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Protein transport into the human ER and related diseases, Sec61-channelopathies

机译:蛋白质转运到人内质网及相关疾病中,Sec61-通道病

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Protein transport into the human endoplasmic reticulum (ER) is relevant to the biogenesis of most soluble and membrane proteins of organelles, which are involved in endo- or exo-cytsosis. It involves amino-terminal signal peptides in the precursor polypeptides and various transport components in the cytosol plus the ER, and can occur co- or post-translationally. The two mechanisms merge at the level of the ER membrane, specifically at the level of the heterotrimeric Sec61 complex, which forms a dynamic polypeptide-conducting channel in the ER membrane. Since the mammalian ER is also the main intracellular calcium storage organelle, and the Sec61 complex is calcium permeable, the Sec61 complex is tightly regulated in its equilibrium between the closed and open conformations, or "gated", by ligands, such as signal peptides of the transport substrates and the ER lumenal Hsp70-type molecular chaperone BiP. Furthermore, BiP binding to the incoming polypeptide contributes to the efficiency and unidirectionality of transport. Recent insights into the structure and dynamic equilibrium of the Sec61 complex have various mechanistic as well as medical implications.
机译:蛋白质转运到人内质网(ER)与大多数细胞器的可溶性和膜蛋白的生物发生有关,这些细胞器参与胞内或胞外胞化。它涉及前体多肽中的氨基末端信号肽和胞质液中的各种转运成分以及ER,并且可以共翻译或翻译后出现。两种机制在ER膜的水平,特别是在异源三聚体Sec61复合体的水平,在ER膜中形成了动态的多肽传导通道。由于哺乳动物的ER也是主要的细胞内钙存储细胞器,并且Sec61复合物是钙可渗透的,因此Sec61复合物在封闭和开放构象或“门控”之间的平衡受到配体(例如信号肽)的严格调节。转运底物和ER腔Hsp70型分子伴侣BiP。此外,BiP与传入多肽的结合有助于提高转运效率和单向性。对Sec61复合物的结构和动态平衡的最新见解具有各种机理和医学意义。

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