Genomic profiling of pan-drug resistant proteus mirabilis Isolates reveals antimicrobial resistance and virulence gene landscape

IF 3.9 4区生物学 Q1 GENETICS & HEREDITY

Functional & Integrative Genomics Pub Date : 2024-09-03 DOI:10.1007/s10142-024-01419-7

Sarah Soliman, Salah Abdalla, Amal Zedan, Shymaa Enany

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Abstract

Proteus mirabilis is a gram-negative pathogen that caused significant opportunistic infections. In this study we aimed to identify antimicrobial resistance (AMR) genes and virulence determinants in two pan-drug resistant isolate “Bacteria_11” and “Bacteria_27” using whole genome sequencing. Proteus mirabilis “Bacteria_11” and “Bacteria_27” were isolated from two different hospitalized patients in Egypt. Antimicrobial susceptibility determined using Vitek 2 system, then whole genome sequencing (WGS) using MinION nanopore sequencing was done. Antimicrobial resistant genes and virulence determinants were identified using ResFinder, CADR AMR database, Abricate tool and VF analyzer were used respectively. Multiple sequence alignment was performed using MAFFT and FastTree, respectively. All genes were present within bacterial chromosome and no plasmid was detected. “Bacteria_11” and “Bacteria_27” had sizes of approximately 4,128,657 bp and 4,120,646 bp respectively, with GC content of 39.15% and 39.09%. “Bacteria_11” and “Bacteria_27” harbored 43 and 42 antimicrobial resistance genes respectively with different resistance mechanisms, and up to 55 and 59 virulence genes respectively. Different resistance mechanisms were identified: antibiotic inactivation, antibiotic efflux, antibiotic target replacement, and antibiotic target change. We identified several genes associated with aminoglycoside resistance, sulfonamide resistance. trimethoprim resistance tetracycline resistance proteins. Also, those responsible for chloramphenicol resistance. For beta-lactam resistance, only blaVEB and blaCMY-2 genes were detected. Genome analysis revealed several virulence factors contribution in isolates pathogenicity and bacterial adaptation. As well as numerous typical secretion systems (TSSs) were present in the two isolates, including T6SS and T3SS. Whole genome sequencing of both isolates identify their genetic context of antimicrobial resistant genes and virulence determinants. This genomic analysis offers detailed representation of resistant mechanisms. Also, it clarifies P. mirabilis ability to acquire resistance and highlights the emergence of extensive drug resistant (XDR) and pan-drug resistant (PDR) strains. This may help in choosing the most appropriate antibiotic treatment and limiting broad spectrum antibiotic use.

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对具有泛耐药性的 mirabilis 蛋白球菌分离物进行基因组分析，揭示抗菌药耐药性和毒力基因图谱。

奇异变形杆菌（Proteus mirabilis）是一种革兰氏阴性病原体，可引起严重的机会性感染。在这项研究中，我们旨在利用全基因组测序鉴定两种泛耐药分离物 "Bacteria_11 "和 "Bacteria_27 "中的抗菌药耐药性（AMR）基因和毒力决定因素。神奇变形杆菌 "Bacteria_11 "和 "Bacteria_27 "是从埃及两名不同的住院病人身上分离出来的。使用 Vitek 2 系统测定了抗菌药敏感性，然后使用 MinION 纳米孔测序技术进行了全基因组测序（WGS）。分别使用 ResFinder、CADR AMR 数据库、Abricate 工具和 VF 分析仪鉴定了抗菌药耐药基因和毒力决定因素。分别使用 MAFFT 和 FastTree 进行了多重序列比对。所有基因都存在于细菌染色体中，没有检测到质粒。"细菌_11 "和 "细菌_27 "的大小分别约为 4,128,657 bp 和 4,120,646 bp，GC 含量分别为 39.15%和 39.09%。"细菌_11 "和 "细菌_27 "分别含有 43 和 42 个具有不同抗药性机制的抗菌药抗性基因，以及多达 55 和 59 个毒力基因。我们发现了不同的抗性机理：抗生素失活、抗生素外流、抗生素靶标替代和抗生素靶标改变。我们发现了几个与氨基糖苷类抗药性、磺胺类抗药性、三甲双胍抗药性和四环素抗药性蛋白相关的基因。此外，还有氯霉素耐药性基因。在抗β-内酰胺方面，只检测到 blaVEB 和 blaCMY-2 基因。基因组分析表明，一些毒力因子对分离物的致病性和细菌适应性有影响。此外，这两种分离物中还存在许多典型分泌系统（TSS），包括 T6SS 和 T3SS。对这两种分离物进行的全基因组测序确定了其抗菌基因和毒力决定因子的遗传背景。这种基因组分析提供了耐药机制的详细表述。此外，它还阐明了 P. mirabilis 获得耐药性的能力，并突出了广泛耐药（XDR）和泛耐药（PDR）菌株的出现。这可能有助于选择最合适的抗生素治疗方法和限制广谱抗生素的使用。

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

Functional & Integrative Genomics 生物-遗传学

CiteScore

3.50

自引率

3.40%

发文量

审稿时长

2 months

期刊介绍： Functional & Integrative Genomics is devoted to large-scale studies of genomes and their functions, including systems analyses of biological processes. The journal will provide the research community an integrated platform where researchers can share, review and discuss their findings on important biological questions that will ultimately enable us to answer the fundamental question: How do genomes work?