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Evidence for Intermolecular Interactions between the Intracellular Domains of the Arabidopsis Receptor-Like Kinase ACR4 Its Homologs and the Wox5 Transcription Factor

机译:拟南芥受体激酶激酶ACR4其同源物和Wox5转录因子的胞内域之间的分子间相互作用的证据。

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摘要

Arabidopsis CRINKLY4 (ACR4) is a receptor-like kinase (RLK) involved in the global development of the plant. The Arabidopsis genome encodes four homologs of ACR4 that contain sequence similarity and analogous architectural elements to ACR4, termed Arabidopsis CRINKLY4 Related (AtCRRs) proteins. Additionally, a signaling module has been previously proposed including a postulated peptide ligand, CLE40, the ACR4 RLK, and the WOX5 transcription factor that engage in a possible feedback mechanism controlling stem cell differentiation. However, little biochemical evidence is available to ascertain the molecular aspects of receptor heterodimerization and the role of phosphorylation in these interactions. Therefore, we have undertaken an investigation of the in vitro interactions between the intracellular domains (ICD) of ACR4, the CRRs and WOX5. We demonstrate that interaction can occur between ACR4 and all four CRRs in the unphosphorylated state. However, phosphorylation dependency is observed for the interaction between ACR4 and CRR3. Furthermore, sequence analysis of the ACR4 gene family has revealed a conserved ‘KDSAF’ motif that may be involved in protein-protein interactions among the receptor family. We demonstrate that peptides harboring this conserved motif in CRR3 and CRK1are able to bind to the ACR4 kinase domain. Our investigations also indicate that the ACR4 ICD can interact with and phosphorylate the transcription factor WOX5.
机译:拟南芥CRINKLY4(ACR4)是一种参与受体的类激酶(RLK),参与植物的全球发展。拟南芥基因组编码ACR4的四个同源物,它们与ACR4包含序列相似性和相似的结构元件,称为拟南芥CRINKLY4相关(AtCRRs)蛋白。另外,先前已经提出了信号传导模块,包括假定的肽配体,CLE40,ACR4 RLK和WOX5转录因子,它们参与控制干细胞分化的可能反馈机制。但是,很少有生化证据可用于确定受体异二聚化的分子方面以及这些相互作用中磷酸化的作用。因此,我们进行了ACR4,CRR和WOX5的胞内域(ICD)之间的体外相互作用的研究。我们证明了相互作用可以发生在ACR4和所有四个CRR在未磷酸化状态之间。但是,ACR4和CRR3之间的相互作用观察到磷酸化依赖性。此外,对ACR4基因家族的序列分析表明,保守的“ KDSAF”基序可能与受体家族之间的蛋白质-蛋白质相互作用有关。我们证明,在CRR3和CRK1中具有这种保守基序的肽能够与ACR4激酶域结合。我们的研究还表明,ACR4 ICD可以与转录因子WOX5相互作用并使其磷酸化。

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