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. 2024 May;41(S 01):e2539-e2546.
doi: 10.1055/s-0043-1772226. Epub 2023 Aug 9.

Cervicovaginal Microbial-Immune State and Group B Streptococcus Colonization in Pregnancy

Jennifer A McCoy  1 Heather H Burris  1   2 Kristin D Gerson  1 Clare McCarthy  1 Jacques Ravel  3 Michal A Elovitz  4
Affiliations

Cervicovaginal Microbial-Immune State and Group B Streptococcus Colonization in Pregnancy

Jennifer A McCoy et al. Am J Perinatol. 2024 May.

Abstract

Objective: Maternal colonization with Group B Streptococcus (GBS) is a significant risk factor for serious neonatal morbidity. There are limited data on how the cervicovaginal (CV) microbiota and host immune factor β-defensin-2 might influence GBS colonization in pregnant individuals. This study sought to determine if the CV microbiota is associated with GBS colonization in pregnant individuals, and if β-defensin-2 modifies this relationship.

Study design: This was a secondary analysis of a prospective cohort study of pregnant individuals with singleton pregnancies who had CV microbiota specimens analyzed at 16 to 20, 20 to 24, and 24 to 28 weeks' gestation, along with a third trimester GBS rectovaginal (RV) culture (n = 492). Microbiota data were analyzed with 16S rRNA gene sequencing and classified into community state types (CSTs). Log-binomial multivariable regression was used to model associations between CST and GBS RV status and to calculate risk ratios. β-defensin-2, an immune factor known to modulate the relationship between CST and pregnancy outcomes, was examined as an effect modifier.

Results: Of 492 individuals, 34.3% were GBS RV + . Compared with individuals with CST I at 16 to 20 weeks, individuals with CST IV-A and CST II had a significantly elevated relative risk of subsequent GBS RV+ status. When stratified by high and low β-defensin-2 levels, β-defensin-2 was found to be an effect modifier of the association between CST IV-A and GBS RV+ status. In individuals with low β-defensin-2 levels, CST VI-A was associated with GBS RV+ status, but among individuals with high β-defensin-2 levels, there was no such association (interaction p-value = 0.03).

Conclusion: Pregnant individuals with CV microbiota characterized by CST IV-A and CST II had significantly elevated risk of GBS RV colonization in the third trimester compared with those with CST I, and β-defensin-2 was an effect modifier of the association between CST IV-A and GBS RV+ status. Future research should investigate if manipulation of the CV microbiota can prevent GBS colonization, thereby reducing intrapartum antibiotic prophylaxis and the risks of neonatal GBS infection.

Key points: · The relationship between the CV microbiota and GBS RV colonization is unknown.. · A Lactobacillus-deficient, anaerobic rich vaginal community, CST IV-A, is associated with increased risk of GBS RV colonization.. · β-defensin-2 is an effect modifier of the association between CST IV-A and GBS RV+ status..

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Conflict of interest statement

None declared.

Figures

Fig. 1
Fig. 1
Study enrollment flow chart. GBS, Group B Streptococcus; RV, rectovaginal.
Fig. 2
Fig. 2
Forest plot showing the association between CST and GBS RV +, stratified by βD (n = 491)*. *n = 1 individual in cohort missing βD value. βD, β-defensin; CST, community state type; GBS, Group B Streptococcus; RV, rectovaginal.
See this image and copyright information in PMC

References

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