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海洋微生物中高效双功能β-内酰胺和同型半胱氨酸内酯降解酶的结构与机制。

Structure and mechanism of potent bifunctional β-lactam- and homoserine lactone-degrading enzymes from marine microorganisms.

机构信息

School of Chemistry and Molecular Biosciences, The University of Queensland, St. Lucia, QLD, 4072, Australia.

Australian Centre for Ecogenomics, The University of Queensland, St. Lucia, QLD, 4072, Australia.

出版信息

Sci Rep. 2020 Jul 30;10(1):12882. doi: 10.1038/s41598-020-68612-z.

Abstract

Genes that confer antibiotic resistance can rapidly be disseminated from one microorganism to another by mobile genetic elements, thus transferring resistance to previously susceptible bacterial strains. The misuse of antibiotics in health care and agriculture has provided a powerful evolutionary pressure to accelerate the spread of resistance genes, including those encoding β-lactamases. These are enzymes that are highly efficient in inactivating most of the commonly used β-lactam antibiotics. However, genes that confer antibiotic resistance are not only associated with pathogenic microorganisms, but are also found in non-pathogenic (i.e. environmental) microorganisms. Two recent examples are metal-dependent β-lactamases (MBLs) from the marine organisms Novosphingobium pentaromativorans and Simiduia agarivorans. Previous studies have demonstrated that their β-lactamase activity is comparable to those of well-known MBLs from pathogenic sources (e.g. NDM-1, AIM-1) but that they also possess efficient lactonase activity, an activity associated with quorum sensing. Here, we probed the structure and mechanism of these two enzymes using crystallographic, spectroscopic and fast kinetics techniques. Despite highly conserved active sites both enzymes demonstrate significant variations in their reaction mechanisms, highlighting both the extraordinary ability of MBLs to adapt to changing environmental conditions and the rather promiscuous acceptance of diverse substrates by these enzymes.

摘要

赋予抗生素抗性的基因可以通过可移动遗传元件迅速从一种微生物传播到另一种微生物,从而将抗性转移到以前敏感的细菌菌株上。在医疗保健和农业中滥用抗生素为加速抗性基因的传播提供了强大的进化压力,包括那些编码β-内酰胺酶的基因。这些酶在使大多数常用的β-内酰胺抗生素失活方面非常有效。然而,赋予抗生素抗性的基因不仅与致病性微生物有关,而且也存在于非致病性(即环境)微生物中。最近有两个例子是来自海洋生物 Novosphingobium pentaromativorans 和 Simiduia agarivorans 的金属依赖型β-内酰胺酶(MBL)。以前的研究表明,它们的β-内酰胺酶活性与来自致病性来源的知名 MBL(如 NDM-1、AIM-1)相当,但它们也具有高效的内酯酶活性,这种活性与群体感应有关。在这里,我们使用晶体学、光谱学和快速动力学技术研究了这两种酶的结构和机制。尽管活性位点高度保守,但这两种酶的反应机制存在显著差异,这突出了 MBL 适应不断变化的环境条件的非凡能力,以及这些酶对各种底物的相当混杂的接受能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f38a/7392888/02712723adf9/41598_2020_68612_Sch1_HTML.jpg

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