| Literature DB >> 29261177 |
Alison Dalton Archibald1,2,3, Melanie Jane Smith1,2, Trent Burgess1,2,3, Katrina Louise Scarff1, Justine Elliott1, Clare Elizabeth Hunt1, Zoe McDonald, Caitlin Barns-Jenkins1,2, Chelsea Holt1,2, Karina Sandoval1,2, Vanessa Siva Kumar1,2, Lisa Ward1,2, Emily Caroline Allen2,3, Sarah Valerie Collis2,3, Shannon Cowie1, David Francis1,2, Martin B Delatycki1,2,3,4, Eppie Mildred Yiu2,3,4, R John Massie2,3,4, Mark Domenic Pertile1,2,3, Desirée du Sart1,2,3, Damien Bruno1,2,3, David J Amor1,2,3,4.
Abstract
PurposeTo describe our experience of offering simultaneous genetic carrier screening for cystic fibrosis (CF), fragile X syndrome (FXS), and spinal muscular atrophy (SMA).MethodsCarrier screening is offered through general practice, obstetrics, fertility, and genetics settings before or in early pregnancy. Carriers are offered genetic counseling with prenatal/preimplantation genetic diagnosis available to those at increased risk.ResultsScreening of 12,000 individuals revealed 610 carriers (5.08%; 1 in 20): 342 CF, 35 FXS, 241 SMA (8 carriers of 2 conditions), approximately 88% of whom had no family history. At least 94% of CF and SMA carriers' partners were tested. Fifty couples (0.42%; 1 in 240) were at increased risk of having a child with one of the conditions (14 CF, 35 FXS, and 1 SMA) with 32 pregnant at the time of testing. Of these, 26 opted for prenatal diagnosis revealing 7 pregnancies affected (4 CF, 2 FXS, 1 SMA).ConclusionThe combined affected pregnancy rate is comparable to the population risk for Down syndrome, emphasizing the need to routinely offer carrier screening. The availability of appropriate genetic counseling support and a collaborative approach between laboratory teams, genetics services, health professionals offering screening, and support organizations is essential.Entities:
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Year: 2017 PMID: 29261177 DOI: 10.1038/gim.2017.134
Source DB: PubMed Journal: Genet Med ISSN: 1098-3600 Impact factor: 8.822