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DOXYL-硬脂酸对重组NCD-4标记的细胞色素c氧化酶复合物的荧光猝灭作用。

Fluorescence quenching of reconstituted NCD-4-labeled cytochrome c oxidase complex by DOXYL-stearic acids.

作者信息

Musser S M, Larsen R W, Chan S I

机构信息

Arthur Amos Noyes Laboratory of Chemical Physics, California Institute of Technology, Pasadena 91125.

出版信息

Biophys J. 1993 Dec;65(6):2348-59. doi: 10.1016/S0006-3495(93)81309-2.

Abstract

It has been known for some time that dicyclohexylcarbodiimide (DCCD) inhibits the proton translocation function of the cytochrome c oxidase complex (CcO) and that there is one major site in subunit III which is modified upon reaction with DCCD (Glu-90 for the bovine enzyme). We have examined the reaction of bovine CcO with N-cyclohexyl-N'-(4-dimethylamino-alpha-napthyl)carbodiimide (NCD-4), a fluorescent analog of DCCD. NCD-4 labeling of CcO is strongly inhibited by DCCD implicating Glu-90 of subunit III as the site of chemical modification by NCD-4. The fluorescence of reconstituted NCD-4-labeled bovine CcO is strongly quenched by hydrophobic nitroxides, whereas hydrophilic nitroxides and iodide ions have a reduced quenching ability. It is concluded that the Glu-90 of subunit III resides near the protein-lipid interface of the membrane spanning region of the enzyme. Different quenching abilities of 5-, 7-, 10-, 12-, and 16-4,4-dimethyl-3-oxazolinyloxy-stearic acids suggest that the NCD-4 label is located in the membrane bilayer in the region near the middle of the hydrocarbon tail of stearic acid. In light of these results, it is unlikely that Glu-90 is part of a proton channel that is associated with the proton pumping machinery of the enzyme but the outcome of this study does not eliminate an allosteric regulatory role for this residue.

摘要

一段时间以来,人们已经知道二环己基碳二亚胺(DCCD)会抑制细胞色素c氧化酶复合体(CcO)的质子转运功能,并且在亚基III中有一个主要位点,与DCCD反应时会被修饰(牛酶的Glu-90)。我们研究了牛CcO与N-环己基-N'-(4-二甲基氨基-α-萘基)碳二亚胺(NCD-4)(一种DCCD的荧光类似物)的反应。DCCD强烈抑制NCD-4对CcO的标记,这表明亚基III的Glu-90是NCD-4进行化学修饰的位点。重构的NCD-4标记的牛CcO的荧光会被疏水氮氧化物强烈猝灭,而亲水氮氧化物和碘离子的猝灭能力则降低。由此得出结论,亚基III的Glu-90位于该酶跨膜区域的蛋白质-脂质界面附近。5-、7-、10-、12-和16-4,4-二甲基-3-恶唑啉基氧基-硬脂酸的不同猝灭能力表明,NCD-4标记位于硬脂酸烃链中部附近的膜双层区域。鉴于这些结果,Glu-90不太可能是与该酶质子泵机制相关的质子通道的一部分,但这项研究的结果并未排除该残基的变构调节作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ddf6/1225976/3efa25a47d65/biophysj00081-0087-a.jpg

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