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小窝蛋白与PHB结构域蛋白家族:膜筏、线虫与麻醉剂

Flotillins and the PHB domain protein family: rafts, worms and anaesthetics.

作者信息

Morrow Isabel C, Parton Robert G

机构信息

Institute for Molecular Bioscience, Centre for Microscopy and Microanalysis, University of Queensland, Brisbane, Queensland 4072, Australia.

出版信息

Traffic. 2005 Sep;6(9):725-40. doi: 10.1111/j.1600-0854.2005.00318.x.

DOI:10.1111/j.1600-0854.2005.00318.x
PMID:16101677
Abstract

While our understanding of lipid microdomains has advanced in recent years, many aspects of their formation and dynamics are still unclear. In particular, the molecular determinants that facilitate the partitioning of integral membrane proteins into lipid raft domains are yet to be clarified. This review focuses on a family of raft-associated integral membrane proteins, termed flotillins, which belongs to a larger class of integral membrane proteins that carry an evolutionarily conserved domain called the prohibitin homology (PHB) domain. A number of studies now suggest that eucaryotic proteins carrying this domain have affinity for lipid raft domains. The PHB domain is carried by a diverse array of proteins including stomatin, podocin, the archetypal PHB protein, prohibitin, lower eucaryotic proteins such as the Dictyostelium discoideum proteins vacuolin A and vacuolin B and the Caenorhabditis elegans proteins unc-1, unc-24 and mec-2. The presence of this domain in some procaryotic proteins suggests that the PHB domain may constitute a primordial lipid recognition motif. Recent work has provided new insights into the trafficking and targeting of flotillin and other PHB domain proteins. While the function of this large family of proteins remains unclear, studies of the C. elegans PHB proteins suggest possible links to a class of volatile anaesthetics raising the possibility that these lipophilic agents could influence lipid raft domains. This review will discuss recent insights into the cell biology of flotillins and the large family of evolutionarily conserved PHB domain proteins.

摘要

尽管近年来我们对脂质微区的理解有了进展,但其形成和动态的许多方面仍不清楚。特别是,促进整合膜蛋白分配到脂筏结构域的分子决定因素尚未阐明。本综述聚焦于一类与脂筏相关的整合膜蛋白,称为flotillins,它属于一类更大的整合膜蛋白,这类蛋白带有一个在进化上保守的结构域,称为抗增殖蛋白同源(PHB)结构域。现在许多研究表明,携带该结构域的真核蛋白对脂筏结构域具有亲和力。PHB结构域存在于多种蛋白质中,包括气孔蛋白、足突蛋白、典型的PHB蛋白抗增殖蛋白、低等真核生物蛋白,如盘基网柄菌的液泡蛋白A和液泡蛋白B,以及秀丽隐杆线虫的蛋白unc-1、unc-24和mec-2。在一些原核生物蛋白中也存在该结构域,这表明PHB结构域可能构成一个原始的脂质识别基序。最近的研究为flotillin和其他PHB结构域蛋白的运输和靶向提供了新的见解。虽然这一大类蛋白的功能仍不清楚,但对秀丽隐杆线虫PHB蛋白的研究表明它们可能与一类挥发性麻醉剂有关,这增加了这些亲脂性药物可能影响脂筏结构域的可能性。本综述将讨论关于flotillins和进化上保守的PHB结构域蛋白大家族细胞生物学的最新见解。

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Flotillins and the PHB domain protein family: rafts, worms and anaesthetics.小窝蛋白与PHB结构域蛋白家族:膜筏、线虫与麻醉剂
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