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两类短杆菌肽A跨膜通道:基于单通道特性的分子模型

Two classes of alamethicin transmembrane channels: molecular models from single-channel properties.

作者信息

Mak D O, Webb W W

机构信息

Physics Department, Cornell University, Ithaca, New York 14853, USA.

出版信息

Biophys J. 1995 Dec;69(6):2323-36. doi: 10.1016/S0006-3495(95)80102-5.

Abstract

Molecular structures of transmembrane channels formed by alamethicin polypeptide aggregates were analyzed by measuring open-channel conductances and state-transition kinetics using voltage-clamp technique with artificial phospholipid bilayers isolated onto micropipettes by a novel solvent-free tip-dip method. Two distinct classes of alamethicin channels, each with a unique set of conductance states and kinetic properties, were identified. Alamethicin Rf50 at low temperatures forms mostly nonpersistent channels with lifetimes of < 1 min. Long-lasting persistent channels are formed by alamethicin Rf30 at all temperatures and by alamethicin Rf50 at room temperature. In the "modified barrel-stave" model for persistent channels based on the crystalline alamethicin secondary structure, the aqueous pore of the channel surrounded by parallel alamethicin monomers has a constriction generated by amino acid side chains protruding from the alamethicin helices into the pore. The model explains quantitatively the nonohmic channel conductance at high applied voltages and the conductance values and ion selectivities of various persistent channel states. The kinetic properties of nonpersistent channels are explained qualitatively by the "reversed-molecule" model in which nonpersistent channels differ from persistent channels by having one of the channel-forming alamethicin monomers oriented antiparallel to the others.

摘要

通过使用电压钳技术,采用一种新颖的无溶剂尖端浸渍法将人工磷脂双层隔离到微吸管上,测量开放通道电导和状态转换动力学,分析了由短杆菌肽多肽聚集体形成的跨膜通道的分子结构。鉴定出了两类不同的短杆菌肽通道,每类都具有一组独特的电导状态和动力学特性。低温下的短杆菌肽Rf50主要形成寿命小于1分钟的非持久性通道。在所有温度下,短杆菌肽Rf30以及在室温下短杆菌肽Rf50都会形成持久的长寿命通道。在基于结晶短杆菌肽二级结构的持久性通道“改良桶板”模型中,由平行短杆菌肽单体包围的通道水孔具有由从短杆菌肽螺旋突出到孔中的氨基酸侧链产生的收缩。该模型定量解释了高施加电压下的非欧姆通道电导以及各种持久通道状态的电导值和离子选择性。非持久性通道的动力学特性通过“反向分子”模型进行定性解释,在该模型中,非持久性通道与持久性通道的不同之处在于,形成通道的短杆菌肽单体之一与其他单体呈反平行排列。

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本文引用的文献

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Hydrophilic surface maps of channel-forming peptides: analysis of amphipathic helices.
Eur Biophys J. 1993;22(4):269-77. doi: 10.1007/BF00180261.
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Alamethicin. A rich model for channel behavior.阿拉米辛。通道行为的丰富模型。
Biophys J. 1984 Jan;45(1):233-47. doi: 10.1016/S0006-3495(84)84151-X.

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