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Prenatal diagnosis of haemophilia: our experience of 44 cases

Authors :
Rosaria Ingino
Giuseppe Castaldo
Veronica Sanna
Giovanni Di Minno
Federica Zarrilli
Rita Santamaria
Antonio Coppola
Angiola Rocino
Zarrilli, F
Sanna, V
Ingino, R
Santamaria, Rita
Rocino, A
Coppola, Antonio
DI MINNO, Giovanni
Castaldo, Giuseppe
Publication Year :
2013

Abstract

Background: Haemophilia A and B (HA, HB) are the most frequent X-linked bleeding diseases; two-thirds of cases are severe. Methods: We counselled 51 couples for prenatal diagnosis (PD) of haemophilia. In 7/51 (13.7%) cases, the couple decided not to undergo PD because counselling revealed that they were carriers of a mild form of the disease, while we performed 44 PD for severe HA (36 cases) or HB (8 cases). The indication for PD was a haemophilic child (30/44, 68.2%) or an affected family member (12/44, 27.3%); in two cases the non-carrier mother of isolated haemophilic patients requested PD because of the risk of mosaicism. Results: We completed PD in 43/44 cases; in one case, the prenatal sample was contaminated by maternal DNA; however, molecular analysis revealed the female sex of the foetus. We performed PD for 16 of the 36 couples at risk of HA (44.4%) by analysing the intron (IVS)22 inversion; in 1/36 cases (2.8%) the mother had the IVS1 inversion, and in 8/36 (22.2%) the family mutation was identified by sequencing; in 11/36 (30.6%) cases the family mutation was unknown, and PD was performed by linkage (no recombination nor uninformative cases occurred). For HB, in 6/8 (75.0%) cases, PD was performed by DHPLC or by sequencing; in 2/8 cases we tested intragenic markers (again with no cases of recombination or uninformative families). Conclusions: PD in well-equipped laboratories, and multidisciplinary counselling are an aid to planning reproductive and early therapeutic strategies in families with severe haemophilia.

Details

Language :
English
Database :
OpenAIRE
Accession number :
edsair.doi.dedup.....c2b3b364f511d2824e20c9e34f55ec61