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跨膜和膜外因素对膜蛋白热稳定性的影响:钠通道NaChBac的研究

Transmembrane and extramembrane contributions to membrane protein thermal stability: studies with the NaChBac sodium channel.

作者信息

Powl Andrew M, Miles Andrew J, Wallace B A

机构信息

Department of Crystallography, University of London, London, UK.

出版信息

Biochim Biophys Acta. 2012 Mar;1818(3):889-95. doi: 10.1016/j.bbamem.2011.12.019. Epub 2011 Dec 29.

DOI:10.1016/j.bbamem.2011.12.019
PMID:22226848
Abstract

The thermal stabilities of the extramembranous and transmembranous regions of the bacterial voltage-gated sodium channel NaChBac have been characterised using thermal-melt synchrotron radiation circular dichroism (SRCD) spectroscopy. A series of constructs, ranging from the full-length protein containing both the C-terminal cytoplasmic and the transmembranous domains, to proteins with decreasing amounts of the cytoplasmic domain, were examined in order to separately define the roles of these two types of domains in the stability and processes of unfolding of a membrane protein. The sensitivity of the SRCD measurements over a wide range of wavelengths and temperatures has meant that subtle but reproducible conformational changes could be detected with accuracy. The residues in the C-terminal extramembranous domain were highly susceptible to thermal denaturation, but for the most part the transmembrane residues were not thermally-labile and retained their helical character even at very elevated temperatures. The process of thermal unfolding involved an initial irreversible unfolding of the highly labile distal extramembranous C-terminal helical region, which was accompanied by a reversible unfolding of a small number of helical residues in the transmembrane domain. This was then followed by the irreversible unfolding of a limited number of additional transmembrane helical residues at greatly elevated temperatures. Hence this study has been able to determine the different contributions and roles of the transmembrane and extramembrane residues in the processes of thermal denaturation of this multipass integral membrane protein.

摘要

利用热熔同步辐射圆二色光谱(SRCD)对细菌电压门控钠通道NaChBac的膜外区域和跨膜区域的热稳定性进行了表征。研究了一系列构建体,从包含C端胞质结构域和跨膜结构域的全长蛋白,到胞质结构域含量逐渐减少的蛋白,以便分别确定这两种结构域在膜蛋白稳定性和去折叠过程中的作用。SRCD测量在很宽的波长和温度范围内的灵敏度意味着可以精确检测到细微但可重复的构象变化。C端膜外结构域中的残基对热变性高度敏感,但在很大程度上,跨膜残基对热不稳定,即使在非常高的温度下也能保持其螺旋特征。热去折叠过程涉及高度不稳定的远端膜外C端螺旋区域的初始不可逆去折叠,这伴随着跨膜结构域中少量螺旋残基的可逆去折叠。随后在非常高的温度下,有限数量的额外跨膜螺旋残基发生不可逆去折叠。因此,这项研究能够确定跨膜和膜外残基在这种多次跨膜整合膜蛋白热变性过程中的不同贡献和作用。

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