Assessment of laboratory methods used in the diagnosis of congenital toxoplasmosis after maternal treatment with spiramycin in pregnancy.

[congenital toxoplasmosis]

The different laboratory methods used in the diagnosis of congenital toxoplasmosis have variable sensitivity and specificity . There is no evidence to prove that maternal treatment reduces the risk of fetal infection . The purpose of this study was to assess methods for the confirmation of congenital toxoplasmosis after maternal treatment with spiramycin during pregnancy , and to evaluate the effect of this treatment on clinical manifestations of the disease in newborns (NB ).This was a community-based , cross-sectional study of acute toxoplasmosis in newborns at risk of acquiring congenital infection . Participating newborns were born in the Clinical Hospital Maternity Ward of the Federal University of Goiás . Eligible participants were divided into 2 groups : group 1 consisted of 44 newborns born to mothers treated with spiramycin during pregnancy and group 2 consisted of 24 newborns born to mothers not treated with spiramycin during pregnancy because the diagnosis of toxoplasmosis was not performed . The sensitivity and specifity of PCR for T . gondii DNA in peripheral blood and serological testing for specific anti-T . gondii IgM and IgA , and the effects of maternal spiramycin treatment on these parameters , were determined by associating test results with clinical manifestations of disease .The sensitivity of the markers (T . gondii DNA detected by PCR , and the presence of specific anti-T . gondii IgM and IgA ) for congenital toxoplasmosis was higher in group 2 than in group 1 (31 .6 , 68 .4 , 36 .8 % and 3 .7 , 25 .9 , 11 .1 % respectively ). Even with a low PCR sensitivity , the group 2 results indicate the importance of developing new techniques for the diagnosis of congenital toxoplasmosis in newborns . Within group 1 , 70 .4 % of the infected newborns were asymptomatic and , in group 2 , 68 .4 % showed clinical manifestations of congenital toxoplasmosis .The higher proportion of infants without clinical symptoms in group 1 (70 .4 %) suggests the maternal treatment with spiramycin delays fetal infection , reducing the clinical sequelae of the disease in newborns . Given the low sensitivity of the tests used , when there is suspicion of congenital transmission several serological and parasitological tests are required in order to confirm or exclude congenital toxoplasmosis in newborns .