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Should we routinely test for Mycoplasma genitalium when testing for other sexually transmitted infections?

James D Stewart, Brooke Webb, Michelle Francis, Maryza Graham and Tony M Korman
Med J Aust 2020; 212 (1): 30-31. || doi: 10.5694/mja2.50399
Published online: 9 December 2019

Mycoplasma genitalium is a sexually transmitted bacterium that was initially identified as a cause of non‐gonococcal urethritis in men.1 Associations with other genitourinary tract syndromes, including cervicitis and pelvic inflammatory disease in women, are now recognised, albeit with limited understanding of the natural history of infection.1,2 However, the significance of M. genitalium in asymptomatic individuals, including pregnant women, is uncertain. Local and international guidelines advise testing only symptomatic patients unless an asymptomatic person has had sexual contact with someone infected with M. genitalium or is to have genitourinary tract surgery that breaches the cervical barrier.3,4,5 We report the first data on the epidemiology of M. genitalium in an Australian hospital, including in pregnant women, and discuss the difficulties associated with testing asymptomatic patients for M. genitalium.

Monash Health is a large health care network in Melbourne that includes three emergency departments and an obstetric service with more than 9000 births each year. Over the 3‐month period 1 May – 31 July 2017, we included routine nucleic acid amplification testing (NAAT) (High‐Plex Urinogenital multiplex, AusDiagnostics) for M. genitalium when sexually transmitted infection multiplex testing of genitourinary specimens (including urine, endocervical, vaginal, and urethral swabs) for Chlamydia trachomatis and Neisseria gonorrhoeae was requested for emergency department, outpatient clinic, or admitted patients. Testing for C. trachomatis is recommended in Australia as part of routine antenatal screening.4 Our study received ethics approval from the Monash Health Human Research Ethics Committee (reference, RES‐17‐0000‐466Q).

Of 1176 tested patients, 56 (5%) were positive for M. genitalium; 67 (6%) were positive for C. trachomatis, 12 (1%) for N. gonorrhoeae. The prevalence of M. genitalium was 3% in men (12 of 365), 5% in women (44 of 811), and 9% in pregnant women (8 of 92) (Box).

The median age of patients positive for M. genitalium (24 years; interquartile range [IQR], 19–29 years) was lower than for M. genitalium‐negative patients (29 years; IQR, 22–39 years), and larger proportions were positive for C. trachomatis (odds ratio [OR], 4.6; 95% confidence interval [CI], 2.3–9.5) or N. gonorrhoeae (OR, 7.6; 95% CI, 1.8–27). The difference in median age was statistically significant for both males and females, but not clinically significant for female patients (Box). M. genitalium was detected in five men with epididymo‐orchitis and one with urethritis, and in three women with pelvic inflammatory disease, all without other diagnosed sexually transmitted infections. Four of the pregnant women positive for M. genitalium had genitourinary symptoms, but none that were typical for M. genitalium infections.

Our case series, although small, has important implications for multiplex sexually transmitted infection NAAT testing. The significance of detecting M. genitalium in an asymptomatic patient is unclear. It is important that laboratories, as diagnostic stewards, liaise closely with their clinical colleagues to ensure they undertake only clinically useful testing, and do not deliver clinicians unrequested results of uncertain value.

The significance of M. genitalium infection in pregnant women is also unclear, and treatment options are limited. A meta‐analysis identified associations with pre‐term delivery and stillbirth,2 but these findings were not confirmed by prospective studies.6

We do not recommend routine testing for M. genitalium. With increasing awareness of the potential harm of unnecessary antibiotic therapy, this conclusion is in accordance with clinical guidelines recommending treating M. genitalium infections only if the patient is symptomatic, has had sexual contact with an infected person, or is to have surgery that breaches the cervical barrier.3,4,5 The clinical significance of asymptomatic infections remains to be elucidated.

Box – Mycoplasma genitalium testing results for 1176 patients at the Monash Medical Centre, Melbourne, May–July 2017

 

M. genitalium testing


P *

Odds ratio (95% CI)

Total

Negative result

Positive result


Number of patients

1176

1120 (95%)

56 (5%)

 

 

Age (years), median (IQR)

29 (22–39)

29 (22–39)

24 (19–29)

< 0.001

Co‐infection

 

 

 

 

 

  C. trachomatis

67 (6%)

56 (5%)

11 (20%)

4.6 (2.3–9.5)

  N. gonorrhoeae

12 (1%)

9 (0.8%)

3 (5%)

7.0 (1.8–27)

Men

 

 

 

 

 

Number of patients

365

353 (97%)

12 (3%)

 

 

Age (years), median (IQR)

36 (25–50)

36 (25–50)

24 (21–35)

0.009

Co‐infections

 

 

 

 

 

  C. trachomatis

20 (6%)

18 (5%)

2 (17%)

3.7 (0.76–18)

  N. gonorrhoeae

7 (2%)

7 (2%)

0

Women

 

 

 

 

 

Number of patients

811

767 (95%)

44 (5%)

 

 

Age (years), median (IQR)

27 (20–35)

26 (20–35)

24 (19–29)

0.030

Pregnant

92 (11%)

84 (11%)

8 (18%)

1.8 (0.8–4.0)

Co‐infections

 

 

 

 

 

  C. trachomatis

47 (6%)

36 (5%)

9 (21%)

5.2 (2.3–12)

  N. gonorrhoeae

5 (0.06)

2 (0.3%)

3 (7%)

28 (4.6–172)

Pregnant women

 

 

 

 

 

Number of patients

92

84 (91%)

8 (9%)

 

 

Age (years), median (IQR)

23 (20–29)

23 (20–29)

21 (19–21)

0.28

Asymptomatic screen

58 (63%)

54 (64%)

4 (50%)

 

 


CI = confidence interval; IQR = interquartile range. * Mann–Whitney U test.

Received 27 February 2019, accepted 2 August 2019

  • James D Stewart1,2
  • Brooke Webb1
  • Michelle Francis1
  • Maryza Graham1,2
  • Tony M Korman1,2

  • 1 Monash Medical Centre, Melbourne, VIC
  • 2 Monash University, Melbourne, VIC


Correspondence: jim.d.stewart@outlook.com

Competing interests:

No relevant disclosures.

  • 1. Taylor‐Robinson D, Jensen JS. Mycoplasma genitalium: from chrysalis to multicolored butterfly. Clin Microbiol Rev 2011; 24: 498–514.
  • 2. Lis R, Rowhani‐Rahbar A, Manhart LE. Mycoplasma genitalium infection and female reproductive tract disease: a meta‐analysis. Clin Infect Dis 2015; 61: 418–426.
  • 3. Australasian Sexual Health Alliance. Mycoplasma genitalium (Australian STI management guidelines for use in primary care). Updated July 2018. http://www.sti.guidelines.org.au/sexually-transmissible-infections/mycoplasma-genitalium (viewed Dec 2018).
  • 4. Australasian Sexual Health Alliance. Pregnant woman (Australian STI management guidelines for use in primary care). Updated Dec 2014. http://www.sti.guidelines.org.au/populations-and-situations/pregnant-women (viewed Dec 2018).
  • 5. Jensen JS, Cusini M, Gomberg M, Moi H. 2016 European guideline on Mycoplasma genitalium infections. J Eur Acad Dermatol Venereol 2016; 30: 1650–1656.
  • 6. Peuchant O, Le Roy C, Desveaux C, et al. Screening for Chlamydia trachomatis, Neisseria gonorrhoeae, and Mycoplasma genitalium should it be integrated into routine pregnancy care in French young pregnant women? Diagn Microbiol Infect Dis 2015; 82: 14–19.

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