Toxoplasmosis

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Toxoplasmosis is caused by Toxoplasma gondii, an intracellular protozoan parasite. Its main host is the cat. It is one of the most common human parasites. Primary infection is usually subclinical but sometimes leads to chorioretinitis, or may damage the fetus if acquired in pregnancy. Reactivation of latent infection can occur in immunocompromised patients and may cause life-threatening encephalitis.

See also the article on Congenital, Perinatal and Neonatal Infections.

T. gondii oocysts are excreted in cat faeces, mature in the environment and may be ingested by secondary hosts (humans, cattle, sheep, pigs, rodents and birds). In these hosts, there is disseminated infection, which is controlled by the immune response. The active proliferating forms of the organism are called tachyzoites. They can be found in any organ but occur most commonly in the brain, skeletal muscle and heart muscle.

Following a successful immune response, dormant parasites remain encysted in the host tissues for years. They can reactivate if there is immune suppression - notably, AIDS.

The life cycle is completed by cats eating infected animal tissue.

Domestic cats are the main source of infection. Infectious oocysts are excreted by the cat for up to two weeks after the initial infection and can survive in warm, moist soil for more than one year.

Humans become infected via the following routes:

  • Ingestion/handling of oocytes from cat faeces - via contaminated soil, water or food.
  • Eating or handling undercooked or raw meat which is infected - mainly pork and lamb.
  • There’s a small risk during the lambing season of toxoplasmosis infection passing from sheep to humans. The T. gondii parasite is sometimes found in the afterbirth and on newborn lambs after an infected sheep has given birth.[3]
  • Maternal-to-fetal transmission - occurs almost solely when the primary infection is acquired during pregnancy.[4]
  • Organ transplantation - usually in the context of a donor seropositive for T. gondii and a seronegative recipient.

T. gondii is worldwide in distribution but the disease occurs less frequently in areas where the environment is unfavourable for the oocysts, such as colder or drier regions and high altitudes. The seroprevalence of populations varies widely - for example:

  • A systematic review found that in the USA 16-40% of the population were infected compared to 50-80% in South America.[5]
  • One study of women attending antenatal clinics in an ethnically diverse population in central London found seroprevalence for T. gondii was 17.32% in 2,610 samples tested.[6]
  • About 350 cases are diagnosed in the UK per year.[3]

Toxoplasma infections may present in four main ways:

Acquired infection in immunocompetent adults and children

  • This is asymptomatic in most cases.
  • It is said that 10% have symptoms - eg, nonspecific illness or isolated lymphadenopathy (of occipital or cervical nodes, usually resolving within six weeks). However, studies have reported subtle changes in behaviour, personality and psychomotor performance in infected individuals, so the incidence of symptomatic toxoplasmosis may be higher.[7]
  • Studies suggest a link between toxoplasmosis and schizophrenia.[8]
  • More chronic lymphadenopathy can occur.
  • Rarely, there may be polymyositis, myocarditis, pericarditis, pneumonitis, hepatitis or encephalitis.
  • Cases of severe, acute disseminated toxoplasmosis in immunocompetent patients, due to atypical strains mainly from the Amazonian rainforest, have been reported.[9]

Ocular toxoplasmosis[10, 11]

  • Toxoplasmic chorioretinitis can occur in both immunocompetent and immunocompromised patients, through acute infection, reactivation or congenital infection.
  • Presentation varies:
    • Possible symptoms are reduced visual acuity and floaters.
    • The typical ocular findings are focal retinochoroiditis, a nearby retinochoroidal scar and moderate-to-severe vitreous inflammation.
    • Atypical presentations can occur, such as anterior uveitis, scleritis and optic disc or optic nerve pathologies.
    • Pain is not a common feature (since pain is unusual in chorioretinitis). However, pain may occur in some of the atypical presentations - eg, with scleritis or endophthalmitis.

See also the separate Chorioretinal Inflammation article.

Congenital infection in immunocompetent patients[12]

  • The mother is usually asymptomatic, although some have malaise and lymphadenopathy or rarely chorioretinitis.
  • The fetal consequences are more severe if infection takes place within the first ten weeks of conception. The risk of maternal-fetal transmission increases as the pregnancy proceeds but the consequences become less severe.[13]
  • May cause miscarriage or fetal abnormalities which are detectable on ultrasound.
  • May have no apparent symptoms at birth, with complications developing only later in life.
  • Neonatal features of infection vary and include hydrocephalus, microcephaly, intracranial calcifications, chorioretinitis, strabismus, severe sight impairment, epilepsy, developmental delay, thrombocytopenia and anaemia.
  • The classical triad of congenital infection comprises chorioretinitis, intracranial calcifications and hydrocephalus; however, this is rare.

Immunocompromised patients

  • Toxoplasmosis can be life-threatening for immunocompromised patients, usually due to reactivation of chronic infection.
  • Toxoplasmic encephalitis is the most common feature, with varying presentations:[14]
    • It may be acute (eg, acute confusional state) or evolve over days to weeks.
    • Clinical features include confusion, seizures, focal neurological deficits (eg, hemiparesis or dysphasia), cerebellar signs and neuropsychiatric features.
    • Toxoplasmic encephalitis is a common complication of AIDS.
  • Other presentations in immunocompromised people include chorioretinitis, pneumonitis, and multiorgan involvement with respiratory failure and shock.
  • This depends on the clinical scenario.
  • With suspected toxoplasmic encephalitis, the differential diagnosis includes central nervous system (CNS) lymphoma, progressive multifocal leukoencephalopathy and other infections (cytomegalovirus (CMV), Cryptococcus spp., Aspergillus spp., Nocardia spp., or bacterial abscess).
  • With congenital infection, the differential diagnosis includes rubella, herpes simplex virus, CMV and syphilis.

Various tests are available, depending on the type of case (eg, immunocompetent, HIV/AIDS, congenital, organ transplant, ocular infection). They include:

  • Reference serology test - IgG and IgM (Sabin-Feldman Dye Test - DT).
  • IgM EIA.
  • IgM/IgA Immunosorbent Agglutination Assay (ISAGA).
  • Molecular Diagnosis (PCR).
  • Enhanced Immunohisto-staining.
  • Toxoplasma IgG/IgM Immunoblot.

Imaging

  • MRI or CT scanning for brain lesions. Typical CNS findings are multiple ring-enhancing lesions.[17] MRI is more sensitive[18]
  • Fetal or neonatal ultrasonography can be used if there is known/suspected transplacental infection. However, the findings are not diagnostic. There may be ventriculomegaly, CNS calcifications, placental changes, hepatomegaly, splenomegaly, ascites and pericardial or pleural effusion.[4]

Trial of therapy

Empirical anti-toxoplasmosis treatment is accepted practice for immunocompromised patients with multiple ring-enhancing brain lesions; patients usually improve within 7-10 days.[19]

Most infections caused by Toxoplasma gondii are self-limiting, and treatment is not necessary. Exceptions are patients with eye involvement (toxoplasma choroidoretinitis), and those who are immunosuppressed.

There may be life-threatening illness (usually in immunocompromised patients), with encephalitis, pneumonitis, or myocarditis. Patients may require stabilisation and treatment of acute symptoms such as seizures, respiratory failure and cardiovascular compromise.[21]

Specific treatment against T. gondii, if required, will depend on the clinical situation and will always be under specialist/expert supervision:

  • The treatment of choice for immunocompromised people is a combination of pyrimethamine and sulfadiazine, given for several weeks.
  • Pyrimethamine is a folate antagonist, and therefore folinic acid supplements are also required, along with weekly blood counts.
  • Alternative regimens use combinations of pyrimethamine with clindamycin or clarithromycin or azithromycin.
  • Long-term secondary prophylaxis is required after treatment of toxoplasmosis in immunocompromised patients, and prophylaxis should continue until immunity recovers.
  • If toxoplasmosis is acquired in pregnancy, transplacental infection may lead to severe disease in the fetus. Specialist advice should be sought on management.
  • Spiramycin [unlicensed] (available from ‘special-order’ manufacturers or specialist importing companies) may reduce the risk of transmission of maternal infection to the fetus.
  • Clinical infection in the mother is with either trimethoprim-sulfamethoxazole or pyrimethamine-sulfadiazine. A meta-analysis found there was little to choose between them.[14]
  • Pyrimethamine with sulfadiazine and folinic acid is an option when fetal infection is documented or suspected (eg, positive amniotic fluid PCR) with monitoring for haemotoxicity. Pyrimethamine should be avoided in the first trimester, as it is teratogenic.
  • Alternative drugs such as azithromycin have been used. One study reported good control of T.gondii infection in human villous explants.[22]
  • Many protocols also treat the child postnatally; usually for twelve months.[23]
  • Termination of pregnancy may be considered.[3]

Ocular toxoplasmosis
See the separate Chorioretinal Inflammation article.

  • Nervous system involvement can lead to seizures, developmental delay, deafness or other CNS lesions.
  • Ocular disease can lead to visual impairment or, rarely, severe sight impairment.
  • Acute infection in the immunocompromised may cause haemodynamic abnormalities similar to septic shock.
  • Life-threatening involvement of internal organs (CNS, heart and lungs) - usually in immunocompromised patients.
  • Other possible, although uncommon, complications in AIDS patients are panhypopituitarism, diabetes insipidus, syndrome of inappropriate antidiuretic hormone secretion, orchitis and myositis.
  • Most cases in immunocompetent healthy individuals remain subclinical or resolve spontaneously.
  • The prognosis in AIDS patients was poor but has improved considerably since the advent of ART (also called HAART).[25]
  • The overall prognosis with maternal infection is fairly good:[26]
    • The overall risk of vertical transmission with maternal seroconversion is 26%.
    • Among infected children, 33% have retinal lesion(s) but bilateral visual impairment seems to be unusual; in one survey, no child was severely sight impaired.[27]
    • One expert suggested: "the biggest danger to the fetus is not the parasite but the mother's anxiety."[26]

Hygiene measures, particularly for pregnant women and seronegative immunocompromised patients:[28]

  • Wash hands before handling food.
  • Thoroughly wash all fruit and vegetables, including ready-prepared salads, before eating.
  • Thoroughly cook raw meats and ready-prepared chilled meals.
  • Wear gloves and thoroughly wash hands after handling soil and gardening.
  • Avoid cat faeces in cat litter or in soil.

Some countries - eg, France - routinely screen pregnant women for toxoplasmosis. This is not done in the UK or the USA, where prevalences are lower. National Institute for Health and Care Excellence (NICE) antenatal care guidelines and the UK National Screening Committee (NSC) concluded that there was insufficient evidence to recommend screening.[28, 29]

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Further reading and references

  1. Zhou Y, Zhang H, Cao J, et al; Epidemiology of toxoplasmosis: role of the tick Haemaphysalis longicornis. Infect Dis Poverty. 2016 Feb 205:14. doi: 10.1186/s40249-016-0106-0.

  2. Smith NC, Goulart C, Hayward JA, et al; Control of human toxoplasmosis. Int J Parasitol. 2021 Feb51(2-3):95-121. doi: 10.1016/j.ijpara.2020.11.001. Epub 2020 Dec 19.

  3. Toxoplasmosis: diagnosis, epidemiology and prevention; GOV.UK

  4. Paquet C et al; Toxoplasmosis in Pregnancy: Prevention, Screening, and Treatment, SOGC, 2013.

  5. Torgerson PR, Mastroiacovo P; The global burden of congenital toxoplasmosis: a systematic review. Bull World Health Organ. 2013 Jul 191(7):501-8. doi: 10.2471/BLT.12.111732. Epub 2013 May 3.

  6. Flatt A, Shetty N; Seroprevalence and risk factors for toxoplasmosis among antenatal women in London: a re-examination of risk in an ethnically diverse population. Eur J Public Health. 2013 Aug23(4):648-52. doi: 10.1093/eurpub/cks075. Epub 2012 Jun 13.

  7. Flegr J, Preiss M, Klose J; Toxoplasmosis-associated difference in intelligence and personality in men depends on their Rhesus blood group but not ABO blood group. PLoS One. 2013 Apr 108(4):e61272. doi: 10.1371/journal.pone.0061272. Print 2013.

  8. Bhadra R, Cobb DA, Weiss LM, et al; Psychiatric disorders in toxoplasma seropositive patients--the CD8 connection. Schizophr Bull. 2013 May39(3):485-9. doi: 10.1093/schbul/sbt006. Epub 2013 Feb 20.

  9. Robert-Gangneux F, Darde ML; Epidemiology of and diagnostic strategies for toxoplasmosis. Clin Microbiol Rev. 2012 Apr25(2):264-96. doi: 10.1128/CMR.05013-11.

  10. Soheilian M et al; How to Diagnose & Treat Ocular Toxoplasmosis, Review of Ophthalmology, 2011

  11. Kalogeropoulos D, Sakkas H, Mohammed B, et al; Ocular toxoplasmosis: a review of the current diagnostic and therapeutic approaches. Int Ophthalmol. 2022 Jan42(1):295-321. doi: 10.1007/s10792-021-01994-9. Epub 2021 Aug 9.

  12. Deganich M, Boudreaux C, Benmerzouga I; Toxoplasmosis Infection during Pregnancy. Trop Med Infect Dis. 2022 Dec 218(1):3. doi: 10.3390/tropicalmed8010003.

  13. Stillwaggon E, Carrier CS, Sautter M, et al; Maternal serologic screening to prevent congenital toxoplasmosis: a decision-analytic economic model. PLoS Negl Trop Dis. 2011 Sep5(9):e1333. doi: 10.1371/journal.pntd.0001333. Epub 2011 Sep 27.

  14. Yan J, Huang B, Liu G, et al; Meta-analysis of prevention and treatment of toxoplasmic encephalitis in HIV-infected patients. Acta Trop. 2013 Sep127(3):236-44. doi: 10.1016/j.actatropica.2013.05.006. Epub 2013 May 23.

  15. Shah K et al; Central Nervous System Infections in Immunocompromised Hosts, 2013

  16. Toxoplasma Reference Unit

  17. Oprisan A, Popescu BO; Intracranial cysts: an imagery diagnostic challenge. ScientificWorldJournal. 2013 May 22013:172154. doi: 10.1155/2013/172154. Print 2013.

  18. Kumar GG, Mahadevan A, Guruprasad AS, et al; Eccentric target sign in cerebral toxoplasmosis: neuropathological correlate to the imaging feature. J Magn Reson Imaging. 2010 Jun31(6):1469-72. doi: 10.1002/jmri.22192.

  19. Madi D, Achappa B, Rao S, et al; Successful treatment of cerebral toxoplasmosis with clindamycin: a case report. Oman Med J. 2012 Sep27(5):411-2. doi: 10.5001/omj.2012.100.

  20. Dunay IR, Gajurel K, Dhakal R, et al; Treatment of Toxoplasmosis: Historical Perspective, Animal Models, and Current Clinical Practice. Clin Microbiol Rev. 2018 Sep 1231(4):e00057-17. doi: 10.1128/CMR.00057-17. Print 2018 Oct.

  21. Kappagoda S, Singh U, Blackburn BG; Antiparasitic therapy. Mayo Clin Proc. 2011 Jun86(6):561-83. doi: 10.4065/mcp.2011.0203.

  22. Castro-Filice LS, Barbosa BF, Angeloni MB, et al; Azithromycin is able to control Toxoplasma gondii infection in human villous explants. J Transl Med. 2014 May 1912:132. doi: 10.1186/1479-5876-12-132.

  23. Kieffer F, Wallon M; Congenital toxoplasmosis. Handb Clin Neurol. 2013112:1099-101. doi: 10.1016/B978-0-444-52910-7.00028-3.

  24. Weiss LM, Dubey JP; Toxoplasmosis: A history of clinical observations. Int J Parasitol. 2009 Jul 139(8):895-901. Epub 2009 Feb 13.

  25. Contini C; Clinical and diagnostic management of toxoplasmosis in the immunocompromised patient. Parassitologia. 2008 Jun50(1-2):45-50.

  26. Peyron F; When are we going to celebrate the centenary of the discovery of efficient treatment for congenital toxoplasmosis? Mem Inst Oswaldo Cruz. 2009 Mar104(2):316-9.

  27. Stanford MR, Tan HK, Gilbert RE; Toxoplasmic retinochoroiditis presenting in childhood: clinical findings in a UK survey. Br J Ophthalmol. 2006 Dec90(12):1464-7. Epub 2006 Aug 9.

  28. Antenatal care; NICE guidance (August 2021)

  29. Toxoplasmosis screening in pregnancy; UK Antenatal Screening Programme.

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