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甲硝唑治疗通过对细菌性阴道病相关细菌而不是乳杆菌的作用,迅速减轻生殖器炎症。

Metronidazole treatment rapidly reduces genital inflammation through effects on bacterial vaginosis-associated bacteria rather than lactobacilli.

机构信息

Department of Medicine, University of Toronto, Toronto, Ontario, Canada.

Department of Obstetrics, Gynecology & Reproductive Sciences and.

出版信息

J Clin Invest. 2022 Mar 15;132(6). doi: 10.1172/JCI152930.

Abstract

BackgroundBacterial vaginosis (BV) causes genital inflammation and increases HIV risk, whereas a vaginal microbiota dominated by Lactobacillus species is associated with immune quiescence and relative HIV protection. BV treatment reduces genital inflammation, but it is unclear whether this reduction is driven by a decrease in BV-associated bacteria or an increase in Lactobacillus species.METHODSTo evaluate the short-term effect of standard BV treatment on genital immunology and the vaginal microbiota, vaginal swabs were collected immediately before and after metronidazole treatment for BV and analyzed with multiplex ELISA, metagenomic sequencing, and quantitative PCR.RESULTSTopical metronidazole treatment rapidly reduced vaginal levels of proinflammatory cytokines, chemokines, and soluble immune markers of epithelial barrier disruption. Although the vaginal microbiota shifted to dominance by L. iners or L. jensenii, this proportional shift was primarily driven by a 2 to 4 log10-fold reduction in BV-associated bacteria absolute abundance. BV treatment induced no change in the absolute abundance of L. crispatus or L. iners and only minor (<1 log10-fold) increases in L. gasseri and L. jensenii that were not independently associated with reduced inflammation in multivariable models.CONCLUSIONThe genital immune benefits that are associated with Lactobacillus dominance after BV treatment were not directly attributable to an absolute increase in lactobacilli, but rather to the loss of BV-associated bacteria.Trial REGISTRATIONParticipants were recruited as part of a randomized controlled trial (ClinicalTrials.gov NCT02766023) from 2016 to 2019.FUNDINGCanadian Institutes of Health Research (PJT-156123) and the National Institute of Allergy and Infectious Diseases (HHSN2722013000141 and HHSN27200007).

摘要

背景

细菌性阴道病 (BV) 会引起生殖器炎症并增加 HIV 风险,而以乳杆菌属为主的阴道微生物群与免疫静止和相对 HIV 保护有关。BV 治疗可减少生殖器炎症,但尚不清楚这种减少是由 BV 相关细菌减少还是乳杆菌属增加引起的。

方法

为了评估标准 BV 治疗对生殖器免疫学和阴道微生物群的短期影响,在甲硝唑治疗 BV 前后立即采集阴道拭子,并通过多重 ELISA、宏基因组测序和定量 PCR 进行分析。

结果

局部甲硝唑治疗可迅速降低阴道中促炎细胞因子、趋化因子和上皮屏障破坏的可溶性免疫标志物水平。尽管阴道微生物群向 L. iners 或 L. jensenii 主导转变,但这种比例的转变主要是由 BV 相关细菌绝对丰度降低 2 到 4 个对数级驱动的。BV 治疗未引起 L. crispatus 或 L. iners 的绝对丰度变化,仅引起 L. gasseri 和 L. jensenii 略有增加(<1 个对数级),且在多变量模型中与炎症减少无关。

结论

与 BV 治疗后乳杆菌属主导相关的生殖器免疫益处并非直接归因于乳杆菌属的绝对增加,而是归因于 BV 相关细菌的丧失。

试验注册

参与者作为随机对照试验(ClinicalTrials.gov NCT02766023)的一部分于 2016 年至 2019 年招募。

资金

加拿大卫生研究院(PJT-156123)和美国国立过敏和传染病研究所(HHSN2722013000141 和 HHSN27200007)。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/73d9/8920324/7565fe21abe8/jci-132-152930-g095.jpg

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