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Prenatal diagnosis and carrier detection in fragile X

✍ Scribed by Von Koskull, Harriet ;Nordström, Ann-Marie ;Salonen, Riitta ;Peltonen, Leena


Publisher
John Wiley and Sons
Year
1992
Tongue
English
Weight
498 KB
Volume
43
Category
Article
ISSN
0148-7299

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✦ Synopsis


Abstract

Prenatal diagnosis was performed in 81 cases at risk for the fragile X syndrome. There were 12 fra (X)‐positive cases, two of which showed low expression in cultured amniotic fluid cells. FUdR and high thymidine were used for induction of fra(X) (q27.3) expression in all cases. In 21 cases linkage studies were performed, 7 with probes for the loci DXS52, DXS98 and DXS105, 13 with probes for DXS369 and DXS296, DXS304 or DXS374 and one with the probe Do33 for DXS465. In 11 of these cases linkage analysis gave risk figures higher than 95% or lower than 5%, all in concordance with the cytogenetic findings. Discordance was found in three cases studied earlier, the two cases with low expression mentioned above and one cytogenetically normal case, which were now restudied with the new probes. RFLP‐studies and linkage analysis was also performed for 24 cytogenetically fra(X)‐negative females having a 50%, 25% or 12.5% risk of being carriers according to pedigree data. In 15 cases the risk dropped to 1% or less. Six of these women were pregnant and had asked for prenatal diagnosis but after genetic counseling prenatal diagnosis was avoided.


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