The cervicovaginal microbiome is highly associated with women's health with microbial communities dominated by spp. being considered optimal. Conversely, a lack of lactobacilli and a high abundance of strict and facultative anaerobes including , have been associated with adverse reproductive outcomes. However, the molecular pathways modulated by microbe interactions with the cervicovaginal epithelia remain unclear. Using RNA-sequencing, we characterize the cervicovaginal epithelial transcriptional response to different vaginal bacteria and their culture supernatants. We showed that upregulated genes were associated with an activated innate immune response including anti-microbial peptides and inflammasome pathways, represented by NLRP3-mediated increases in caspase-1, IL-1β and cell death. Cervicovaginal epithelial cells exposed to showed limited transcriptomic changes, while exposure to culture supernatants resulted in a shift in the epigenomic landscape of cervical epithelial cells. ATAC-sequencing confirmed epigenetic changes with reduced chromatin accessibility. This study reveals new insight into host-microbe interactions in the lower reproductive tract and suggest potential therapeutic strategies leveraging the vaginal microbiome to improve reproductive health.

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http://www.ncbi.nlm.nih.gov/pmc/articles/PMC10680926PMC
http://dx.doi.org/10.21203/rs.3.rs-3580132/v1DOI Listing

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