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Role of the 14-3-3 C-Terminal Region in the Interaction with the Plasma Membrane H+-ATPase

机译:14-3-3 C末端区域在与质膜H + -ATPase相互作用中的作用

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摘要

The 14-3-3 proteins are a family of proteins present in a number of isoforms in all eukaryotes and involved in the control of many cellular functions. Regulation of different activities is achieved by binding to phosphorylated targets through a conserved mechanism. Although in many systems isoform specificity has been demonstrated, the underlying molecular basis is still unclear. The sequences of 14-3-3 isoforms are highly conserved, divergence occurring at the N- and C-terminal regions. Recently it has been suggested that the C-terminal domain of 14-3-3 may regulate protein binding to the targets. Here we study the role of the C-terminal region of maize isoform GF14-6 in the interaction with the plant plasma membrane H+-ATPase. Results obtained demonstrate that removal of the last 22 amino acids residues of GF14-6 increases binding to H+-ATPase and stimulation of its activity. C-terminal deletion, moreover, reduces 14-3-3 sensitivity to cations. We also show that a peptide reproducing the GF14-6 C-terminus is able to bind to the C-terminal domain of H+-ATPase and to stimulate the enzyme activity. The implications of these findings for a integrated model of 14-3-3 interaction with H+-ATPase are discussed.
机译:14-3-3蛋白是蛋白质家族,存在于所有真核生物的许多同工型中,并参与许多细胞功能的控制。通过保守机制结合磷酸化的靶标来实现对不同活性的调节。尽管已在许多系统中证实了同工型特异性,但尚不清楚潜在的分子基础。 14-3-3同工型的序列高度保守,在N端和C端区域发散。最近,有人提出14-3-3的C末端结构域可调节蛋白质与靶标的结合。在此我们研究了玉米同工型GF14-6的C末端区域在与植物质膜H + -ATPase相互作用中的作用。获得的结果表明,去除GF14-6的最后22个氨基酸残基增加了与H + -ATPase的结合并刺激了其活性。此外,C末端缺失会降低14-3-3对阳离子的敏感性。我们还表明,能够复制GF14-6 C端的肽能够与H + -ATPase的C端结构域结合并刺激该酶的活性。讨论了这些发现对于与H + -ATPase相互作用的14-3-3集成模型的意义。

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