利用模型系统研究Nox/Duox酶的生物学功能。

Darren R Ritsick, William A Edens, James W McCoy, J David Lambeth
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引用次数: 26

摘要

活性氧;包括超氧化物和H202)通常被认为具有广泛的反应性和细胞毒性。吞噬细胞利用NADPH氧化酶产生大量ROS,并利用其毒性作为宿主防御机制来杀死入侵的微生物。然而,最近在许多非吞噬细胞中表达的Nox和Duox酶的发现表明,ROS的“故意”产生具有额外的细胞作用,目前尚不完全清楚。ROS在哺乳动物中的功能主要是从细胞培养实验中推断出来的,包括有丝分裂生长、细胞凋亡和血管生成的信号传导。Nox/Duox酶也可以提供H202作为过氧化物酶的底物(或者,在Duox的情况下,为其自身的过氧化物酶结构域),从而支持过氧化反应。跨物种和王国对活性氧和氮氧化物酶的生物学功能的广泛比较提供了对哺乳动物可能功能的见解。为了进一步了解Nox/Duox酶的新生物学作用,我们在秀丽隐杆线虫、黑胃果蝇和小鼠等模式生物中操纵Nox/Duox酶的表达。本章着重于从这些方法中获得的对Nox酶的作用的新见解。
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The use of model systems to study biological functions of Nox/Duox enzymes.

ROS (reactive oxygen species; including superoxide and H202) are conventionally thought of as being broadly reactive and cytotoxic. Phagocytes utilize an NADPH oxidase to generate large amounts of ROS, and exploit their toxic properties as a host-defence mechanism to kill invading microbes. However, the recent discovery of the Nox and Duox enzymes that are expressed in many non-phagocytic cells implies that the 'deliberate' generation of ROS has additional cellular roles, which are currently incompletely understood. Functions of ROS in mammals have been inferred primarily from cell-culture experiments, and include signalling for mitogenic growth, apoptosis and angiogenesis. Nox/Duox enzymes may also provide H202 as a substrate for peroxidase enzymes (or, in the case of Duox, for its own peroxidase domain), thereby supporting peroxidative reactions. A broad comparison of biological functions of ROS and Nox enzymes across species and kingdoms provides insights into possible functions in mammals. To further understand novel biological roles for Nox/Duox enzymes, we are manipulating the expression of Nox/Duox enzymes in model organisms including Caenorhabditis elegans, Drosophila melanogaster and mouse. This chapter focuses on new insights into the roles of Nox enzymes gained from these approaches.

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