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昆虫中酚氧化酶诱导黑色素合成的分子调控

Molecular control of phenoloxidase-induced melanin synthesis in an insect.

作者信息

Kan Hongnan, Kim Chan-Hee, Kwon Hyun-Mi, Park Ji-Won, Roh Kyung-Baeg, Lee Hanna, Park Bum-Joon, Zhang Rong, Zhang Jinghai, Söderhäll Kenneth, Ha Nam-Chul, Lee Bok Luel

机构信息

National Research Laboratory of Defense Proteins, College of Pharmacy, Busan 609-735, Korea; School of Life Science and Biopharmaceutics, Shenyang Pharmaceutical University, Shenyang 110016, China.

National Research Laboratory of Defense Proteins, College of Pharmacy, Busan 609-735, Korea.

出版信息

J Biol Chem. 2008 Sep 12;283(37):25316-25323. doi: 10.1074/jbc.M804364200. Epub 2008 Jul 15.

Abstract

The melanization reaction induced by activated phenoloxidase in arthropods must be tightly controlled because of excessive formation of quinones and excessive systemic melanization damage to the hosts. However, the molecular mechanism by which phenoloxidase-induced melanin synthesis is regulated in vivo is largely unknown. It is known that the Spätzle-processing enzyme is a key enzyme in the production of cleaved Spätzle from pro-Spätzle in the Drosophila Toll pathway. Here, we provide biochemical evidence that the Tenebrio molitor Spätzle-processing enzyme converts both the 79-kDa Tenebrio prophenoloxidase and Tenebrio clip-domain SPH1 zymogen to an active melanization complex. This complex, consisting of the 76-kDa Tenebrio phenoloxidase and an active form of Tenebrio clip-domain SPH1, efficiently produces melanin on the surface of bacteria, and this activity has a strong bactericidal effect. Interestingly, we found the phenoloxidase-induced melanization reaction to be tightly regulated by Tenebrio prophenoloxidase, which functions as a competitive inhibitor of melanization complex formation. These results demonstrate that the Tenebrio Toll pathway and the melanization reaction share a common serine protease for the regulation of these two major innate immune responses.

摘要

由于节肢动物中活化的酚氧化酶诱导的黑化反应会过度形成醌类物质,并对宿主造成全身性过度黑化损伤,因此必须对其进行严格控制。然而,酚氧化酶诱导的黑色素合成在体内的调控分子机制在很大程度上尚不清楚。已知斯佩茨尔加工酶是果蝇Toll途径中从原斯佩茨尔产生裂解斯佩茨尔的关键酶。在此,我们提供了生化证据,表明黄粉虫斯佩茨尔加工酶可将79 kDa的黄粉虫前酚氧化酶和黄粉虫clip结构域SPH1酶原都转化为活性黑化复合物。这种由76 kDa的黄粉虫酚氧化酶和活性形式的黄粉虫clip结构域SPH1组成的复合物,能在细菌表面高效产生黑色素,且这种活性具有很强的杀菌作用。有趣的是,我们发现酚氧化酶诱导的黑化反应受到黄粉虫前酚氧化酶的严格调控,黄粉虫前酚氧化酶作为黑化复合物形成的竞争性抑制剂发挥作用。这些结果表明,黄粉虫Toll途径和黑化反应共享一种共同的丝氨酸蛋白酶来调控这两种主要的固有免疫反应。

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