Biological characterization of the phage lysin AVPL and its efficiency against Aerococcus viridans-induced mastitis in a murine model.

IF 3.9 2区 生物学 Q2 BIOTECHNOLOGY & APPLIED MICROBIOLOGY Applied and Environmental Microbiology Pub Date : 2024-08-21 Epub Date: 2024-07-16 DOI:10.1128/aem.00461-24
Hengyu Xi, Yalu Ji, Yao Fu, Chong Chen, Wenyu Han, Jingmin Gu
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Abstract

Aerococcus viridans (A. viridans) is an important opportunistic zoonotic pathogen that poses a potential threat to the animal husbandry industry, such as cow mastitis, due to the widespread development of multidrug-resistant strains. Phage lysins have emerged as a promising alternative antibiotic treatment strategy. However, no lysins have been reported to treat A. viridans infections. In this study, the critical active domain and key active sites of the first A. viridans phage lysin AVPL were revealed. AVPL consists of an N-terminal N-acetylmuramoyl-L-alanine amidase catalytic domain and a C-terminal binding domain comprising two conserved LysM. H40, N44, E52, W68, H147, T157, F60, F64, I77, N92, Q97, H159, V160, D161, and S42 were identified as key sites for maintaining the activity of the catalytic domain. The LysM motif plays a crucial role in binding AVPL to bacterial cell wall peptidoglycan. AVPL maintains stable activity in the temperature range of 4-45°C and pH range of 4-10, and its activity is independent of the presence of metal ions. In vitro, the bactericidal effect of AVPL showed efficient bactericidal activity in milk samples, with 2 µg/mL of AVPL reducing A. viridans by approximately 2 Log10 in 1 h. Furthermore, a single dose (25 µg) of lysin AVPL significantly reduces bacterial load (approximately 2 Log10) in the mammary gland of mice, improves mastitis pathology, and reduces the concentration of inflammatory cytokines (TNF-α, IL-1β, and IL-6) in mammary tissue. Overall, this work provides a novel alternative therapeutic drug for mastitis induced by multidrug-resistant A. viridans.

Importance: A. viridans is a zoonotic pathogen known to cause various diseases, including mastitis in dairy cows. In recent years, there has been an increase in antibiotic-resistant or multidrug-resistant strains of this pathogen. Phage lysins are an effective approach to treating infections caused by multidrug-resistant strains. This study revealed the biological properties and key active sites of the first A. viridans phage lysin named AVPL. AVPL can effectively kill multidrug-resistant A. viridans in pasteurized whole milk. Importantly, 25 μg AVPL significantly alleviates the symptoms of mouse mastitis induced by A. viridans. Overall, our results demonstrate the potential of lysin AVPL as an antimicrobial agent for the treatment of mastitis caused by A. viridans.

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噬菌体溶菌酶 AVPL 的生物学特性及其在小鼠模型中对病毒性厌氧球菌诱发的乳腺炎的防治效果。
病毒性厌氧球菌(A. viridans)是一种重要的机会性人畜共患病原体,由于耐多药菌株的广泛发展,它对畜牧业(如奶牛乳腺炎)构成了潜在威胁。噬菌体溶菌素已成为一种很有前景的替代抗生素治疗策略。然而,目前还没有关于溶菌素可治疗病毒性甲沟炎感染的报道。本研究揭示了第一个A. viridans噬菌体溶菌素AVPL的关键活性域和关键活性位点。AVPL 由 N 端 N-acetylmuramoyl-L-alanine amidase 催化结构域和 C 端结合结构域组成,结合结构域包括两个保守的 LysM.H40、N44、E52、W68、H147、T157、F60、F64、I77、N92、Q97、H159、V160、D161 和 S42 被鉴定为维持催化域活性的关键位点。LysM 基序在 AVPL 与细菌细胞壁肽聚糖结合过程中起着关键作用。AVPL 在 4-45°C 的温度范围和 4-10 的 pH 值范围内都能保持稳定的活性,而且其活性与金属离子的存在无关。此外,单剂量(25 µg)的溶菌素 AVPL 能显著减少小鼠乳腺中的细菌量(约 2 Log10),改善乳腺炎病理,并降低乳腺组织中炎症细胞因子(TNF-α、IL-1β 和 IL-6)的浓度。总之,这项研究为耐多药病毒性甲沟炎引起的乳腺炎提供了一种新的替代治疗药物:A.viridans是一种人畜共患的病原体,可引起多种疾病,包括奶牛乳腺炎。近年来,这种病原体的抗生素耐药株或多重耐药株有所增加。噬菌体溶菌素是治疗耐多药菌株引起的感染的有效方法。这项研究揭示了第一个名为 AVPL 的 A. viridans 噬菌体溶菌素的生物学特性和关键活性位点。AVPL 能有效杀灭巴氏杀菌全脂牛奶中的耐多药病毒株。重要的是,25 μg AVPL 能明显缓解病毒性阿米巴痢疾杆菌诱发的小鼠乳腺炎症状。总之,我们的研究结果证明了溶菌素 AVPL 作为一种抗菌剂治疗由病毒性花叶病毒引起的乳腺炎的潜力。
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来源期刊
Applied and Environmental Microbiology
Applied and Environmental Microbiology 生物-生物工程与应用微生物
CiteScore
7.70
自引率
2.30%
发文量
730
审稿时长
1.9 months
期刊介绍: Applied and Environmental Microbiology (AEM) publishes papers that make significant contributions to (a) applied microbiology, including biotechnology, protein engineering, bioremediation, and food microbiology, (b) microbial ecology, including environmental, organismic, and genomic microbiology, and (c) interdisciplinary microbiology, including invertebrate microbiology, plant microbiology, aquatic microbiology, and geomicrobiology.
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