临床收集的细菌性阴道病诊断样本中阴道微生物组的特征。

IF 3.7 2区 生物学 Q2 MICROBIOLOGY
Microbiology spectrum Pub Date : 2025-04-01 Epub Date: 2025-02-25 DOI:10.1128/spectrum.02582-24
Hayden N Brochu, Qimin Zhang, Kuncheng Song, Ling Wang, Emily A Deare, Jonathan D Williams, Crystal R Icenhour, Lakshmanan K Iyer
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引用次数: 0

摘要

细菌性阴道病(BV)是一种由细菌过度生长引起的阴道炎症,扰乱了阴道的健康微生物群。现有的细菌性阴道炎临床检测主要基于阴道分泌物的物理和显微镜检查。现代基于pcr的临床检测以bv相关微生物为目标,如Labcorp的NuSwab检测,其目标是阴道托泊菌(Fannyhessea)、Megasphaera-1和细菌性阴道病相关细菌(BVAB)-2。对临床收集的NuSwab阴道拭子进行DNA提取和16S V3-V4 rRNA基因测序,以分析除Labcorp NuSwab测试中包括的微生物外的微生物。利用每个样本中检测到的最丰富的分类群来确定群落状态类型(CSTs)。将NuSwab板微生物靶点的PCR结果与相应的微生物组谱进行比较。代谢途径丰度通过扩增子序列变异(asv)的宏基因组预测来表征。75份剩余阴道拭子16S V3-V4 rRNA基因测序得到492个独特的16S V3-V4 asv,鉴定83个独特属。NuSwab法与测序法的结果具有较强的一致性(P < 0.01)。CST-I(18 / 18, 100%)、CST-II(3 / 3, 100%)、CST-III(17 / 15, 88%)和CST-V(1 / 1, 100%)的样本通过NuSwab面板大部分被归类为bv阴性,而大多数CST-IV样本(36 / 28,78%)为bv阳性或bv不确定。bv相关的微生物和预测代谢特征在多个cst中共享。这些发现突出了Labcorp NuSwab基于测序的BV微生物定量,准确区分由不同乳酸菌主导的阴道微生物组CSTs,并扩大了BV相关细菌和代谢生物标志物的鉴定。细菌性阴道病(BV)对育龄期及以后的妇女造成了重大的健康负担。目前细菌性阴道炎的诊断要么依赖于选定的微生物组,要么依赖于技术人员的物理和显微镜评估。在这里,我们对先前通过Labcorp NuSwab测试诊断的样品的微生物组谱进行了测序,以更好地了解BV期间阴道微生物组的破坏。我们发现微生物测序可以忠实地再现目标PCR诊断结果,并可以提高我们对健康和bv相关微生物和代谢生物标志物的认识。这项工作强调了一个强大的、不可知的BV分类方案,具有未来发展基于测序的BV诊断工具的潜力。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Characterization of vaginal microbiomes in clinician-collected bacterial vaginosis diagnosed samples.

Bacterial vaginosis (BV) is a type of vaginal inflammation caused by bacterial overgrowth, upsetting the healthy microbiome of the vagina. Existing clinical testing for BV is primarily based upon physical and microscopic examination of vaginal secretions. Modern PCR-based clinical tests target panels of BV-associated microbes, such as the Labcorp NuSwab test that targets Atopobium (Fannyhessea) vaginae, Megasphaera-1, and Bacterial Vaginosis Associated Bacterium (BVAB)-2. Remnant clinician-collected NuSwab vaginal swabs underwent DNA extraction and 16S V3-V4 rRNA gene sequencing to profile microbes in addition to those included in the Labcorp NuSwab test. Community state types (CSTs) were determined using the most abundant taxon detected in each sample. PCR results for NuSwab panel microbial targets were compared against the corresponding microbiome profiles. Metabolic pathway abundances were characterized via metagenomic prediction from amplicon sequence variants (ASVs). 16S V3-V4 rRNA gene sequencing of 75 remnant vaginal swabs yielded 492 unique 16S V3-V4 ASVs, identifying 83 unique genera. NuSwab microbe quantification was strongly concordant with quantification by sequencing (P < 0.01). Samples in CST-I (18 of 18, 100%), CST-II (three of three, 100%), CST-III (15 of 17, 88%), and CST-V (one of one, 100%) were largely categorized as BV-negative via the NuSwab panel, while most CST-IV samples (28 of 36, 78%) were BV-positive or BV-indeterminate. BV-associated microbial and predicted metabolic signatures were shared across multiple CSTs. These findings highlight robust sequencing-based quantification of Labcorp NuSwab BV microbes, accurate discrimination of vaginal microbiome CSTs dominated by distinct Lactobacilli, and expanded the identification of BV-associated bacterial and metabolic biomarkers.IMPORTANCEBacterial vaginosis (BV) poses a significant health burden for women during reproductive years and onward. Current BV diagnostics rely on either panels of select microbes or on physical and microscopic evaluations by technicians. Here, we sequenced the microbiome profiles of samples previously diagnosed by the Labcorp NuSwab test to better understand disruptions to the vaginal microbiome during BV. We show that microbial sequencing can faithfully reproduce targeted PCR diagnostic results and can improve our knowledge of healthy and BV-associated microbial and metabolic biomarkers. This work highlights a robust, agnostic BV classification scheme with potential for future development of sequencing-based BV diagnostic tools.

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来源期刊
Microbiology spectrum
Microbiology spectrum Biochemistry, Genetics and Molecular Biology-Genetics
CiteScore
3.20
自引率
5.40%
发文量
1800
期刊介绍: Microbiology Spectrum publishes commissioned review articles on topics in microbiology representing ten content areas: Archaea; Food Microbiology; Bacterial Genetics, Cell Biology, and Physiology; Clinical Microbiology; Environmental Microbiology and Ecology; Eukaryotic Microbes; Genomics, Computational, and Synthetic Microbiology; Immunology; Pathogenesis; and Virology. Reviews are interrelated, with each review linking to other related content. A large board of Microbiology Spectrum editors aids in the development of topics for potential reviews and in the identification of an editor, or editors, who shepherd each collection.
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