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Activation of PDE10 and PDE11 Phosphodiesterases

机译:PDE10和PDE11磷酸二酯酶的激活

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摘要

The most recently identified cyclic nucleotide phosphodiesterases, PDE10 and PDE11, contain a tandem of so-called GAF domains in their N-terminal regulatory regions. In PDE2 and PDE5, the GAF domains mediate cGMP stimulation; however, their function in PDE10 and PDE11 remains controversial. Although the GAF domains of PDE10 mediate cAMP-induced stimulation of chimeric adenylyl cyclases, cAMP binding did not stimulate the PDE10 holoenzyme. Comparable data about cGMP and the PDE11 GAF domains exist. Here, we identified synthetic ligands for the GAF domains of PDE10 and PDE11 to reduce interference of the GAF ligand with the catalytic reaction of PDE. With these ligands, GAF-mediated stimulation of the PDE10 and PDE11 holoenzymes is demonstrated for the first time. Furthermore, PDE10 is shown to be activated by cAMP, which paradoxically results in potent competitive inhibition of cGMP turnover by cAMP. PDE11, albeit susceptible to GAF-dependent stimulation, is not activated by the native cyclic nucleotides cAMP and cGMP. In summary, PDE11 can be stimulated by GAF domain ligands, but its native ligand remains to be identified, and PDE10 is the only PDE activated by cAMP.
机译:最近鉴定出的环状核苷酸磷酸二酯酶PDE10和PDE11在其N端调节区中包含一串所谓的GAF域。在PDE2和PDE5中,GAF域介导cGMP刺激。但是,它们在PDE10和PDE11中的功能仍存在争议。尽管PDE10的GAF域介导了cAMP诱导的嵌合腺苷酸环化酶的刺激,但是cAMP结合并没有刺激PDE10的全酶。存在有关cGMP和PDE11 GAF域的可比较数据。在这里,我们确定了PDE10和PDE11的GAF域的合成配体,以减少GAF配体对PDE催化反应的干扰。利用这些配体,首次证明了GAF介导的PDE10和PDE11全酶的刺激。此外,显示PDE10被cAMP激活,这自相矛盾地导致cAMP有效竞争性抑制cGMP周转。 PDE11尽管容易受到GAF依赖的刺激,但并未被天然环状核苷酸cAMP和cGMP激活。总之,PDE11可以被GAF域配体刺激,但其天然配体仍有待确定,PDE10是cAMP激活的唯一PDE。

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