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肉碱/酰基肉碱转位酶RX2PANAAXF独特基序内残基的功能表征。

Functional characterization of residues within the carnitine/acylcarnitine translocase RX2PANAAXF distinct motif.

作者信息

De Lucas J Ramon, Indiveri Cesare, Tonazzi Annamaria, Perez Patricia, Giangregorio Nicola, Iacobazzi Vito, Palmieri Ferdinando

机构信息

Departamento de Microbiología y Parasitología, Facultad de Farmacia, Campus Universitario, Universidad de Alcalá, Alcalá de Henares, Madrid, Spain.

出版信息

Mol Membr Biol. 2008 Feb;25(2):152-63. doi: 10.1080/09687680701697476.

Abstract

The mitochondrial carnitine/acylcarnitine carrier (CAC) is characterized by the presence of a distinct motif, RXXPANAAXF, within its sixth transmembrane alpha-helix. In this study, we analysed the role of the amino acids of this motif in the structure-function relationships of the human CAC by using two complementary approaches. First, we performed functional analysis in the model fungus Aspergillus nidulans of selected mutations with structural and functional relevance. Second, similar mutant human CACs were biochemically characterized after their reconstitution into liposomes. Both analyses have provided relevant information on the importance and role of the CAC motif residues in the activity and metabolic function of CAC. Only the two adjacent alanines, Ala281 and Ala282 in the human CAC, have been found not to be crucial for transport activity and in vivo function. Results obtained from amino acid substitutions of residues Arg275, Asn280 and Phe284 of human CAC together with structural analysis using molecular modelling of the carrier suggest that R275, N280 and F284 are involved in substrate binding during acylcarnitine/carnitine translocation. Furthermore, functional analysis of mutations of residues Pro278 and Ala279 in A. nidulans, together with kinetic data in reconstituted liposomes, suggest a predominant structural role for these amino acids.

摘要

线粒体肉碱/脂酰肉碱载体(CAC)的特征是在其第六个跨膜α-螺旋内存在一个独特的基序RXXPANAAXF。在本研究中,我们通过两种互补方法分析了该基序中的氨基酸在人CAC结构-功能关系中的作用。首先,我们在构巢曲霉模型真菌中对具有结构和功能相关性的选定突变进行了功能分析。其次,将类似的突变型人CAC重构到脂质体中后对其进行了生化表征。这两种分析都提供了有关CAC基序残基在CAC活性和代谢功能中的重要性和作用的相关信息。仅发现人CAC中的两个相邻丙氨酸Ala281和Ala282对转运活性和体内功能并非至关重要。从人CAC的Arg275、Asn280和Phe284残基的氨基酸取代获得的结果,以及使用该载体的分子模型进行的结构分析表明,R275、N280和F284在酰基肉碱/肉碱转运过程中参与底物结合。此外,对构巢曲霉中Pro278和Ala279残基突变的功能分析,以及重构脂质体中的动力学数据表明,这些氨基酸起主要的结构作用。

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