Anti-P30 IgA antibodies as prenatal markers of congenital toxoplasma infection

Author:

DECOSTER A12,DARCY F1,CARON A1,VINATIER D3,DE L'AULNOIT D HOUZE4,VITTU G2,NIEL G5,HEYER F6,LECOLIER B7,DELCROIX M4,MONNIER J C3,DUHAMEL M2,CAPRON A1

Affiliation:

1. Cenlre d'lmmunologie et de Biologie Parasitaire, Unité mixte INSERM U 167, Institut Pasteur

2. Hôpital St Antoine, Centre Hospitalier Feron-Vrau

3. Maternite Pavillion Olivier du C.H.U., Lille

4. Maternité du Centre Hospitalier St Philibert, Lomme

5. Laboratoire de parasitologie, Centre Hospitalier Pitie-Salpetriere

6. Centre Hospitalier Cochin

7. Maternité Notre-Dame du Bon Secours, Paris, France

Abstract

SUMMARY This study extends a previous study and confirms that the detection of anti-P30 IgA antibodies is very helpful in the diagnosis of acute acquired or congenital toxoplasmosis. Moreover, we demonstrate that an anti-P30 IgA response can be mounted in the fetuses infected by Toxoplasma gondii during their inira-utcrine life as early as week 23 of gestation. A double-sandwich ELISA described in our previous work was used to detect anti-P30 IgA antibodies in 1378 human serum samples collected from 551 patients, including 162 fetuses whose mothers had been infected by T. gondii during pregnancy, 46 congenitally infected and 90 uninfected newborns and 253 women suspected of having been infected during pregnancy, including the mothers of fetuses and newborns previously described. Anti-P30 IgA antibodies were detected in all cases of acute toxoplasmosis but in no case of chronic toxoplasmosis: in the majority of cases, the IgA antibody litre fell below cut-off in 3–9 months. Among the 46 congenitally infected newborns, anti-P30 IgA antibodies were detected in sera of 41 infected newborns (38 at birth, two in the first months of life, one in the seventh month of life), while anti-P30 IgM antibodies were detected in only 30 cases at birth and in one case during the first month of life. Among 162 fetuses, anti-P30 IgA response was observed in five infected fetuses, but was not detected in either 152 uninfected fetuses or in five fetuses considered as infected. The absence or presence of anti-P30 IgA antibodies in the fetus is discussed in relation to the date of maternal infection and collection of the fetal blood. It clearly appears from our study that the combined testing of both IgM and IgA in the fetus and the newborn is essential for a more efficient diagnosis of infection.

Publisher

Oxford University Press (OUP)

Subject

Immunology,Immunology and Allergy

Reference35 articles.

1. Early prenatal diagnosis of congenital toxoplasmosis using amniotic fluid samples and tissue culture;Derouin;Eur J Clin Microbiol Infect Dis,1988

2. L'isolement du parasite dans la toxoplasmose congénitale. Intérêt pratique et théorique;Desmonts;Arch Fr Ped,1974

3. Prenatal diagnosis of congenital toxoplasmosis;Desmonts;Lancet,1985

4. IgA antibodies against P30 as markers of congenital and acute toxoplasmosis;Decoster;Lancet,1988

5. Les IgA anti-P30, marqueurs de toxoplasmose évolutive. Application au diagnostic de la toxoplasmose congénitale en période prénatale et néonatale;Decoster,1989

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