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一种新型的细胞质 PSD-95 相互作用蛋白(Cypin)短异构体调节神经元发育。

A Novel Short Isoform of Cytosolic PSD-95 Interactor (Cypin) Regulates Neuronal Development.

机构信息

Department of Cell Biology and Neuroscience, Rutgers University (USA), 604 Allison Road, Piscataway, NJ, 08854-8082, USA.

Graduate Program in Neurosciences, Rutgers University (USA), New Brunswick, NJ, USA.

出版信息

Mol Neurobiol. 2018 Aug;55(8):6269-6281. doi: 10.1007/s12035-017-0849-z. Epub 2018 Jan 2.

Abstract

The guanine deaminase cypin (cytosolic PSD-95 interactor) binds to PSD-95 (postsynaptic density protein 95) and regulates dendrite branching by promoting microtubule polymerization. Here, we identify a novel short isoform of cypin, termed cypinS, which is expressed in mouse and human, but not rat, tissues. Cypin and cypinS mRNA and protein levels peak at P7 and P14 in the mouse brain, suggesting a role for these isoforms during development. Interestingly, although cypinS lacks guanine deaminase activity, overexpression of cypinS increases dendrite branching. This increase occurs further away from soma than do increases resulting from overexpression of cypin. In contrast, overexpression of cypin, but not cypinS, decreases dendritic spine density and maturity. This suggests that changes to spines, but not to dendrites, may be dependent on guanine deaminase activity. Furthermore, overexpression of either cypin or cypinS increases miniature excitatory postsynaptic current (mEPSC) frequency, pointing to a presynaptic role for both isoforms. Interestingly, overexpression of cypinS results in a significantly greater increase in frequency than does overexpression of cypin. Thus, cypin and cypinS play distinct roles in neuronal development.

摘要

鸟嘌呤脱氨酶 Cypin(细胞质 PSD-95 相互作用蛋白)与 PSD-95(突触后密度蛋白 95)结合,通过促进微管聚合来调节树突分支。在这里,我们鉴定了 Cypin 的一种新型短亚型,称为 CypinS,它在小鼠和人类组织中表达,但在大鼠组织中不表达。Cypin 和 CypinS 的 mRNA 和蛋白水平在小鼠大脑中于 P7 和 P14 达到峰值,表明这些亚型在发育过程中发挥作用。有趣的是,尽管 CypinS 缺乏鸟嘌呤脱氨酶活性,但 CypinS 的过表达会增加树突分支。这种增加发生在离体细胞体更远的地方,而不是 Cypin 过表达导致的增加。相比之下,Cypin 的过表达,而不是 CypinS 的过表达,会降低树突棘密度和成熟度。这表明,与树突相比,棘突的变化可能依赖于鸟嘌呤脱氨酶活性。此外,Cypin 或 CypinS 的过表达都会增加微小兴奋性突触后电流(mEPSC)的频率,这表明两种亚型都具有突触前作用。有趣的是,CypinS 的过表达导致频率的显著增加,超过了 Cypin 的过表达。因此,Cypin 和 CypinS 在神经元发育中发挥不同的作用。

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