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培养的人类阴道微生物群落影响阴道黏膜培养物中寨卡病毒和单纯疱疹病毒的复制。

Cultivated Human Vaginal Microbiome Communities Impact Zika and Herpes Simplex Virus Replication in Vaginal Mucosal Cultures.

作者信息

Amerson-Brown Megan H, Miller Aaron L, Maxwell Carrie A, White Mellodee M, Vincent Kathleen L, Bourne Nigel, Pyles Richard B

机构信息

Graduate School of Biomedical Sciences, The University of Texas Medical Branch at Galveston, Galveston, TX, United States.

Department of Pediatrics, The University of Texas Medical Branch at Galveston, Galveston, TX, United States.

出版信息

Front Microbiol. 2019 Jan 14;9:3340. doi: 10.3389/fmicb.2018.03340. eCollection 2018.

Abstract

The human vaginal microbiome (VMB) is a complex bacterial community that interacts closely with vaginal epithelial cells (VECs) impacting the mucosal phenotype and its responses to pathogenic insults. The VMB and VEC relationship includes nutrient exchange and regulation of signaling molecules that controls numerous host functions and defends against invading pathogens. To better understand infection and replication of sexually transmitted viral pathogens in the human vaginal mucosa we used our VEC multilayer culture system. We tested the hypothesis that selected VMB communities could be identified that alter the replication of sexually transmitted viruses consistent with reported clinical associations. Sterile VEC multilayer cultures or those colonized with VMB dominated by specific spp., or VMB lacking lactobacilli, were infected with Zika virus, (ZIKV) a single stranded RNA virus, or Herpes Simplex Virus type 2 (HSV-2), a double stranded DNA virus. The virus was added to the apical surface of the cultured VEC multilayer to model transmission during vaginal intercourse. Viral replication was measured 48 h later by qPCR. The results indicated that VEC cultures colonized by VMB containing spp., previously reported as inflammatory, significantly reduced the quantity of viral genomes produced by ZIKV. HSV-2 titers were decreased by nearly every VMB tested relative to the sterile control, although spp.-dominated VMBs caused the greatest reduction in HSV-2 titer consistent with clinical observations. To explore the mechanism for reduced ZIKV titers, we investigated inflammation created by ZIKV infection, VMB colonization or pre-exposure to selected TLR agonists. Finally, expression levels of human beta defensins 1-3 were quantified in cultures infected by ZIKV and those colonized by VMBs that impacted ZIKV titers. Human beta defensins 1-3 produced by the VEC showed no association with ZIKV titers. The data presented expands the utility of this model system providing controlled and reproducible methods to study the VMB impact on STIs and indicated an association between viral replication and specific bacterial species within the VMB.

摘要

人类阴道微生物群(VMB)是一个复杂的细菌群落,与阴道上皮细胞(VEC)密切相互作用,影响黏膜表型及其对病原体侵袭的反应。VMB与VEC的关系包括营养物质交换和信号分子调节,这些信号分子控制着众多宿主功能并抵御入侵病原体。为了更好地理解性传播病毒病原体在人类阴道黏膜中的感染和复制情况,我们使用了VEC多层培养系统。我们检验了这样一个假设,即可以识别出特定的VMB群落,它们能够改变性传播病毒的复制情况,这与已报道的临床关联相符。用寨卡病毒(ZIKV,一种单链RNA病毒)或2型单纯疱疹病毒(HSV - 2,一种双链DNA病毒)感染无菌的VEC多层培养物,或感染以特定菌属为主导的VMB定植的培养物,或缺乏乳酸杆菌的VMB定植的培养物。将病毒添加到培养的VEC多层的顶端表面,以模拟阴道性交期间的传播过程。48小时后通过定量聚合酶链反应(qPCR)测量病毒复制情况。结果表明,被先前报道具有炎症性的含特定菌属的VMB定植的VEC培养物,显著降低了ZIKV产生的病毒基因组数量。相对于无菌对照,几乎每种测试的VMB都降低了HSV - 2滴度,尽管以特定菌属为主导的VMB导致HSV - 2滴度下降幅度最大,这与临床观察结果一致。为了探究ZIKV滴度降低的机制,我们研究了ZIKV感染、VMB定植或预先暴露于选定的Toll样受体(TLR)激动剂所引发的炎症反应。最后,对感染ZIKV的培养物以及被影响ZIKV滴度的VMB定植的培养物中的人β - 防御素1 - 3的表达水平进行了定量分析。VEC产生的人β - 防御素1 - 3与ZIKV滴度无关。所呈现的数据扩展了该模型系统的实用性,提供了可控且可重复的方法来研究VMB对性传播感染的影响,并表明了病毒复制与VMB内特定细菌种类之间的关联。

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