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Structure of the E. coli protein-conducting channel bound to a translating ribosome

机译:大肠杆菌蛋白传导通道与翻译核糖体结合的结构

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摘要

Secreted and membrane proteins are translocated across or into cell membranes through a protein-conducting channel (PCC). Here we present a cryo-electron microscopy reconstruction of the Escherichia coli PCC, SecYEG, complexed with the ribosome and a nascent chain containing a signal anchor. This reconstruction shows a messenger RNA, three transfer RNAs, the nascent chain, and detailed features of both a translocating PCC and a second, non-translocating PCC bound to mRNA hairpins. The translocating PCC forms connections with ribosomal RNA hairpins on two sides and ribosomal proteins at the back, leaving a frontal opening. Normal mode-based flexible fitting of the archaeal SecYEβ structure into the PCC electron microscopy densities favours a front-to-front arrangement of two SecYEG complexes in the PCC, and supports channel formation by the opening of two linked SecY halves during polypeptide translocation. On the basis of our observation in the translocating PCC of two segregated pores with different degrees of access to bulk lipid, we propose a model for co-translational protein translocation.
机译:分泌蛋白和膜蛋白通过蛋白传导通道(PCC)跨细胞膜或进入细胞膜。在这里,我们介绍了大肠杆菌PCC,SecYEG与核糖体和一条包含信号锚点的新生链复合而成的低温电子显微镜重建技术。这种重建显示了信使RNA,三个转移RNA,新生链以及与mRNA发夹结合的易位PCC和第二个非易位PCC的详细特征。易位的PCC与两侧的核糖体RNA发夹和背面的核糖体蛋白形成连接,从而留下额叶开口。基于正常模式的古细菌SecYEβ结构到PCC电子显微镜密度的柔性拟合有利于PCC中两个SecYEG复合物的从前到前排列,并通过多肽转运过程中两个相连的SecY半部分的打开来支持通道形成。基于我们在两个分离的毛孔的易位PCC中的观察结果,这些毛孔具有不同程度的进入大脂质的能力,我们提出了共翻译蛋白易位的模型。

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