首页> 外文期刊>The Journal of Physiology >Amino-termini isoforms of the Slack K+ channel, regulated by alternative promoters, differentially modulate rhythmic firing and adaptation.
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Amino-termini isoforms of the Slack K+ channel, regulated by alternative promoters, differentially modulate rhythmic firing and adaptation.

机译:Slack K +通道的氨基末端同工型,由其他启动子调控,差异地调节节律性发声和适应。

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The rates of activation and unitary properties of Na+-activated K+ (K(Na)) currents have been found to vary substantially in different types of neurones. One class of K(Na) channels is encoded by the Slack gene. We have now determined that alternative RNA splicing gives rise to at least five different transcripts for Slack, which produce Slack channels that differ in their predicted cytoplasmic amino-termini and in their kinetic properties. Two of these, termed Slack-A channels, contain an amino-terminus domain closely resembling that of another class of K(Na) channels encoded by the Slick gene. Neuronal expression of Slack-A channels and of the previously described Slack isoform, now called Slack-B, are driven by independent promoters. Slack-A mRNAs were enriched in the brainstem and olfactory bulb and detected at significant levels in four different brain regions. When expressed in CHO cells, Slack-A channels activate rapidly upon depolarization and, in single channel recordings in Xenopus oocytes, are characterized by multiple subconductance states with only brief transient openings to the fully open state. In contrast, Slack-B channels activate slowly over hundreds of milliseconds, with openings to the fully open state that are approximately 6-fold longer than those for Slack-A channels. In numerical simulations, neurones in which outward currents are dominated by a Slack-A-like conductance adapt very rapidly to repeated or maintained stimulation over a wide range of stimulus strengths. In contrast, Slack-B currents promote rhythmic firing during maintained stimulation, and allow adaptation rate to vary with stimulus strength. Using an antibody that recognizes all amino-termini isoforms of Slack, Slack immunoreactivity is present at locations that have no Slack-B-specific staining, including olfactory bulb glomeruli and the dendrites of hippocampal neurones, suggesting that Slack channels with alternate amino-termini such as Slack-A channels are present at these locations. Our data suggest that alternative promoters of the Slack gene differentially modulate the properties of neurones.
机译:已经发现,在不同类型的神经元中,Na +激活的K +(K(Na))电流的激活速率和单位性质均发生显着变化。 Slack基因编码一类K(Na)通道。现在我们已经确定,替代性的RNA剪接产生至少五个不同的Slack转录本,这些转录本产生Slack通道,其预测的胞质氨基末端和动力学特性不同。其中两个称为Slack-A通道,其氨基末端结构域与Slick基因编码的另一类K(Na)通道的结构域非常相似。 Slack-A通道和先前描述的Slack亚型(现在称为Slack-B)的神经元表达由独立的启动子驱动。 Slack-A mRNA在脑干和嗅球中富集,并在四个不同的大脑区域中以显着水平检测到。当在CHO细胞中表达时,Slack-A通道会在去极化时迅速激活,并且在非洲爪蟾卵母细胞的单通道记录中,其特征在于多个亚电导状态,只有短暂的短暂打开到完全打开状态。相比之下,Slack-B通道在数百毫秒内缓慢激活,其打开到完全打开状态的时间比Slack-A通道长约6倍。在数值模拟中,外向电流受类Slack-A型电导控制的神经元非常迅速地适应了在广泛的刺激强度范围内重复或维持的刺激。相反,Slack-B电流在维持刺激的过程中促进有节奏的射击,并允许适应率随刺激强度而变化。使用识别Slack的所有氨基末端异构体的抗体,Slack的免疫反应性存在于没有Slack-B特异性染色的位置,包括嗅球和肾小球和海马神经元的树突,这表明Slack通道具有交替的氨基末端因为在这些位置存在Slack-A通道。我们的数据表明,Slack基因的替代启动子有差异地调节神经元的特性。

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