Abstract

Chlamydia trachomatis is among the most prevalent of sexually transmitted diseases. While Chlamydia infection is a reportable event and screening has increased over time, enhanced surveillance has not resulted in a reduction in the rate of infections, and Chlamydia infections frequently recur. The development of a preventative vaccine for Chlamydia may be the only effective approach for reducing infection and the frequency of pathological outcomes. Current vaccine research efforts involve time consuming and/or invasive approaches for assessment of disease state, and MRI presents a clinically translatable method for assessing infection and related pathology both quickly and non-invasively. Longitudinal T2-weighted MRI was performed over 63 days on both control or Chlamydia muridarum challenged mice, either with or without elementary body (EB) immunization, and gross necropsy was performed on day 65. A scoring system was developed to assess the number of regions affected by Chlamydia pathology and was used to document pathology over time and at necropsy. The scoring system documented increasing incidence of pathology in the unimmunized and challenged mice (significantly greater compared to the control and EB immunized-challenged groups) by 21 days post-challenge. No differences between the unchallenged and EB immunized-challenged mice were observed. MRI scores at Day 63 were consistently higher than gross necropsy scores at Day 65, although two of the three groups of mice showed no significant differences between the two techniques. In this work we describe the application of MRI in mice for the potential evaluation of disease pathology and sequelae caused by C. muridarum infection and this technique’s potential for evaluation of vaccines for Chlamydia.

Highlights

  • Chlamydia trachomatis is the most commonly reported disease in the United States and among the most prevalent of sexually transmitted diseases

  • Upon quantitative polymerase chain reaction (qPCR) evaluation of vaginal swab samples, 100% of the control mice were negative for C. muridarum infection at Days 7, 14, and 21

  • The elementary body (EB) immunized-challenged group had 50% of the mice infected at Day 7, 20% at Day 14, and 10% at Day 21. 100% of the naïve-challenged mice doi:10.1371/journal.pone.0160055.g001

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Summary

Introduction

Chlamydia trachomatis is the most commonly reported disease in the United States and among the most prevalent of sexually transmitted diseases. From 1999–2008, the prevalence of Chlamydia infection in sexually active females from 14–19 years of age was 6.8% [2]. While Chlamydia infection is a reportable event and screening has increased over time, enhanced surveillance has not resulted in a reduction in the rate of infections [3]. Ascending Chlamydia infection can lead to additional chronic disease sequelae that may include pelvic inflammatory disease (PID), ectopic pregnancy, or even tubal factor infertility (TFI) [5, 6]. Recurrent infections occur in up to 30% of women and may increase the risk of complications, and antibiotic treatment may enhance the recurrence of infection by limiting development of protective immune responses [7]

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