arabidopsis, Tracheary Element Differentiation Inhibitory Factor Receptor (TDR) and its ligand TDIF signaling pathway is involved in the regulation of procambial cell proliferation and inhibiting its differentiation into xylem cells. Here we present the crystal structures of the extracellular domains (ECD) of TDR alone and in complex with its ligand TDIF resolved at 2.65 Ǻ and 2.75 Ǻ respectively. These structures provide insights about the ligand perception and specific interactions between the CLE peptides and their cognate receptors. Our in vitro biochemical studies indicate that the interactions between the ligands and the receptors at the C-terminal anchoring site provide conserved binding. While the binding interactions occurring at the N-terminal anchoring site dictate differential binding specificities between different ligands and receptors. Our studies will open different unknown avenues of TDR-TDIF signaling pathways that will enhance our knowledge in this field highlighting the receptor ligand interaction, receptor activation, signaling network, modes of action and will serve as a structure function relationship model between the ligand and the receptor for various similar leucine-rich repeat receptor-like kinases (LRR-RLKs).
机译:气管元素分化抑制因子(TDIF)属于翻译后修饰的CLE(CLAVATA3 /胚胎周围区域(ESR)相关)肽激素家族,其控制根的生长并定义SAM中干细胞增殖与分化之间的微妙平衡(根尖分生组织)或RAM(根尖分生组织)。在拟南芥中,气管元件分化抑制因子受体(TDR)及其配体TDIF信号传导途径参与了原细菌细胞增殖的调节并抑制了其分化为木质部细胞的过程。在这里,我们介绍了TDR的细胞外结构域(ECD)的晶体结构,以及其配体TDIF的复合结构,分别在2.65Ǻ和2.75 resolved分辨。这些结构提供了有关配体感知以及CLE肽与其同源受体之间特异性相互作用的见解。我们的体外生化研究表明,配体与C末端锚定位点的受体之间的相互作用提供了保守的结合。虽然在N末端锚定位点发生的结合相互作用决定了不同配体和受体之间的差异结合特异性。我们的研究将开辟TDR-TDIF信号传导途径的不同未知途径,这些途径将增强我们在该领域的知识,突出受体配体相互作用,受体激活,信号网络,作用方式,并作为配体与受体之间的结构功能关系模型。各种类似的富含亮氨酸的重复受体样激酶(LRR-RLK)的受体。

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