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乳酸杆菌对泌尿生殖道生物膜的破坏。

Disruption of urogenital biofilms by lactobacilli.

机构信息

Human Microbiology and Probiotics, Lawson Health Research Institute, London, Ontario N6A 4V2, Canada.

出版信息

Colloids Surf B Biointerfaces. 2011 Aug 1;86(1):58-64. doi: 10.1016/j.colsurfb.2011.03.016. Epub 2011 Mar 23.

DOI:10.1016/j.colsurfb.2011.03.016
PMID:21497071
Abstract

The process that changes a relatively sparse vaginal microbiota of healthy women into a dense biofilm of pathogenic and potentially pathogenic bacteria is poorly understood. Likewise, the reverse step whereby an aberrant biofilm is displaced and returns to a healthy lactobacilli dominated microbiota is unclear. In order to study these phenomena, in vitro experiments were performed to examine the structure of biofilms associated with aerobic vaginosis, urinary tract infections, and bacterial vaginosis (BV). Uropathogenic Escherichia coli were able to form relatively thin biofilms within five days (6 μm height), while Atopobium vaginae and Gardnerella vaginalis formed thicker biofilms 12 μm in height within two days. Challenge of E. coli biofilms with lactobacilli did not result in pathogen displacement. However, the resulting thicker lactobacilli infused biofilms, caused significant E. coli killing. E. coli biofilms challenged with secreted products of L. rhamnosus GR-1 caused a marked decrease in cell density, and increased cell death. Similarly challenge of BV biofilms with lactobacilli infiltrated BV biofilms and caused bacterial cell death. Metronidazole produced holes in the biofilm but did not eradicate the organisms. The findings provide some evidence of how lactobacilli probiotics might interfere with an aberrant vaginal microbiota, and strengthen the position that combining probiotics with antimicrobials could better eradicate pathogenic biofilms.

摘要

健康女性相对稀疏的阴道微生物群转变为致病性和潜在致病性细菌密集生物膜的过程尚未得到很好的理解。同样,异常生物膜被取代并恢复为健康的乳杆菌主导的微生物群的反向步骤也不清楚。为了研究这些现象,进行了体外实验以检查与需氧性阴道炎、尿路感染和细菌性阴道病(BV)相关的生物膜的结构。尿路致病性大肠杆菌能够在五天内形成相对较薄的生物膜(6μm 高度),而 Atopobium vaginae 和 Gardnerella vaginalis 在两天内形成较厚的生物膜(12μm 高度)。用乳杆菌挑战大肠杆菌生物膜不会导致病原体移位。然而,由此产生的较厚的乳杆菌输注生物膜导致显著的大肠杆菌杀伤。用 L. rhamnosus GR-1 的分泌产物挑战大肠杆菌生物膜会导致细胞密度明显降低和细胞死亡增加。同样,用乳杆菌挑战 BV 生物膜会渗透到 BV 生物膜中并导致细菌细胞死亡。甲硝唑在生物膜中产生孔,但不能根除生物。这些发现为乳杆菌益生菌如何可能干扰异常阴道微生物群提供了一些证据,并加强了将益生菌与抗生素联合使用可以更好地根除致病生物膜的观点。

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