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对氨基酸序列改变的线性短杆菌肽进行的单通道研究。对第1位和第11位苯丙氨酸、色氨酸和酪氨酸取代情况的比较。

Single-channel studies on linear gramicidins with altered amino acid sequences. A comparison of phenylalanine, tryptophane, and tyrosine substitutions at positions 1 and 11.

作者信息

Mazet J L, Andersen O S, Koeppe R E

出版信息

Biophys J. 1984 Jan;45(1):263-76. doi: 10.1016/S0006-3495(84)84153-3.

Abstract

The relation between chemical structure and permeability characteristics of transmembrane channels has been investigated with the linear gramicidins (A, B, and C), where the amino acid at position 1 was chemically replaced by phenylalanine, tryptophane or tyrosine. The purity of most of the compounds was estimated to be greater than 99.99%. The modifications resulted in a wide range of conductance changes in NaCl solutions: sixfold from tryptophane gramicidin A to tyrosine gramicidin B. The conductance changes induced by a given amino acid substitution at position 1 are not the same as at position 11. The only important change in the Na+ affinity was observed when the first amino acid was tyrosine. No major conformational changes of the polypeptide backbone structure could be detected on the basis of experiments with mixtures of different analogues and valine gramicidin A (except possibly with tyrosine at position 1), as all the compounds investigated could form hybrid channels with valine gramicidin A. The side chains are not in direct contact with the permeating ions. The results were therefore interpreted in terms of modifications of the energy profile for ion movement through the channel, possibly due to an electrostatic interaction between the dipoles of the side chains and ions in the channel.

摘要

利用线性短杆菌肽(A、B和C)研究了跨膜通道的化学结构与通透性特征之间的关系,其中第1位的氨基酸被苯丙氨酸、色氨酸或酪氨酸化学取代。大多数化合物的纯度估计大于99.99%。这些修饰导致在NaCl溶液中电导发生广泛变化:从色氨酸短杆菌肽A到酪氨酸短杆菌肽B变化了六倍。在第1位由给定氨基酸取代引起的电导变化与在第11位时不同。当第一个氨基酸为酪氨酸时,观察到Na+亲和力的唯一重要变化。基于不同类似物与缬氨酸短杆菌肽A混合物的实验(可能第1位为酪氨酸除外),未检测到多肽主链结构的主要构象变化,因为所有研究的化合物都能与缬氨酸短杆菌肽A形成杂合通道。侧链不与渗透离子直接接触。因此,这些结果是根据离子通过通道的能量分布变化来解释的,这可能是由于侧链偶极与通道中离子之间的静电相互作用所致。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5708/1435278/f9578a581185/biophysj00210-0266-a.jpg

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