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兼职鸟苷酸环化酶的比较:在信号传导方向中的作用?

Comparison of moonlighting guanylate cyclases: roles in signal direction?

作者信息

Freihat Lubna, Muleya Victor, Manallack David T, Wheeler Janet I, Irving Helen R

机构信息

*Monash Institute of Pharmaceutical Sciences, Monash University, 381 Royal Parade, Parkville, VIC 3052, Australia.

出版信息

Biochem Soc Trans. 2014 Dec;42(6):1773-9. doi: 10.1042/BST20140223.

DOI:10.1042/BST20140223
PMID:25399605
Abstract

Over 30 receptor-like kinases contain a guanylate cyclase (GC) catalytic centre embedded within the C-terminal region of their kinase domain in the model plant Arabidopsis. A number of the kinase GCs contain both functional kinase and GC activity in vitro and the natural ligands of these receptors stimulate increases in cGMP within isolated protoplasts. The GC activity could be described as a minor or moonlighting activity. We have also identified mammalian proteins that contain the novel GC centre embedded within kinase domains. One example is the interleukin 1 receptor-associated kinase 3 (IRAK3). We compare the GC functionality of the mammalian protein IRAK3 with the cytoplasmic domain of the plant prototype molecule, the phytosulfokine receptor 1 (PSKR1). We have developed homology models of these molecules and have undertaken in vitro experiments to compare their functionality and structural features. Recombinant IRAK3 produces cGMP at levels comparable to those produced by PSKR1, suggesting that IRAK3 contains GC activity. Our findings raise the possibility that kinase-GCs may switch between downstream kinase-mediated or cGMP-mediated signalling cascades to elicit desired outputs to particular stimuli. The challenge now lies in understanding the interaction between the GC and kinase domains and how these molecules utilize their dual functionality within cells.

摘要

在模式植物拟南芥中,超过30种类受体激酶在其激酶结构域的C端区域含有一个鸟苷酸环化酶(GC)催化中心。许多激酶GC在体外同时具有功能性激酶和GC活性,并且这些受体的天然配体可刺激分离原生质体内cGMP的增加。GC活性可被描述为一种次要或兼职活性。我们还鉴定出了在激酶结构域中含有新型GC中心的哺乳动物蛋白。一个例子是白细胞介素1受体相关激酶3(IRAK3)。我们将哺乳动物蛋白IRAK3的GC功能与植物原型分子植物硫肽激素受体1(PSKR1)的胞质结构域进行了比较。我们构建了这些分子的同源模型,并进行了体外实验以比较它们的功能和结构特征。重组IRAK3产生cGMP的水平与PSKR1相当,这表明IRAK3具有GC活性。我们的研究结果增加了激酶 - GC可能在下游激酶介导或cGMP介导的信号级联反应之间切换,以引发对特定刺激的期望输出的可能性。现在的挑战在于理解GC和激酶结构域之间的相互作用,以及这些分子如何在细胞内利用其双重功能。

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