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一种新型大肠杆菌噬菌体与抗生素在化学计量生态位中协同抑制尿路致病性菌株CFT073的生长。

A novel coli myophage and antibiotics synergistically inhibit the growth of the uropathogenic strain CFT073 in stoichiometric niches.

作者信息

Khunti Patiphan, Chantakorn Kittapart, Tantibhadrasapa Arishabhas, Htoo Htut Htut, Thiennimitr Parameth, Nonejuie Poochit, Chaikeeratisak Vorrapon

机构信息

Department of Biochemistry, Faculty of Science, Chulalongkorn University , Bangkok, Thailand.

Institute of Molecular Biosciences, Mahidol University , Nakhon Pathom, Thailand.

出版信息

Microbiol Spectr. 2023 Sep 21;11(5):e0088923. doi: 10.1128/spectrum.00889-23.

Abstract

Urinary tract infections are widespread bacterial infections affecting millions of people annually, with being the most prevalent. Although phage therapy has recently gained interest as a promising alternative therapy for antibiotic-resistant bacteria, several studies have raised concerns regarding the evolution of phage resistance, making the therapy ineffective. In this study, we discover a novel coli myophage designated as Killian that targets strains, including the uropathogenic (UPEC) strain CFT073. It requires at least 20 minutes for 90% of its particles to adsorb to the host cells, undergoes subcellular activities for replication for 30 minutes, and eventually lyses the cells with a burst size of about 139 particles per cell. Additionally, Killian can withstand a wide variety of temperatures (4-50°C) and pHs (4-10). Genome analysis reveals that Killian's genome consists of 169,905 base pairs with 35.5% GC content, encoding 276 open reading frames; of these, 209 are functionally annotated with no undesirable genes detected, highlighting its potential as an antibiotic alternative against UPEC. However, after an 8-hour phage treatment at high multiplicities of infection, bacterial density continuously increases, indicating an onset of bacterial growth revival. Thus, the combination study between the phage and three different antibiotics, including amikacin, ciprofloxacin, and piperacillin, was performed and showed that certain pairs of phage and antibiotics exhibited synergistic interactions in suppressing the bacterial growth revival. These findings suggest that Killian-antibiotic combinations are effective in inhibiting the growth of UPEC. IMPORTANCE Phage therapy has recently been in the spotlight as a viable alternative therapy for bacterial infections. However, several studies have raised concerns about the emergence of phage resistance that occurs during treatment, making the therapy not much effective. Here, we present the discovery of a novel myophage that, by itself, can effectively kill the uropathogenic , but the emergence of bacterial growth revival was detected during the treatment. Phage and antibiotics are then combined to improve the efficiency of the phage in suppressing the bacterial re-growth. This research would pave the way for the future development of phage-antibiotic cocktails for the sustainable use of phages for therapeutic purposes.

摘要

尿路感染是一种广泛存在的细菌感染,每年影响数百万人,其中[具体细菌名称]最为常见。尽管噬菌体疗法最近作为一种针对抗生素耐药菌的有前景的替代疗法而受到关注,但多项研究对噬菌体耐药性的演变提出了担忧,导致该疗法无效。在本研究中,我们发现了一种新型大肠杆菌噬菌体,命名为基利安(Killian),它靶向[具体细菌名称]菌株,包括尿路致病性大肠杆菌(UPEC)菌株CFT073。其至少90%的颗粒需要20分钟才能吸附到宿主细胞上,进行30分钟的亚细胞复制活动,最终以每个细胞约139个颗粒的爆发量裂解细胞。此外,基利安能耐受多种温度(4 - 50°C)和pH值(4 - 10)。基因组分析表明,基利安的基因组由169,905个碱基对组成,GC含量为35.5%,编码276个开放阅读框;其中209个在功能上有注释,未检测到不良基因,突出了其作为对抗UPEC的抗生素替代品的潜力。然而,在高感染复数下进行8小时的噬菌体处理后,细菌密度持续增加,表明细菌生长复苏开始。因此,开展了噬菌体与三种不同抗生素(包括阿米卡星、环丙沙星和哌拉西林)的联合研究,结果表明特定的噬菌体 - 抗生素组合在抑制细菌生长复苏方面表现出协同相互作用。这些发现表明,基利安 - 抗生素组合可有效抑制UPEC的生长。重要性噬菌体疗法最近作为一种可行的细菌感染替代疗法受到关注。然而,多项研究对治疗过程中出现的噬菌体耐药性提出了担忧,使该疗法效果不佳。在此,我们展示了一种新型[具体细菌名称]噬菌体的发现,它本身可以有效杀死尿路致病性[具体细菌名称],但在治疗过程中检测到细菌生长复苏的出现。然后将噬菌体与抗生素联合使用,以提高噬菌体抑制细菌再生长的效率。这项研究将为未来开发噬菌体 - 抗生素鸡尾酒疗法铺平道路,以便可持续地将噬菌体用于治疗目的。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/97e2/10580823/79a5ea45555f/spectrum.00889-23.f001.jpg

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