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氨基酸和肽的中性形式对膜的渗透作用:与肽转运起源的相关性。

Permeation of membranes by the neutral form of amino acids and peptides: relevance to the origin of peptide translocation.

作者信息

Chakrabarti A C, Deamer D W

机构信息

Section of Molecular and Cellular Biology, University of California, Davis 95616.

出版信息

J Mol Evol. 1994 Jul;39(1):1-5. doi: 10.1007/BF00178243.

Abstract

The flux of amino acids and other nutrient solutes such as phosphate across lipid bilayers (liposomes) is 10(5) slower than facilitated inward transport across biological membranes. This suggest that primitive cells lacking highly evolved transport systems would have difficulty transporting sufficient nutrients for cell growth to occur. There are two possible ways by which early life may have overcome this difficulty: (1) The membranes of the earliest cellular life-forms may have been intrinsically more permeable to solutes; or (2) some transport mechanism may have been available to facilitate transbilayer movement of solutes essential for cell survival and growth prior to the evolution of membrane transport proteins. Translocation of neutral species represents one such mechanism. The neutral forms of amino acids modified by methylation (creating protonated weak bases) permeate membranes up to 10(10) times faster than charged forms. This increased permeability when coupled to a transmembrane pH gradient can result in significantly increased rates of net unidirectional transport. Such pH gradients can be generated in vesicles used to model protocells that preceded and were presumably ancestral to early forms of life. This transport mechanism may still play a role in some protein translocation processes (e.g. for certain signal sequences, toxins and thylakoid proteins) in vivo.

摘要

氨基酸和其他营养溶质(如磷酸盐)跨脂质双层(脂质体)的通量比通过生物膜的易化内向转运慢10^5倍。这表明,缺乏高度进化的转运系统的原始细胞在运输足够的营养物质以实现细胞生长方面会遇到困难。早期生命可能有两种方式克服这一困难:(1)最早的细胞生命形式的膜可能对溶质具有更高的内在通透性;或者(2)在膜转运蛋白进化之前,可能已经存在某种转运机制来促进对细胞生存和生长至关重要的溶质的跨双层运动。中性物质的转运就是这样一种机制。经甲基化修饰(形成质子化弱碱)的氨基酸中性形式透过膜的速度比带电形式快10^10倍。当与跨膜pH梯度耦合时,这种增加的通透性可导致净单向转运速率显著提高。在用于模拟早于早期生命形式且可能是其祖先的原始细胞的囊泡中可以产生这样的pH梯度。这种转运机制在体内的一些蛋白质转运过程(例如某些信号序列、毒素和类囊体蛋白)中可能仍然发挥作用。

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