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利用 SB2 菌株在 OB3b 中异源生物合成甲烷菌素

Heterologous Biosynthesis of Methanobactin from sp. Strain SB2 in OB3b.

机构信息

Department of Civil and Environmental Engineering, University of Michigan, Ann Arbor, Michigan 48109-2125, United States.

Roy J. Carver Department of Biochemistry, Biophysics and Molecular Biology, Iowa State University, Ames, Iowa 50011-3260, United States.

出版信息

ACS Synth Biol. 2024 Aug 16;13(8):2347-2356. doi: 10.1021/acssynbio.4c00026. Epub 2024 Aug 7.

Abstract

Aerobic methanotrophs, or methane-consuming microbes, are strongly dependent on copper for their activity. To satisfy this requirement, some methanotrophs produce a copper-binding compound, or chalkophore, called methanobactin (MB). In addition to playing a critical role in methanotrophy, MB has also been shown to have great promise in treating copper-related human diseases, perhaps most significantly Wilson's disease. In this congenital disorder, copper builds up in the liver, leading to irreversible damage and, in severe cases, complete organ failure. Remarkably, MB has been shown to reverse such damage in animal models, and there is a great deal of interest in upscaling MB production for expanded clinical trials. Such efforts, however, are currently hampered as (1) the natural rate of MB production rate by methanotrophs is low, (2) the use of methane as a substrate for MB production is problematic as it is explosive in air, (3) there is limited understanding of the entire pathway of MB biosynthesis, and (4) the most attractive form of MB is produced by sp. strain SB2, a methanotroph that is genetically intractable. Herein, we report heterologous biosynthesis of MB from sp. strain SB2 in an alternative methanotroph, OB3b, not only on methane but also on methanol. As a result, the strategy described herein not only facilitates enhanced MB production but also provides opportunities to construct various mutants to delineate the entire pathway of MB biosynthesis, as well as the creation of modified forms of MB that may have enhanced therapeutic value.

摘要

好氧甲烷营养菌,或甲烷消耗微生物,其活性强烈依赖于铜。为了满足这一需求,一些甲烷营养菌会产生一种结合铜的化合物,或称为甲烷菌素(MB)的 chalkophore。除了在甲烷营养中发挥关键作用外,MB 还被证明在治疗与铜相关的人类疾病方面具有很大的潜力,也许最重要的是威尔逊病。在这种先天性疾病中,铜在肝脏中积聚,导致不可逆转的损伤,在严重的情况下,会导致器官完全衰竭。值得注意的是,MB 已被证明可在动物模型中逆转这种损伤,并且人们对扩大 MB 生产以进行扩大临床试验非常感兴趣。然而,目前这些努力受到阻碍,原因是:(1)甲烷营养菌生产 MB 的自然速率很低;(2)使用甲烷作为 MB 生产的底物存在问题,因为它在空气中具有爆炸性;(3)对 MB 生物合成的整个途径的理解有限;(4)最有吸引力的 MB 形式由 sp. 菌株 SB2 产生,这是一种遗传上难以处理的甲烷营养菌。在此,我们报告了在替代甲烷营养菌 OB3b 中,通过 sp. 菌株 SB2 进行 MB 的异源生物合成,不仅可以利用甲烷,还可以利用甲醇。因此,本文所述的策略不仅促进了 MB 的增强生产,而且还提供了构建各种突变体以描绘 MB 生物合成的整个途径的机会,以及创建可能具有增强治疗价值的修饰形式的 MB 的机会。

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