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The two GAF domains in phosphodiesterase 2A have distinct roles in dimerization and in cGMP binding

机译:磷酸二酯酶2A中的两个GAF域在二聚化和cGMP结合中具有不同的作用

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摘要

Cyclic nucleotide phosphodiesterases (PDEs) regulate all pathways that use cGMP or cAMP as a second messenger. Five of the 11 PDE families have regulatory segments containing GAF domains, 3 of which are known to bind cGMP. In PDE2 binding of cGMP to the GAF domain causes an activation of the catalytic activity by a mechanism that apparently is shared even in the adenylyl cyclase of Anabaena, an organism separated from mouse by 2 billion years of evolution. The 2.9-Å crystal structure of the mouse PDE2A regulatory segment reported in this paper reveals that the GAF A domain functions as a dimerization locus. The GAF B domain shows a deeply buried cGMP displaying a new cGMP-binding motif and is the first atomic structure of a physiological cGMP receptor with bound cGMP. Moreover, this cGMP site is located well away from the region predicted by previous mutagenesis and structural genomic approaches.
机译:环核苷酸磷酸二酯酶(PDE)调节所有将cGMP或cAMP用作第二信使的途径。 11个PDE家族中有5个具有包含GAF域的调控片段,其中3个与cGMP结合。在PDE2中,cGMP与GAF结构域的结合通过一种机制引起催化活性的激活,该机制甚至在鱼腥藻的腺苷酸环化酶中也共有,而鱼腥藻是通过20亿年的进化与小鼠分离的生物。本文报道的小鼠PDE2A调控片段的2.9-Å晶体结构表明,GAFA区域起着二聚化作用。 GAF B结构域显示了一个深埋的cGMP,该cGMP显示了新的cGMP结合基序,并且是具有绑定cGMP的生理cGMP受体的第一个原子结构。而且,该cGMP位点位于远离先前诱变和结构基因组学方法预测的区域的位置。

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