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Chlamydia (genital infection)

Page content: Victorian statutory requirement | Infectious agent | Identification | Incubation period | Public health significance & occurrence | Reservoir | Mode of transmission | Period of communicability | Susceptibility & resistance | Control measures | Outbreak measures | Additional sources of information

Victorian statutory requirement

Chlamydia (Group C disease) must be notified in writing within five days of diagnosis.

Specific information must be notified under the Public Health and Wellbeing Regulations 2009. To maintain confidentiality, only the name code (first two letters of the surname followed by the first two letters of the first name) is required. A questionnaire is sent to the diagnosing doctor to collect additional information on the case that is essential for detecting disease trends and informing policy development.

Medical practitioners have a statutory obligation under the Children and Young Persons Act 1989 to notify the Department of Human Services Child Protection Service if they believe a child is in need of protection on the basis of sexual abuse.

Infectious agent

Chlamydia trachomatis serogroups DK cause disease.

Identification

Clinical features
Most women with urethral or endocervical chlamydial infection are asymptomatic. Clinical manifestations may include vaginal discharge, dysuria and post-coital or intermenstrual bleeding. Less frequent manifestations include urethral syndrome (dysuria and pyuria), bartholinitis, perihepatitis and proctitis.

Complications and sequelae may result in chronic pelvic pain, infertility and ectopic pregnancy. Infections during pregnancy may cause preterm rupture of the membranes and preterm delivery. It can also cause conjunctivitis in the newborn and pneumonitis in the young infant.

The primary presentation of chlamydial infection in males is urethritis but infection may be asymptomatic. Possible sequelae and complications of male urethral infection are epididymitis, infertility, Reiters syndrome and conjunctivitis. Receptive anal intercourse in men who have sex with men (MSM) may result in chlamydial proctitis.

Method of diagnosis
Testing individuals at high risk of chlamydial infection is recommended. High risk individuals include those with a clinical presentation suggestive of chlamydial infection, individuals attending general practitioners for testing of sexually acquired infection (STI), those attending STI and family planning clinics and gay mens health centres and partners of those already diagnosed with an STI.

Laboratory investigations currently available are:

  • cell culture (only in specialised laboratories)
  • antigen assays including direct immunofluorescence or enzyme immunoassay
  • hybridisation assays such as the DNA probe
  • amplification assays including PCR and ligase chain reaction (LCR).

The choice of test depends on the specimen type submitted, the cost of the test, the sensitivity and specificity of the test and the expertise and size of the laboratory.

Incubation period

The incubation period is poorly defined but is probably 7 to 14 days or longer.

Public health significance & occurrence

Infection with C. trachomatis has become a major public health problem because of the long term consequences of infection experienced predominantly by women. These include chronic pelvic pain, ectopic pregnancy and infertility. Rarely males may also become infertile.

Chlamydia is the most commonly notified sexually transmissible bacterial disease in Victoria. It affects both genders. The annual number of notified cases has more than doubled since the early 1990s. Approximately 75% of infections are notified from individuals aged less than 30 years.

The prevalence of chlamydial genital infections in Australia has not been comprehensively established but it has been estimated to be 2.5 14% in STD clinic patients, 5% in family planning clients and up to 15% in commercial sex workers.

While the spontaneous cure rate has been estimated at 7.4%, immunity following infection is thought to be type-specific and only partially protective. As a result recurrent infections are common.

Risk factors for chlamydial infections include a relatively high number of sexual partners, a new sexual partner and lack of use of barrier contraceptive measures.
Endocervical C. trachomatis infection has also been associated with an increased risk of acquiring human immunodeficiency virus (HIV) infection and may also increase HIV infectiousness.

Reservoir

Humans.

Mode of transmission

Transmission of C. trachomatis occurs primarily by sexual contact. Mother to baby transmission occurs when mothers colonised with C. trachomatis infect their babies as they are born vaginally.

A high proportion of infections in women are asymptomatic resulting in untreated disease, ongoing transmission and an increased risk of sequelae.

Period of communicability

The period of communicability is unknown but may be months to years.

Susceptibility & resistance

Everyone is susceptible to infection.

Control measures

Preventive measures
Preventive measures include education about safe sex practices including use of condoms and early detection of infection by testing of those at risk.

Control of case
Azithromycin or doxycycline are used as first line antimicrobials to treat chlamydial infection. Advice on the treatment of chlamydial infections can be found in Therapeutic guidelines: antibiotic (Therapeutic Guidelines Limited) and the National management guidelines for sexually transmissible infections (Venereology Society of Victoria, 2002).

Specialist consultation should be sought for complicated or disseminated infections.

Control of contacts
Sexual partners of individuals with chlamydial infection should be examined and investigated then treated empirically.

Contact tracing assistance can be provided by the Departments partner notification officers (03) 9347 1899.

Control of environment
Not applicable.

Outbreak measures

Not applicable.

Additional sources of information

  • Australian Government Department of Health and Family Services 1997, Contact tracing manual a practical handbook for health care providers managing people with HIV, viral hepatitis, other STDs and HIV-related tuberculosis, Australian Government Department of Health and Family Services.
  • Cates, W & Wasserheit, JN 1991, Genital chlamydia infections: epidemiology and reproductive sequelae, American Journal of Obstetrics and Gynecology, vol. 164, no. 6, pt. 2, pp. 177181.
  • Centers for Disease Control and Prevention 2002, Sexually transmitted diseases treatment guidelines 2002, Morbidity and Mortality Weekly Report, vol. 51 (RR06), pp.180
    www.cdc.gov/mmwr
  • Garland, SM, Gertig, DM & McInnes, JA 1993, Genital Chlamydia trachomatis infection in Australia, Medical Journal of Australia, vol. 159, pp. 906.
  • Genc, M & Mardh, A 1996, A cost-effectiveness analysis of screening and treatment for Chlamydia trachomatis infection in asymptomatic women, Annals of Internal Medicine, vol. 124, no. 1, pt. 1, pp. 17.
  • Pearlman, MD & McNeeley, SG 1992, A review of the microbiology, immunology, and clinical implications of Chlamydia trachomatis infections, Obstetrical and Gynecological Survey, vol. 47, no. 7, pp. 44861.
  • Venereology Society of Victoria 2002, National management guidelines for sexually transmissible diseases, Venereology Society of Victoria
    www.mshc.org.au
  • Weinstock, H, Dean, D & Bolan, G 1994, Chlamydia trachomatis infections, Infectious Disease Clinics of North America, vol. 8, no. 4, pp. 797819.