噬菌体 HZY2308 对抗鲍曼不动杆菌的特性以及耐噬菌体细菌的鉴定。

IF 4 3区 医学 Q2 VIROLOGY
Ruilin Wang, Xiaojuan You, Xinwei Liu, Bing Fei, Yifan Li, Dan Wang, Rui Zhu, Yongwei Li
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引用次数: 0

摘要

背景:鲍曼不动杆菌(AB)是医院获得性感染的主要病因,其中耐碳青霉烯类鲍曼不动杆菌(CRAB)被列为高度优先的关键病原体。噬菌体疗法正在成为对抗耐药细菌感染的一种有前途的替代疗法。本研究从医院污水中分离出一种溶菌噬菌体 HZY2308,并对其生物学特性、生物安全性和抗生物膜特性进行了鉴定。此外,还研究了噬菌体HZY2308与抗生素联合使用的抗菌效果,并证明了噬菌体耐药菌株AB48-R的明显特征,为进一步研究阐明噬菌体耐药性的产生机制提供了数据支持:方法:以临床菌株AB48为宿主菌,采用双琼脂平板法分离出噬菌体HZY2308。方法:以临床菌株 AB48 为宿主,采用双琼脂平板法分离得到噬菌体 HZY2308,用透射电子显微镜(TEM)鉴定了噬菌体 HZY2308 的形态,并通过宿主范围、接种效率(EOP)、对温度、pH 值和氯仿的敏感性、一步生长曲线、最佳感染倍数(MOI)以及内毒素和细胞毒性的检测鉴定了噬菌体 HZY2308 的生物学特性。此外,还利用 CGview 绘制了 HZY2308 的全基因组图谱,并利用 MEGA 构建了 HZY2308 的系统发生树。此外,还使用 Easyfig 比较了 HZY2308 噬菌体和所选噬菌体的全基因组序列。为了研究噬菌体 HZY2308 与替加环素(TGC)的协同作用和杀菌动力学,对它们进行了棋盘试验。通过水晶紫对生物膜的半定量染色、2,3-双(2-甲氧基-4-硝基-5-磺酸苯基)-2 H-四唑-5-甲酰苯胺(XTT)测定法和荧光显微镜观察生物膜结构,研究了 HZY2308 对生物膜的影响。最后,通过菌落形成能力、形态、生长曲线、吸附效率和抗生素敏感性检测,对噬菌体抗性细菌 AB48-R 进行了表征:结果:从医院污水中分离出一种溶菌噬菌体 HZY2308,该噬菌体具有潜伏期短、爆发量大、稳定性强等优点。在基因和细胞层面进行的安全性评估也取得了积极成果。此外,噬菌体 HZY2308 还能有效抑制 AB 生物膜的形成,并破坏已形成的生物膜结构。此外,当噬菌体 HZY2308 与替加环素结合使用时,还能产生协同抗菌效果。有趣的是,通过自然选择筛选出了抗噬菌体菌株 AB48-R。与野生菌株 AB48 相比,噬菌体对 AB48-R 的吸附效率降低了。然而,AB48-R 对头孢吡肟、庆大霉素、阿米卡星和妥布霉素等抗生素的敏感性却增加了,这表明了一种进化上的权衡:结论:HZY2308噬菌体具有很强的抗菌潜力,尤其是与替加环素联合使用时,噬菌体耐药菌株对抗生素的敏感性增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterization of phage HZY2308 against Acinetobacter baumannii and identification of phage-resistant bacteria.

Background: Acinetobacter baumannii (AB) is a notable cause of hospital-acquired infections, with carbapenem-resistant Acinetobacter baumannii (CRAB) classified as a high-priority critical pathogen. Bacteriophage therapy is emerging as a promising alternative to combat drug-resistant bacterial infections. In this study, a lytic phage, HZY2308, was isolated from hospital sewage, and the biological properties, biosafety and anti-biofilm properties of phage HZY2308 were characterized and identified. Moreover, the antibacterial effect of phage HZY2308 in combination with antibiotics was investigated, and the apparent characteristics of phage-resistant strain AB48-R were demonstrated, which provided data support for further studies to elucidate the mechanism of generating phage resistance.

Methods: Phage HZY2308 was isolated by double agar plate method using clinical strain AB48 as the host bacterium. The morphology of phage HZY2308 was identified by transmission electron microscopy (TEM), and biological characteristics of phage HZY2308 were identified by host range, the efficiency of plating (EOP), sensitivity to temperature, pH, and chloroform, one-step growth curve, the optimal multiplicity of infection (MOI), and detection of endotoxin and cytotoxicity. Besides, the complete genome map of HZY2308 was constructed using CGview, and the phylogenetic tree of HZY2308 was constructed with MEGA. Additionally, the full genomic sequence of phage HZY2308 and the selected phage were compared using Easyfig. Checkerboard test of phage HZY2308 in combination with tigecycline (TGC) was performed to investigate their synergistic effect and bactericidal kinetics. The effect of HZY2308 on biofilm was investigated by semi-quantitative staining of biofilm with crystal violet, determination of bacterial activity in biofilm by 2,3-Bis (2-methoxy-4-nitro-5-sulfophenyl) -2 H-tetrazolium-5-carboxanilide (XTT) assay and observation of biofilm structure by fluorescence microscopy. Finally, Phage-resistant bacteria AB48-R were characterized by colony-forming capacity, morphology, growth curves, adsorption efficiency, and antibiotic susceptibility assays.

Results: A lytic phage, HZY2308, was isolated from hospital sewage, which exhibited advantageous traits such as a brief incubation period, large burst size, and robust stability. Safety assessments conducted at both genetic and cellular levels also have yielded positive outcomes. Besides, phage HZY2308 effectively inhibited AB biofilm formation and disrupted established biofilm structures. Furthermore, a synergistic antibacterial effect was noted when phage HZY2308 was combined with tigecycline. Interestingly, the phage-resistant strain, AB48-R was screened through natural selection. Compared to the wild strain AB48, the adsorption efficiency of the phage to AB48-R diminished. However, AB48-R's sensitivity to antibiotics such as cefepime, gentamicin, amikacin, and tobramycin increased, indicating an evolutionary trade-off.

Conclusions: Phage HZY2308 shows strong antimicrobial potential, especially in combination with tigecycline, and the phage-resistant strain exhibits increased antibiotic sensitivity.

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来源期刊
Virology Journal
Virology Journal 医学-病毒学
CiteScore
7.40
自引率
2.10%
发文量
186
审稿时长
1 months
期刊介绍: Virology Journal is an open access, peer reviewed journal that considers articles on all aspects of virology, including research on the viruses of animals, plants and microbes. The journal welcomes basic research as well as pre-clinical and clinical studies of novel diagnostic tools, vaccines and anti-viral therapies. The Editorial policy of Virology Journal is to publish all research which is assessed by peer reviewers to be a coherent and sound addition to the scientific literature, and puts less emphasis on interest levels or perceived impact.
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