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Recognition of transmembrane helices by the endoplasmic reticulum translocon

机译:内质网translocon识别跨膜螺旋

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摘要

Membrane proteins depend on complex translocation machineries for insertion into target membranes. Although it has long been known that an abundance of nonpolar residues in transmembrane helices is the principal criterion for membrane insertion, the specific sequence-coding for transmembrane helices has not been identified. By challenging the endoplasmic reticulum Sec61 translocon with an extensive set of designed polypeptide segments, we have determined the basic features of this code, including a 'biological' hydrophobicity scale. We find that membrane insertion depends strongly on the position of polar residues within transmembrane segments, adding a new dimension to the problem of predicting transmembrane helices from amino acid sequences. Our results indicate that direct protein-lipid interactions are critical during translocon-mediated membrane insertion.
机译:膜蛋白依赖复杂的易位机制插入目标膜。尽管早就知道跨膜螺旋中的大量非极性残基是膜插入的主要标准,但尚未确定跨膜螺旋的特定序列编码。通过用大量设计好的多肽片段挑战内质网Sec61 translocon,我们确定了该密码的基本特征,包括“生物学”疏水性等级。我们发现,膜插入在很大程度上取决于跨膜片段内极性残基的位置,为从氨基酸序列预测跨膜螺旋的问题增加了新的维度。我们的结果表明,直接蛋白-脂质相互作用在translocon介导的膜插入过程中至关重要。

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