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全面研究来自 的β-碳酸酐酶的阴离子抑制特性,以开发创新的抗菌治疗方法。

A comprehensive investigation of the anion inhibition profile of a β-carbonic anhydrase from for crafting innovative antimicrobial treatments.

机构信息

Department of Biology, Agriculture and Food Sciences, National Research Council (CNR), Institute of Biosciences and Bioresources, Naples, Italy.

Neurofarba Department, Pharmaceutical and Nutraceutical Section, University of Florence, Sesto Fiorentino, Italy.

出版信息

J Enzyme Inhib Med Chem. 2024 Dec;39(1):2372731. doi: 10.1080/14756366.2024.2372731. Epub 2024 Jul 16.

Abstract

This study refers to the intricate world of , a resilient pathogenic bacterium notorious for its propensity at antibiotic resistance in nosocomial infections. Expanding upon previous findings that emphasised the bifunctional enzyme PaaY, revealing unexpected γ-carbonic anhydrase (CA) activity, our research focuses on a different class of CA identified within the genome, the β-CA, designated as 𝛽-AbauCA (also indicated as CanB), which plays a crucial role in the resistance mechanism mediated by AmpC beta-lactamase. Here, we cloned, expressed, and purified the recombinant 𝛽-AbauCA, unveiling its distinctive kinetic properties and inhibition profile with inorganic anions (classical CA inhibitors). The exploration of 𝛽-AbauCA not only enhances our understanding of the CA repertoire of but also establishes a foundation for targeted therapeutic interventions against this resilient pathogen, promising advancements in combating its adaptability and antibiotic resistance.

摘要

本研究涉及一种复杂的 ,这是一种具有弹性的致病性细菌,以其在医院感染中对抗生素产生耐药性而臭名昭著。在之前强调多功能酶 PaaY 并揭示出人意料的γ-碳酸酐酶 (CA) 活性的研究基础上,我们的研究集中在 基因组中鉴定出的另一类 CA,即 β-CA,被指定为 𝛽-AbauCA(也表示为 CanB),它在 AmpC β-内酰胺酶介导的耐药机制中发挥关键作用。在这里,我们克隆、表达和纯化了重组 𝛽-AbauCA,揭示了其独特的动力学特性和对无机阴离子(经典 CA 抑制剂)的抑制谱。对 𝛽-AbauCA 的探索不仅增强了我们对 中 CA 库的理解,也为针对这种弹性病原体的靶向治疗干预奠定了基础,有望在对抗其适应性和抗生素耐药性方面取得进展。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5bc4/467105/b33804a0d2c0/IENZ_A_2372731_F0001_C.jpg

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