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首页> 外文期刊>The Journal of Physiology >Developmental expression of the novel voltage-gated sodium channel auxiliary subunit beta3, in rat CNS.
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Developmental expression of the novel voltage-gated sodium channel auxiliary subunit beta3, in rat CNS.

机译:新型电压门控钠通道辅助亚基beta3在大鼠中枢神经系统中的发育表达。

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摘要

1. We have compared the mRNA distribution of sodium channel alpha subunits known to be expressed during development with the known auxiliary subunits Nabeta1.1 and Nabeta2.1 and the novel, recently cloned subunit, beta3. 2. In situ hybridisation studies demonstrated high levels of Nav1.2, Nav1.3, Nav1.6 and beta3 mRNA at embryonic stages whilst Nabeta1.1 and Nabeta2.1 mRNA was absent throughout this period. 3. Nabeta1.1 and Nabeta2.1 expression occurred after postnatal day 3 (P3), increasing steadily in most brain regions until adulthood. beta3 expression differentially decreased after P3 in certain areas but remained high in the hippocampus and striatum. 4. Emulsion-dipped slides showed co-localisation of beta3 with Nav1.3 mRNA in areas of the CNS suggesting that these subunits may be capable of functional interaction. 5. Co-expression in Xenopus oocytes revealed that beta3 could modify the properties of Nav1.3; beta3 changed the equilibrium of Nav1.3 between the fast and slow gating modes and caused a negative shift in the voltage dependence of activation and inactivation. 6. In conclusion, beta3 is shown to be the predominant beta subunit expressed during development and is capable of modulating the kinetic properties of the embryonic Nav1.3 subunit. These findings provide new information regarding the nature and properties of voltage-gated sodium channels during development.
机译:1.我们已经比较了已知在发育过程中表达的钠通道α亚基的mRNA分布与已知的辅助亚基Nabeta1.1和Nabeta2.1以及最近克隆的新型亚基beta3。 2.原位杂交研究表明在胚胎期高水平的Nav1.2,Nav1.3,Nav1.6和beta3 mRNA,而在此期间没有Nabeta1.1和Nabeta2.1 mRNA。 3. Nabeta1.1和Nabeta2.1表达发生于出生后第3天(P3),在大多数大脑区域稳定增长直至成年。在某些区域中,P3后beta3表达差异性降低,但在海马和纹状体中仍然较高。 4.浸有乳剂的玻片在CNS区域显示beta3与Nav1.3 mRNA共定位,表明这些亚基可能具有功能性相互作用。 5.在非洲爪蟾卵母细胞中的共表达表明beta3可以修饰Nav1.3的特性。 beta3在快速和慢速门控模式之间改变了Nav1.3的平衡,并导致激活和失活的电压依赖性发生负向偏移。 6.总而言之,beta3被证明是在发育过程中表达的主要beta亚基,并且能够调节胚胎Nav1.3亚基的动力学特性。这些发现为开发过程中电压门控钠通道的性质和性质提供了新的信息。

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