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脊椎动物类胡萝卜素加氧酶的酶学。

Enzymology of vertebrate carotenoid oxygenases.

机构信息

Program in Human Nutrition, Department of Human Sciences, Ohio State University, Columbus, OH 43210, USA; Ohio State Biochemistry Program, USA.

Program in Human Nutrition, Department of Human Sciences, Ohio State University, Columbus, OH 43210, USA; Foods for Health Discovery Theme, Ohio State University, USA.

出版信息

Biochim Biophys Acta Mol Cell Biol Lipids. 2020 Nov;1865(11):158653. doi: 10.1016/j.bbalip.2020.158653. Epub 2020 Feb 5.

Abstract

Mammals and higher vertebrates including humans have only three members of the carotenoid cleavage dioxygenase family of enzymes. This review focuses on the two that function as carotenoid oxygenases. β-Carotene 15,15'-dioxygenase (BCO1) catalyzes the oxidative cleavage of the central 15,15' carbon-carbon double of β-carotene bond by addition of molecular oxygen. The product of the reaction is retinaldehyde (retinal or β-apo-15-carotenal). Thus, BCO1 is the enzyme responsible for the conversion of provitamin A carotenoids to vitamin A. It also cleaves the 15,15' bond of β-apocarotenals to yield retinal and of lycopene to yield apo-15-lycopenal. β-Carotene 9',10'-dioxygenase (BCO2) catalyzes the cleavage of the 9,10 and 9',10' double bonds of a wider variety of carotenoids, including both provitamin A and non-provitamin A carotenoids, as well as the xanthophylls, lutein and zeaxanthin. Indeed, the enzyme shows a marked preference for utilization of these xanthophylls and other substrates with hydroxylated terminal rings. Studies of the phenotypes of BCO1 null, BCO2 null, and BCO1/2 double knockout mice and of humans with polymorphisms in the enzymes, has clarified the role of these enzymes in whole body carotenoid and vitamin A homeostasis. These studies also demonstrate the relationship between enzyme expression and whole body lipid and energy metabolism and oxidative stress. In addition, relationships between BCO1 and BCO2 and the development or risk of metabolic diseases, eye diseases and cancer have been observed. While the precise roles of the enzymes in the pathophysiology of most of these diseases is not presently clear, these gaps in knowledge provide fertile ground for rigorous future investigations. This article is part of a Special Issue entitled Carotenoids: Recent Advances in Cell and Molecular Biology edited by Johannes von Lintig and Loredana Quadro.

摘要

哺乳动物和包括人类在内的高等脊椎动物只有三种类胡萝卜素双加氧酶家族的酶。本篇综述聚焦于作为类胡萝卜素加氧酶发挥作用的两种酶。β-胡萝卜素 15,15'-双加氧酶(BCO1)催化β-胡萝卜素中央 15,15'碳-碳双键的氧化裂解,通过添加分子氧。反应的产物是视黄醛(视黄醇或β-无锥-15-胡萝卜醛)。因此,BCO1 是将维生素原 A 类胡萝卜素转化为维生素 A 的酶。它还裂解β-无锥胡萝卜醛的 15,15'键,生成视黄醛和番茄红素的 15,15'键,生成无锥-15-番茄红素醛。β-胡萝卜素 9',10'-双加氧酶(BCO2)催化更广泛种类的类胡萝卜素的 9,10 和 9',10'双键的裂解,包括维生素原 A 和非维生素原 A 类胡萝卜素以及叶黄素、玉米黄质和玉米黄素。事实上,该酶对这些叶黄素和其他具有羟基化末端环的底物表现出明显的利用偏好。BCO1 缺失、BCO2 缺失、BCO1/2 双缺失小鼠以及酶中存在多态性的人类的表型研究,阐明了这些酶在全身类胡萝卜素和维生素 A 动态平衡中的作用。这些研究还表明了酶表达与全身脂质和能量代谢以及氧化应激之间的关系。此外,还观察到 BCO1 和 BCO2 与代谢性疾病、眼病和癌症的发生或风险之间的关系。虽然目前尚不清楚这些酶在大多数这些疾病的病理生理学中的精确作用,但这些知识空白为未来的严格研究提供了肥沃的土壤。本文是由 Johannes von Lintig 和 Loredana Quadro 编辑的特刊“类胡萝卜素:细胞和分子生物学的最新进展”的一部分。

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