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M247无细胞上清液的活性:一种有前景的治疗阴道感染的方法。

The activity of cell-free supernatant of M247: a promising treatment against vaginal infections.

作者信息

Santarelli Giulia, Rosato Roberto, Cicchinelli Michela, Iavarone Federica, Urbani Andrea, Sanguinetti Maurizio, Delogu Giovanni, De Maio Flavio

机构信息

Dipartimento di Scienze Biotecnologiche di Base, Cliniche Intensivologiche e Perioperatorie, Università Cattolica del Sacro Cuore, Rome, Italy.

Dipartimento di Scienze di Laboratorio ed Ematologiche, Fondazione Policlinico Universitario A. Gemelli IRCCS, Rome, Italy.

出版信息

Front Cell Infect Microbiol. 2025 Jun 11;15:1586442. doi: 10.3389/fcimb.2025.1586442. eCollection 2025.

Abstract

is renowned for its antimicrobial properties, and some strains are used to treat vaginal dysbiosis, although the mechanisms underlying the antimicrobial properties remain elusive. We isolated M247 (LcM247) from a commercially available probiotic product Crispact and tested its antimicrobial activity against selected pathobionts such as , , , , and using both cocultures and testing the antimicrobial activity of cell-free supernatant (CFS) obtained from the culture of the probiotic strain. Furthermore, we demonstrate that CFS antimicrobial activity is pH dependent and that it is not affected by temperature and proteinase K treatment. Proteomic analysis suggests that this activity is mediated by S-layer secreted proteins. In a series of infection models, we infected Henrietta Lacks' cervical eukaryotic cancer cells (HeLa) with , and at specific multiplicities of infection (MOIs) before the administration of LcM247, CFS, gentamicin or fluconazole alone or in combination with LcM247/CFS. We observed a slight decrease in the microbial burden following LcM247 administration, while treatment with CFS significantly reduced microbial growth compared to control and antimicrobial compounds. These results highlight the antimicrobial properties of LcM247 and its CFS and the likely mechanism of action that contributes to the eradication of common pathobionts. We show that actively replicating LcM247 is less efficient than its CFS, so the oral administration of LcM247 may result in treatment failure. Finally, the use of CFS may result in an upswing of the host strains and promote the engraftment of probiotic treatments.

摘要

以其抗菌特性而闻名,一些菌株被用于治疗阴道生态失调,尽管其抗菌特性背后的机制仍然难以捉摸。我们从市售益生菌产品Crispact中分离出M247(LcM247),并使用共培养以及测试从益生菌菌株培养物中获得的无细胞上清液(CFS)的抗菌活性,来检测其对选定的病理共生菌如[具体菌名缺失]、[具体菌名缺失]、[具体菌名缺失]、[具体菌名缺失]、[具体菌名缺失]和[具体菌名缺失]的抗菌活性。此外,我们证明CFS的抗菌活性是pH依赖性的,并且不受温度和蛋白酶K处理的影响。蛋白质组学分析表明,这种活性是由S层分泌蛋白介导的。在一系列感染模型中,我们在单独或与LcM247/CFS联合给予LcM247、CFS、庆大霉素或氟康唑之前,以特定的感染复数(MOI)用[具体菌名缺失]、[具体菌名缺失]和[具体菌名缺失]感染海瑞塔·拉克斯的宫颈真核癌细胞(HeLa)。我们观察到给予LcM247后微生物负荷略有下降,而与对照和抗菌化合物相比,用CFS处理显著降低了微生物生长。这些结果突出了LcM247及其CFS的抗菌特性以及有助于根除常见病理共生菌的可能作用机制。我们表明,活跃复制的LcM247比其CFS效率低,因此口服LcM247可能导致治疗失败。最后,使用CFS可能导致宿主[具体菌名缺失]菌株增加,并促进[具体菌名缺失]益生菌治疗的植入。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4f32/12187682/db3fda41d729/fcimb-15-1586442-g001.jpg

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