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首页> 外文期刊>Journal of Molecular Biology >A folding zone in the ribosomal exit tunnel for Kv1.3 helix formation.
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A folding zone in the ribosomal exit tunnel for Kv1.3 helix formation.

机译:核糖体出口通道中的折叠区,用于形成Kv1.3螺旋。

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摘要

Although it is now clear that protein secondary structure can be acquired early, while the nascent peptide resides within the ribosomal exit tunnel, the principles governing folding of native polytopic proteins have not yet been elucidated. We now report an extensive investigation of native Kv1.3, a voltage-gated K(+) channel, including transmembrane and linker segments synthesized in sequence. These native segments form helices vectorially (N- to C-terminus) only in a permissive vestibule located in the last 20 A of the tunnel. Native linker sequences similarly fold in this vestibule. Finally, secondary structure acquired in the ribosome is retained in the translocon. These findings emerge from accessibility studies of a diversity of native transmembrane and linker sequences and may therefore be applicable to protein biogenesis in general.
机译:尽管现在很清楚可以早期获得蛋白质二级结构,而新生的肽位于核糖体出口通道内,但尚未阐明控制天然多态蛋白折叠的原理。我们现在报告对原生Kv1.3(电压门控K(+)通道,包括按顺序合成的跨膜和接头片段)的广泛研究。这些原始片段仅在位于隧道最后20 A的许可前庭中矢量地(N端至C端)形成螺旋。天然接头序列在该前庭中类似地折叠。最后,在核糖体中获得的二级结构保留在转位子中。这些发现来自对多种天然跨膜和接头序列的可及性研究,因此,它们可能通常适用于蛋白质生物发生。

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