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结核分枝杆菌 ORF Rv0654 编码一种类胡萝卜素加氧酶,介导常规和芳香类胡萝卜素的中环和偏心裂解。

The Mycobacterium tuberculosis ORF Rv0654 encodes a carotenoid oxygenase mediating central and excentric cleavage of conventional and aromatic carotenoids.

机构信息

Institute of Biology II, Albert-Ludwigs University of Freiburg, Freiburg, Germany.

出版信息

FEBS J. 2010 Nov;277(22):4662-73. doi: 10.1111/j.1742-4658.2010.07873.x. Epub 2010 Oct 4.

Abstract

Mycobacterium tuberculosis, the causative agent of tuberculosis, is assumed to lack carotenoids, which are widespread pigments fulfilling important functions as radical scavengers and as a source of apocarotenoids. In mammals, the synthesis of apocarotenoids, including retinoic acid, is initiated by the β-carotene cleavage oxygenases I and II catalyzing either a central or an excentric cleavage of β-carotene, respectively. The M. tuberculosis ORF Rv0654 codes for a putative carotenoid oxygenase conserved in other mycobacteria. In the present study, we investigated the corresponding enzyme, here named M. tuberculosis carotenoid cleavage oxygenase (MtCCO). Using heterologously expressed and purified protein, we show that MtCCO converts several carotenoids and apocarotenoids in vitro. Moreover, the identification of the products suggests that, in contrast to other carotenoid oxygenases, MtCCO cleaves the central C15-C15' and an excentric double bond at the C13-C14 position, leading to retinal (C(20)), β-apo-14'-carotenal (C(22)) and β-apo-13-carotenone (C(18)) from β-carotene, as well as the corresponding hydroxylated products from zeaxanthin and lutein. Moreover, the enzyme cleaves also 3,3'-dihydroxy-isorenieratene representing aromatic carotenoids synthesized by other mycobacteria. Quantification of the products from different substrates indicates that the preference for each of the cleavage positions is determined by the hydroxylation and the nature of the ionone ring. The data obtained in the present study reveal MtCCO to be a novel carotenoid oxygenase and indicate that M. tuberculosis may utilize carotenoids from host cells and interfere with their retinoid metabolism.

摘要

结核分枝杆菌(Mycobacterium tuberculosis)是结核病的病原体,据推测其缺乏类胡萝卜素,而类胡萝卜素作为广泛存在的色素,具有重要的功能,如作为自由基清除剂和类胡萝卜素的前体。在哺乳动物中,类胡萝卜素的合成,包括视黄酸,是由β-胡萝卜素裂解加氧酶 I 和 II 启动的,它们分别催化β-胡萝卜素的中央或偏心裂解。结核分枝杆菌 ORF Rv0654 编码一种假定的类胡萝卜素加氧酶,在其他分枝杆菌中保守。在本研究中,我们研究了相应的酶,在这里命名为结核分枝杆菌类胡萝卜素裂解加氧酶(MtCCO)。使用异源表达和纯化的蛋白,我们表明 MtCCO 在体外转化几种类胡萝卜素和类胡萝卜素前体。此外,产物的鉴定表明,与其他类胡萝卜素加氧酶不同,MtCCO 裂解中央 C15-C15'和偏心 C13-C14 位置的双键,导致从β-胡萝卜素产生视黄醛(C(20))、β-脱-14'-胡萝卜醛(C(22))和β-脱-13-胡萝卜酮(C(18)),以及从玉米黄质和叶黄素产生相应的羟基化产物。此外,该酶还裂解由其他分枝杆菌合成的芳香类胡萝卜素 3,3'-二羟基异戎烯酸。不同底物产物的定量表明,每种裂解位置的偏好由羟化和类异戊二烯环的性质决定。本研究获得的数据表明 MtCCO 是一种新型的类胡萝卜素加氧酶,并表明结核分枝杆菌可能利用宿主细胞中的类胡萝卜素并干扰其视黄醇代谢。

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