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标准细菌性阴道病治疗后阴道免疫持久效应:乳酸杆菌 crispatus CTV-05(LACTIN-V)的随机、安慰剂对照试验结果。

Sustained effect of LACTIN-V (Lactobacillus crispatus CTV-05) on genital immunology following standard bacterial vaginosis treatment: results from a randomised, placebo-controlled trial.

机构信息

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

Department of Obstetrics, Gynecology, and Reproductive Sciences, University of California, San Francisco, CA, USA.

出版信息

Lancet Microbe. 2022 Jun;3(6):e435-e442. doi: 10.1016/S2666-5247(22)00043-X. Epub 2022 Apr 21.

Abstract

BACKGROUND

Bacterial vaginosis might increase HIV risk by eliciting genital inflammation and epithelial barrier disruption, whereas vaginal Lactobacillus crispatus is associated with immune quiescence and HIV protection. We investigated the effect of a live biotherapeutic containing L crispatus CTV-05 (LACTIN-V) on genital immunology and key vaginal bacteria.

METHODS

This substudy included women aged 18-45 years who participated in the randomised, placebo-controlled, phase 2b trial of LACTIN-V to reduce bacterial vaginosis recurrence, conducted at four universities and hospitals in the USA. Women with negative results for sexually transmitted infection, pregnancy, and urinary tract infection were provided a 5-day course of vaginal metronidazole 0·75% gel. Those who met at least three of four clinical Amsel criteria for bacterial vaginosis and had a Nugent score of 4-10 from Gram staining were eligible. Participants in the LACTIN-V trial were randomly assigned (2:1) to receive either LACTIN-V or placebo, applied vaginally once per day for 5 days during the first week and then twice per week for 10 more weeks. Follow-up visits occurred 4, 8, 12, and 24 weeks after enrolment. Soluble immune factors and the absolute abundance of bacterial taxa were assayed by mutliplex ELISA and quantitative PCR. The primary outcomes were vaginal levels of IL-1α and soluble E-cadherin at 24 weeks (ie, 13 weeks after treatment cessation).

FINDINGS

Between Feb 21, 2020 and March 18, 2021, we characterised genital immune parameters and the vaginal microbiota in a subset of 66 highly adherent participants who were randomly selected, with no exclusion criteria, from those who had attended all study follow-up visits (n=166) in the larger LACTIN-V clinical trial (n=288). 32 (48%) participants received LACTIN-V and 34 (52%) received placebo. LACTIN-V treatment was significantly associated with lower concentrations of the proinflammatory cytokine IL-1α (β coefficient 0·310, SE 0·149; p=0·042) and soluble E-cadherin (0·429, 0·199; p=0·035), a biomarker of epithelial barrier disruption.

INTERPRETATION

Vaginal administration of LACTIN-V following standard bacterial vaginosis therapy resulted in a sustained reduction in genital inflammation and a biomarker of epithelial integrity. The potential of LACTIN-V to reduce HIV susceptibility merits further investigation.

FUNDING

Canadian Institutes of Health Research and the National Institutes of Health National Institute of Allergy and Infectious Diseases.

摘要

背景

细菌性阴道病可能通过引发生殖器炎症和上皮屏障破坏来增加 HIV 风险,而阴道中的乳酸杆菌 crispatus 与免疫静止和 HIV 保护有关。我们研究了含有乳酸杆菌 crispatus CTV-05(LACTIN-V)的活菌生物治疗对生殖器免疫和关键阴道细菌的影响。

方法

本亚研究纳入了年龄在 18-45 岁之间的女性,她们参加了一项在美国四所大学和医院进行的、针对 LACTIN-V 降低细菌性阴道病复发的随机、安慰剂对照、2b 期试验。对性传播感染、怀孕和尿路感染检测呈阴性的女性给予 5 天阴道用甲硝唑 0.75%凝胶治疗。那些至少符合四项细菌性阴道病 Amsel 临床标准中的三项,且革兰氏染色的 Nugent 评分在 4-10 分之间的女性有资格参加。LACTIN-V 试验的参与者被随机分配(2:1)接受 LACTIN-V 或安慰剂,在第一周每天阴道给药一次,共 5 天,然后每周两次,共 10 周。在入组后 4、8、12 和 24 周进行随访。通过多重 ELISA 和定量 PCR 检测可溶性免疫因子和细菌分类群的绝对丰度。主要结局是 24 周(即治疗停止后 13 周)时阴道中 IL-1α 和可溶性 E-钙黏蛋白的水平。

结果

在 2020 年 2 月 21 日至 2021 年 3 月 18 日期间,我们从更大的 LACTIN-V 临床试验(n=288)中所有研究随访的参与者(n=166)中随机选择了没有排除标准的 66 名高度依从性的参与者,对其进行了生殖器免疫参数和阴道微生物组的特征分析。32(48%)名参与者接受了 LACTIN-V 治疗,34(52%)名参与者接受了安慰剂治疗。LACTIN-V 治疗与促炎细胞因子 IL-1α(β系数 0.310,SE 0.149;p=0.042)和上皮屏障破坏的生物标志物可溶性 E-钙黏蛋白(0.429,0.199;p=0.035)的浓度降低显著相关。

解释

细菌性阴道病标准治疗后阴道给予 LACTIN-V 可导致生殖器炎症和上皮完整性生物标志物持续减少。LACTIN-V 降低 HIV 易感性的潜力值得进一步研究。

资助

加拿大卫生研究院和美国国立卫生研究院过敏和传染病研究所国家过敏和传染病研究所。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0832/9188188/d6bc83b422ac/nihms-1812593-f0001.jpg

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