Simultaneous Profiling of Sexually Transmitted Bacterial Pathogens, Microbiome, and Concordant Host Response in Cervical Samples Using Whole Transcriptome Sequencing Analysis

Overview

Journal Microb Cell

Specialty Microbiology

Date 2019 Mar 12

PMID 30854394

Citations 6

Authors

Catherine M OConnell

Hayden Brochu

Jenna Girardi

Erin Harrell

Aiden Jones

Toni Darville

Arlene C Sena

Xinxia Peng

Affiliations

Soon will be listed here.

Abstract

Pelvic inflammatory disease (PID) is a female upper genital tract inflammatory disorder that arises after sexually transmitted bacterial infections (STI). Factors modulating risk for reproductive sequelae include co-infection, microbiota, host genetics and physiology. In a pilot study of cervical samples obtained from women at high risk for STIs, we examined the potential for unbiased characterization of host, pathogen and microbiome interactions using whole transcriptome sequencing analysis of ribosomal RNA-depleted total RNAs (Total RNA-Seq). Only samples from women with STI infection contained pathogen-specific sequences (3 to 38% transcriptome coverage). Simultaneously, we identified and quantified their active microbial communities. After integration with host-derived reads from the same data, we detected clustering of host transcriptional profiles that reflected microbiome differences and STI infection. Together, our study suggests that total RNA profiling will advance understanding of the interplay of pathogen, host and microbiota during natural infection and may reveal novel, outcome-relevant biomarkers.

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