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首页> 外文期刊>The Biochemical Journal >Reorientation of the first signal-anchor sequence during potassium channel biogenesis at the Sec61 complex
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Reorientation of the first signal-anchor sequence during potassium channel biogenesis at the Sec61 complex

机译:在SEC61复合物在钾通道生物发生期间重新定向第一信号锚序列

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摘要

The majority of the polytopic proteins that are synthesized at the ER (endoplasrnic reticulum) are integrated co-translationally via the Sec61 translocon, which provides lateral access for their hydrophobic TMs (transmembrane regions) to the phospholipid bilayer. A prolonged association between TMs of the potassium channel subunit, TASK-1 [TWIK (tandem-pore weak inwardly rectifying potassium channel)-related acid-sensitive potassium channel 1], and the Sec61 complex suggests that the ER translocon co-ordinates the folding/assembly of the TMs present in the nascent chain. The N-terminus of both TASK-1 and Kcv (potassium channel protein of chlorella virus), another potassium channel subunit of viral origin, has access to the N-glycosylation machinery located in the ER lumen, indicating that the Sec61 complex can accommodate multiple arrangements/orientations of TMs within the nascent chain, both in vitro and in vivo. Hence the ER translocon can provide the ribosome-bound nascent chain with a dynamic environment in which it can explore a range of different conformations en route to its correct transmembrane topology and final native structure.
机译:在ER(端口碱网上)合成的多种多种多数蛋白质通过SEC61摇合物(Endoplasrnic网状物)合成,通过SEC61摇峰共同整合,其为其疏水性TMS(跨膜区)提供给磷脂双层的横向接近。钾通道亚基的TMS之间的延长关联,任务-1 [Twik(串联孔弱向内整流钾通道) - SEC61复合物表明,ER摇峰协调折叠/组装在新生链中存在的TMS。任务-1和KCV(小球藻病毒钾蛋白质)的N-末端,病毒来源的另一种钾通道亚基,可以进入位于ER流明中的N-糖基化机器,表明SEC61复合物可以容纳多个在体外和体内嗜好链中的TMS在脱血链中的安排/取向。因此,ER转译能够提供具有动态环境的核糖体 - 结合的新生链,其中它可以探索到其正确的跨膜拓扑和最终的天然结构的途中的一系列不同构象。

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