Azithromycin Failure in Mycoplasma genitalium Urethritis

We report significant failure rates (28%, 95% confidence interval 15%–45%) after administering 1 g azithromycin to men with Mycoplasma genitalium–positive nongonococcal urethritis. In vitro evidence supported reduced susceptibility of M. genitalium to macrolides. Moxifloxacin administration resulted in rapid symptom resolution and eradication of infection in all cases. These findings have implications for management of urethritis.


The Study
Cases were derived from a case-control study of acute NGU conducted from March 2004 to March 2005 at Melbourne Sexual Health Centre (MSHC), Australia (12). Participants completed a questionnaire, underwent examination, and had first-void urine samples analyzed by strand-displacement amplification (ProbeTec-ET CT-Amplified-DNA-Assay, Becton, Dickinson and Company, Sparks, MD, NJ, USA) for Chlamydia trachomatis and by polymerase chain reaction (PCR) for M. genitalium (13), herpes simplex viruses (HSV-1 and -2), Trichomonas vaginalis, Ureaplasma urealyticum and parvum, Gardnerella vaginalis, and adenoviruses (12). Culture of urethral samples in modified-Thayer-Martin medium was performed for Neisseria gonorrhoeae.
Men with M. genitalium infection were instructed regarding partner notification and reinfection and were asked to return for a test of cure (TOC) 1 month posttreatment. Men with persistent M. genitalium infection were given 1 g single dose of azithromycin or 1 g weekly for 3 doses, but after apparent failure of azithromycin therapy in 3 men without reinfection, participants with persistent infection were offered moxifloxacin, 400 mg daily for 10 days. Four urethral specimens from men for whom azithromycin therapy failed were inoculated into SP4 medium, frozen (-80°C), and shipped on dry ice to Statens Serum Institut, Denmark, for culture in Vero cells and antimicrobial drug susceptibility testing (6). M. genitalium strains in Vero cell culture were grown in the presence of different concentrations of antimicrobial drugs, and growth of M. genitalium was monitored by quantitative PCR for determination of MIC (6).
The Human Research and Ethics Committee of the Alfred Hospital, Victoria, approved the study. Data were stored in Microsoft Access and analyzed by using SPSS version 12 (SPSS Inc., Chicago, IL, USA). Ninety-five percent confidence intervals (CIs) were calculated for proportions, which were compared by using the Fisher exact test. Patients were excluded from the analysis when information or specimens were not available.
M. genitalium was detected in 31(9.4%) of 329 patients (95% CI 6.6%-12.9%) and 3 of 307 controls. No patients with M. genitalium infection had other pathogens detected (12). Men with M. genitalium had a median age of 33 years (range 22-54 years); 25 were heterosexual, and 9 were homosexual (behavioral and clinical data are presented elsewhere [12]). Six female and 4 male asymptomatic sexual contacts of M. genitalium-infected men were tested; a throat and anal sample in 1 man and a cervical sample in 1 woman were positive for M. genitalium. Contacts were presumptively treated with 1 g single dose of azithromycin; however, the infected male contact required moxifloxacin after azithromycin treatment failed in this patient and in the index patient.
The 4 TOC specimens from men with azithromycin failure available for culture yielded growth of M. genitalium. Antimicrobial drug susceptibility testing showed increased MICs to macrolides: azithromycin >8 mg/L, erythromycin >32 mg/L, and clarithromycin >32 mg/L. All isolates were susceptible to moxifloxacin (MIC range 0.031-0.125 mg/L) and could be considered susceptible to doxycycline (MIC range 0.125-0.25 mg/L). However, correlates between in vitro MICs and treatment efficacy have not yet been established.

Conclusions
The azithromycin failure rate in M. genitalium-positive NGU was 28% (15%-45%) in this study and was associated with recurrent urethral symptoms in 8 of 9 cases. Longer course azithromycin ameliorated but did not resolve symptoms or eradicate infection, whereas moxifloxacin resulted in rapid symptom resolution and eradicated infection. Symptom improvement followed by recrudescence has been reported after levofloxacin failure (9). Culture of M. genitalium from all 4 specimens, and reduced susceptibility to azithromycin in vitro, demonstrates that azithromycin-resistance rather than reinfection caused treatment failure and that nonviable DNA was not the reason for a persistently positive PCR. The availability of strains in pure culture will enable investigation into resistance mechanisms, and work in progress indicates that mutations in region-V of the 23S-rDNA explain the azithromycin resistance (J.S. Jensen, unpub. data).
M. genitalium has been associated with persistent NGU (1). Recent data indicate that sequence variation in the gene mediating adhesion to epithelial cells coincides with the immune response in patients and that changes in this gene occur rapidly with persistent infection (14). In vitro studies also suggest that macrolide-resistant mutants can be selected by serial passage of mycoplasmas in subinhibitory concentrations of macrolide (15). Macrolide resistance in our study could have been induced by singledose azithromycin, which may be suboptimal for eradication of a slow-growing bacterium such as M. genitalium. Studies are ongoing to establish whether resistance in our isolates was present pretreatment or emerged after azithromycin-exposure. It is possible that initial use of higher doses or longer durations of azithromycin in M. genitalium-positive NGU could avoid selection of resistant mutants. The association between azithromycin failure and sexual partners from Asia may be clinically relevant, given the high levels of antimicrobial drug resistance reported in other sexually transmitted infections such as Neisseria gonorrhoeae infections in Asia, and the higher failure rates seen in homosexual men, while not statistically significant, may represent a core-group effect.
Azithromycin or doxycycline is recommended treatment for NGU. While treatment-failure in M. genitaliumpositive NGU appears common with doxycycline (4,7-11), early reports suggest 1 g azithromycin is more effective, with cure rates of 85% (10,11), and that prolonged azithromycin treatment (500 mg on day 1 and 250 mg on days 2-5) eradicates M. genitalium in 95% of cases (10). However, if treatment-failure after 1 g azithromycin is as prevalent as indicated by our study in M. genitalium-positive NGU, this has implications for the use of single-dose azithromycin as first-line treatment for NGU and leaves few evidence-based treatment options. Information regarding sensitivity of M. genitalium to fluoroquinolones has been limited, but reports suggest differential activity against M. genitalium, with levofloxacin (4,9) less active than gatifloxacin, sparfloxacin, and tosufloxacin in vitro and in vivo and moxifloxacin more active than levofloxacin and ciprofloxacin in vitro (6).
We report significant failure rates of azithromycin in M. genitalium-positive NGU that is supported by in vitro evidence of reduced susceptibility to macrolides. Recurrent urethral symptoms following azithromycin therapy only occurred in persons with persistent M. genitalium infection and resolved with moxifloxacin.
Because single-dose azithromycin is recommended treatment for NGU, these findings have implications for treatment guidelines and highlight the need for randomized studies to determine optimal treatment for M. genitalium-positive NGU and M. genitalium infection in women, who are at high risk for sequelae.