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奈瑟脑膜炎球菌中依赖喹诺酮的一氧化氮还原酶的特性,一种发电酶。

Characterization of the quinol-dependent nitric oxide reductase from the pathogen Neisseria meningitidis, an electrogenic enzyme.

机构信息

Department of Biochemistry and Biophysics, Stockholm University, Svante Arrhenius väg 16C, 10691, Stockholm, Sweden.

RIKEN SPring-8 Center, 1-1-1 Kouto, Sayo, Hyogo, 679-5148, Japan.

出版信息

Sci Rep. 2018 Feb 26;8(1):3637. doi: 10.1038/s41598-018-21804-0.

Abstract

Bacterial nitric oxide reductases (NORs) catalyse the reduction of NO to NO and HO. NORs are found either in denitrification chains, or in pathogens where their primary role is detoxification of NO produced by the immune defense of the host. Although NORs belong to the heme-copper oxidase superfamily, comprising proton-pumping O-reducing enzymes, the best studied NORs, cNORs (cytochrome c-dependent), are non-electrogenic. Here, we focus on another type of NOR, qNOR (quinol-dependent). Recombinant qNOR from Neisseria meningitidis, a human pathogen, purified from Escherichia coli, showed high catalytic activity and spectroscopic properties largely similar to cNORs. However, in contrast to cNOR, liposome-reconstituted qNOR showed respiratory control ratios above two, indicating that NO reduction by qNOR was electrogenic. Further, we determined a 4.5 Å crystal structure of the N. meningitidis qNOR, allowing exploration of a potential proton transfer pathway from the cytoplasm by mutagenesis. Most mutations had little effect on the activity, however the E-498 variants were largely inactive, while the corresponding substitution in cNOR was previously shown not to induce significant effects. We thus suggest that, contrary to cNOR, the N. meningitidis qNOR uses cytoplasmic protons for NO reduction. Our results allow possible routes for protons to be discussed.

摘要

细菌一氧化氮还原酶 (NORs) 催化一氧化氮还原为一氧化二氮和水。NORs 存在于反硝化链中,或存在于病原体中,其主要作用是解毒宿主免疫防御产生的一氧化氮。尽管 NORs 属于血红素铜氧化酶超家族,包括质子泵 O 还原酶,但研究最深入的 NORs,cNORs(细胞色素 c 依赖性)是非发电的。在这里,我们关注另一种类型的 NOR,qNOR(依赖醌)。从人类病原体脑膜炎奈瑟菌中纯化的重组 qNOR 来自大肠杆菌,表现出高催化活性和与 cNORs 基本相似的光谱特性。然而,与 cNOR 不同的是,脂质体重建的 qNOR 表现出高于 2 的呼吸控制比,表明 qNOR 的 NO 还原是发电的。此外,我们确定了脑膜炎奈瑟菌 qNOR 的 4.5 Å 晶体结构,通过突变探索了从细胞质中可能的质子转移途径。大多数突变对活性影响不大,但 E-498 变体的活性大大降低,而 cNOR 中的相应取代先前并未显示出显著影响。因此,我们认为,与 cNOR 相反,脑膜炎奈瑟菌 qNOR 使用细胞质质子进行 NO 还原。我们的结果允许讨论质子的可能途径。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/780d/5826923/b740da191a7c/41598_2018_21804_Fig1_HTML.jpg

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