Congenital toxoplasmosis: Difference between revisions
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* Risk of transplacental infection of fetus is lowest in first trimester and highest in third |
* Risk of transplacental infection of fetus is lowest in first trimester and highest in third |
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* Often no history of illness during pregnancy |
* Often no history of illness during pregnancy |
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** Symptoms, if present, tend to be mild with low-grade fever, malaise, and lymphadenopathy |
** Symptoms, if present, tend to be mild with low-grade fever, malaise, and lymphadenopathy |
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Revision as of 17:29, 21 July 2020
Background
- Can be acquired during maternal parasitemia associated with primary infection
- However, it is possible to acquire from reactivation of latent toxoplasmosis in an HIV-infected mother
- Risk of transplacental infection of fetus is lowest in first trimester and highest in third
Clinical Manifestations
- Often no history of illness during pregnancy
- Symptoms, if present, tend to be mild with low-grade fever, malaise, and lymphadenopathy
- At birth, 85% of infected babies are asymptomatic and only 15% are symptomatic
- Risk of infection is related to trimester of infection: 6% in first, 40% in second, and 72% in third
- Risk of signs of congenital infection is inversely related to trimester of infection: 61% in first, 25% in second, and 9% in third
- Classic triad of chorioretinitis (most common), intraparenchymal cerebral calcifications, and hydrocephalus
- Others: thrombocytopenia, hepatitis, hepatosplenomegaly, cataracts, strabismus, microphthalmia
Diagnosis
In pregnancy
- Molecular
- Definitive diagnosis is based on PCR of amniotic fluid around 18 months, usually done after maternal serology to confirm intrauterine infection
- Sensitivity is 64 to 92% and specificity 100% (NPR around 88 to 98%)
- Earlier than 18 weeks has unknown sensitivity and specificity, and has a higher risk of spontaneous abortion
- Can also be done on fetal blood
- Definitive diagnosis is based on PCR of amniotic fluid around 18 months, usually done after maternal serology to confirm intrauterine infection
- Serology
- Can check maternal IgM and IgG
- IgM is not specific to recent infection, however, as it can be present for more than a year
- IgG avidity testing is used to determine recency of infection
- Low avidity is 35-50% and high is >60%
- Low avidity is unhelpful, as avidity can remain low for more than a year
- High avidity, on the other hand, suggests infected at least 3-4 months prior
- Therefore, if infection is suspected in the first 16 weeks of gestation, avidity testing may be able to rule out infection during pregnancy
- Needs serial head ultrasound to monitor for hydrocephalus and intraparenchymal brain calcifications
- May also see hepatic calcifications, splenomegaly, and ascites
In children
- Standard workup starts with serology, then adds PCR and other investigations if clinical suspicion is high
- Serology
- In neonates, IgG serology reflects maternal status, so use IgM and IgA instead
- Molecular testing
- If clinical suspicion is high, add PCR of the peripheral blood, urine, and CSF to the serology
- Other
- If clinical suspicion is high, also get ophthalmologic evaluation, hearing assessment, ultrasound or CT of the brain, and lumbar puncture
Management
In pregnancy
- If infected < 14 weeks gestation, spiramycin 3 g/day until delivery
- However, it doesn't cross the placenta and it's unclear whether it affects outcomes in the baby
- Likely most effective if given within 8 weeks of maternal infection
- Second-line would be monotherapy with sulfadiazine or clindamycin
- If age ≥ 14 weeks gestation and documented fetal infection, or if suspected infection was ≥14 weeks gestation, use standard therapy
- Standard therapy is: pyrimethamine 50 mg q12h for 2 days followed by 50 mg daily (plus folinic acid 10-20 mg daily until 1 week after stopping pyrimethamine), and sulfadiazine 75 mg/kg load followed by 50 mg/kg q12h (maximum 4 g/day)
- This treatment crosses the placenta, which is why it is used in cases of documented or suspected fetal infection, as well as in later-term infections when the risk of fetal infection is higher
- Therefore, if initially started on spiramycin, then switch to standard therapy if amniotic fluid PCR is positive or ultrasound is abnormal
- However, it is teratogenic until 14 weeks gestation so spiramycin is used until then
In children
- Postnatal treatment of neonates is with standard therapy for at least 12 months
- Sulfadiazine 50 mg/kg q12h
- Pyrimethamine 1 mg/kg q12h for 2 days (load), followed by 1 mg/kg for 2 to 6 months, followed by 1 mg/kg qMWF
- Folinic acid 10 mg PO thrice weekly until 1 week after pyrimethamine is stopped
- Treatment of congenital infection in older children is standard therapy until 1 to 2 weeks after resolution of signs or symptoms
- Pyrimethamine 1 mg/kg q12h (max 50 mg) for 2 days, followed by 1 mg/kg/day (max 25 mg)
- Sulfadiazine 75 mg/kg load, followed by 50 mg/kg q12h (max 4 g/day)
- Folinic acid 10-20 mg po thrice weekly
- Can add prednisone for severe chorioretinits at 1 mg/kg/day divided bid (max 40 mg/day), followed by a rapid taper
- Serial evaluations with a clinical assessment, neuroradiology, ophthalmology, and CSF analysis
References
- ^ Effectiveness of prenatal treatment for congenital toxoplasmosis: a meta-analysis of individual patients' data. The Lancet. 2007;369(9556):115-122. doi:10.1016/s0140-6736(07)60072-5.
