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Clinica Chimica Acta 2006-Sep

Lysosomal storage diseases in non-immune hydrops fetalis pregnancies.

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Angelique J A Kooper
Pim M W Janssens
Akosua N J A de Groot
Maria L F Liebrand-van Sambeek
Catharina J M G van den Berg
Gita B Tan-Sindhunata
Paul P van den Berg
Emilia K Bijlsma
Arie P T Smits
Ron A Wevers

Parole chiave

Astratto

BACKGROUND

At least 20 inborn errors of metabolism may cause hydrops fetalis. Most of these are lysosomal storage diseases. The study proposes a diagnostic flowchart for prenatal diagnosis of non-immune hydrops fetalis.

METHODS

This study contains a series of 75 non-immune hydrops fetalis pregnancies. Mucopolysaccharides, oligosaccharides, neuraminic acid and 21 lysosomal enzymes were measured in amniotic fluid and cultured amniotic cells.

RESULTS

The study gives reference values for mucopolysaccharides and neuraminic acid at various stages of gestation. Four definite and two probable lysosomal diagnoses were found among the 75 investigated cases (=5.3-8%). Fetal death was found to cause false positive values for mucopolysaccharides in amniotic fluid. In the galactosialidosis case, two novel mutations were found in the cathepsin A gene.

CONCLUSIONS

Reference values for mucopolysaccharides and neuraminic acid depend on gestational age. In a relatively high percentage of the hydrops foetalis pregnancies, a lysosomal aetiology is found. This study provides a strategy to diagnose lysosomal diseases in hydrops fetalis pregnancies. Awareness of lysosomal storage diseases causing hydrops fetalis is useful as it gives an opportunity for risk evaluation, genetic counseling to parents and targeted prenatal diagnostics for ensuing pregnancies.

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