Literature DB >> 33813547

Associations Between Dysmenorrhea Symptom-Based Phenotypes and Vaginal Microbiome: A Pilot Study.

Chen X Chen, Janet S Carpenter, Xiang Gao, Evelyn Toh, Qunfeng Dong, David E Nelson, Caroline Mitchell, J Dennis Fortenberry.   

Abstract

BACKGROUND: Dysmenorrhea is highly prevalent; it places women at risk for other chronic pain conditions. There is a high degree of individual variability in menstrual pain severity, the number of painful sites, and co-occurring gastrointestinal symptoms. Distinct dysmenorrhea symptom-based phenotypes were previously identified, but the biological underpinnings of these phenotypes are less known. One underexplored contributor is the vaginal microbiome. The vaginal microbiota differs significantly among reproductive-age women and may modulate as well as amplify reproductive tract inflammation, which may contribute to dysmenorrhea symptoms.
OBJECTIVES: The objective of this study was to examine associations between dysmenorrhea symptom-based phenotypes and vaginal microbiome compositions on- and off-menses.
METHODS: We conducted a prospective, longitudinal, pilot study of 20 women (aged 15-24 years) grouped into three dysmenorrhea symptom-based phenotypes: "mild localized pain," "severe localized pain," and "severe multiple pain and gastrointestinal symptoms." Over one menstrual cycle, participants provided vaginal swabs when they were on- and off-menses. We assayed the vaginal microbiome using 16S rRNA gene sequencing. Permutational multivariate analysis of variance tests were used to compare microbiome compositions across phenotypes, with heat maps generated to visualize the relative abundance of bacterial taxa.
RESULTS: The vaginal microbiome compositions (n = 40) were different across the three phenotypes. After separating the on-menses (n = 20) and off-menses (n = 20) specimens, the statistically significant difference was seen on-menses, but not off-menses. Compared to the "mild localized pain" phenotype, participants in the "multiple severe symptoms" phenotype had a lower lactobacilli level and a higher abundance of Prevotella, Atopobium, and Gardnerella when on-menses. We also observed trends of differences across phenotypes in vaginal microbiome change from off- to on-menses. DISCUSSION: The study provides proof-of-concept data to support larger studies on associations between dysmenorrhea symptom-based phenotypes and vaginal microbiome that might lead to new intervention targets and/or biomarkers for dysmenorrhea. This line of research has the potential to inform precision dysmenorrhea treatment that can improve women's quality of life.
Copyright © 2021 Wolters Kluwer Health, Inc. All rights reserved.

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Year:  2021        PMID: 33813547      PMCID: PMC8222084          DOI: 10.1097/NNR.0000000000000510

Source DB:  PubMed          Journal:  Nurs Res        ISSN: 0029-6562            Impact factor:   2.381


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2.  Bacteria in the vaginal microbiome alter the innate immune response and barrier properties of the human vaginal epithelia in a species-specific manner.

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4.  Perceived Ineffectiveness of Pharmacological Treatments for Dysmenorrhea.

Authors:  Chen X Chen; Janet S Carpenter; Michelle LaPradd; Susan Ofner; J Dennis Fortenberry
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Review 5.  Self-report pain and symptom measures for primary dysmenorrhoea: a critical review.

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7.  Endogenous levels of prostaglandin F2alpha and its main metabolites in plasma and endometrium of normal and dysmenorrheic women.

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8.  Metabolic signatures of bacterial vaginosis.

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9.  phyloseq: an R package for reproducible interactive analysis and graphics of microbiome census data.

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10.  Characterization of the vaginal microbiota of healthy Canadian women through the menstrual cycle.

Authors:  Bonnie Chaban; Matthew G Links; Teenus Paramel Jayaprakash; Emily C Wagner; Danielle K Bourque; Zoe Lohn; Arianne Yk Albert; Julie van Schalkwyk; Gregor Reid; Sean M Hemmingsen; Janet E Hill; Deborah M Money
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  1 in total

1.  Menstrual Cycle Variation in MRI-Based Quantification of Intraluminal Gas in Women With and Without Dysmenorrhea.

Authors:  Hyeyoung Oh; Eli D Ehrenpreis; Frank F Tu; Katlyn E Dillane; Ellen F Garrison; Nondas Leloudas; Pottumarthi V Prasad; Kevin M Hellman
Journal:  Front Pain Res (Lausanne)       Date:  2022-05-11
  1 in total

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