Mechanisms of Bacterial Drug Resistance with Special Emphasis on Phenotypic and Molecular Characterization of Extended Spectrum Beta-lactamase.

IF 1.5 4区 医学 Q4 MICROBIOLOGY New Microbiologica Pub Date : 2024-05-01
Daniel Geleta, Gemeda Abebe, Bikila Alemu, Netsanet Workneh, Getenet Beyene
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Abstract

Antibiotics are designed to effectively treat bacterial infections while minimizing harm to the human body. They work by targeting specific components of bacteria or by disrupting essential processes such as cell wall synthesis, membrane function, protein production, and metabolic pathways. However, the misuse and overuse of antibiotics have led to the emergence of drug resistance in humans, animals, and agriculture, contributing to the global spread of this problem. Drug resistance can be either innate or acquired, with acquired resistance involving changes in the bacterial chromosomes or transferable elements. Bacterial species employ various mechanisms of drug resistance, including modifying the antibiotic targets, inactivating the drug, reducing uptake or increasing efflux, overexpressing the target, utilizing alternative pathways, and forming biofilms. One significant concern in the realm of drug resistance revolves around the emergence and proliferation of extended-spectrum beta-lactamases (ESBLs), a gene that is found in most gram-negative bacteria, primarily carried by Escherichia coli and Klebsiella pneumoniae in healthcare settings. ESBL-mediated resistance poses challenges for diagnosis, treatment, infection control, and antibiotic stewardship. Accurate detection of ESBL genes is crucial, and phenotypic methods are commonly used for initial screening. However, these methods have limitations, and confirmatory molecular techniques such as PCR and DNA sequencing are employed to accurately identify ESBL genes. Despite the significant global concerns surrounding ESBLs, they have spread worldwide, mainly facilitated by healthcare settings, inappropriate antimicrobial use, and host susceptibility. Addressing this issue requires implementing comprehensive measures, including enhanced surveillance, strict infection control practices, antibiotic stewardship programs, rapid diagnostic methods, alternative therapies, public education initiatives, and research focused on developing new drugs. Furthermore, collaboration among the healthcare, public health, and research sectors is pivotal in effectively combating the escalating threat posed by ESBL-mediated resistance. Antibiotics have revolutionized medical care by effectively treating bacterial infections. However, the emergence of ESBL gene resistance poses a global challenge that requires an integrated approach to prevent a threatening future.

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细菌耐药性机制,特别强调广谱β-内酰胺酶的表型和分子特征。
抗生素旨在有效治疗细菌感染,同时尽量减少对人体的伤害。它们针对细菌的特定成分或通过破坏细胞壁合成、膜功能、蛋白质生成和代谢途径等基本过程发挥作用。然而,抗生素的滥用和过度使用已导致人类、动物和农业中出现抗药性,造成这一问题在全球蔓延。耐药性可以是先天性的,也可以是后天获得的,后天获得的耐药性涉及细菌染色体或可转移元素的变化。细菌的抗药性机制多种多样,包括改变抗生素靶点、使药物失活、减少吸收或增加外流、过度表达靶点、利用替代途径以及形成生物膜。耐药性领域的一个重大问题是广谱β-内酰胺酶(ESBLs)的出现和扩散,这种基因存在于大多数革兰氏阴性细菌中,主要由医疗机构中的大肠埃希菌和肺炎克雷伯菌携带。ESBL 介导的耐药性给诊断、治疗、感染控制和抗生素管理带来了挑战。准确检测 ESBL 基因至关重要,表型方法通常用于初步筛选。然而,这些方法有其局限性,因此需要采用 PCR 和 DNA 测序等确证分子技术来准确鉴定 ESBL 基因。尽管全球对 ESBLs 的关注度很高,但 ESBLs 仍在全球范围内传播,这主要是由于医疗环境、抗菌药物使用不当以及宿主易感性等因素造成的。要解决这一问题,需要采取综合措施,包括加强监测、严格的感染控制措施、抗生素管理计划、快速诊断方法、替代疗法、公众教育活动以及以开发新药为重点的研究。此外,医疗保健、公共卫生和研究部门之间的合作对于有效应对 ESBL 介导的耐药性不断升级的威胁至关重要。抗生素能有效治疗细菌感染,给医疗带来了革命性的变化。然而,ESBL 基因耐药性的出现带来了全球性的挑战,需要采取综合方法来防止威胁未来的发生。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
New Microbiologica
New Microbiologica 生物-微生物学
CiteScore
2.20
自引率
5.60%
发文量
40
审稿时长
6-12 weeks
期刊介绍: The publication, diffusion and furtherance of research and study on all aspects of basic and clinical Microbiology and related fields are the chief aims of the journal.
期刊最新文献
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