Recurrence risk due to germ line mosaicism: Duchenne and Becker muscular dystrophy |
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| Authors: | ATJM Helderman-van den Enden R de Jong JT den Dunnen JJ Houwing-Duistermaat ALJ Kneppers HB Ginjaar MH Breuning and E Bakker |
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| Institution: | Center for Human and Clinical Genetics;, and Department of Medical Statistics and Bioinformatics, Leiden University Medical Center, Leiden, the Netherlands |
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| Abstract: | The presence of multiple affected offspring from apparently non-carrier parents is caused by germ line mosaicism. Although germ line mosaicism has been reported for many diseases, figures for recurrence risks are known for only a few of them. In X-linked Duchenne and Becker muscular dystrophies (DMD/BMD), the recurrence risk for non-carrier females due to germ line mosaicism has been estimated to be between 14% and 20% (95% confidence interval 3–30) if the risk haplotype is transmitted. In this study, we have analyzed 318 DMD/BMD cases in which the detected mutation was de novo with the aim of obtaining a better estimate of the 'true' number of germ line mosaics and a more precise recurrence risk. This knowledge is essential for genetic counseling. Our data indicate a recurrence risk of 8.6% (4.8–12.2) if the risk haplotype is transmitted, but there is a remarkable difference between proximal (15.6%) (4.1–27.0) and distal (6.4%) (2.1–10.6) deletions. Overall, most mutations originated in the female. Deletions occur more often on the X chromosome of the maternal grandmother, whereas point mutations occur on the X chromosome of the maternal grandfather. In unhaplotyped de novo DMD/BMD families, the risk of recurrence of the mutation is 4.3%. |
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| Keywords: | de novo Duchenne muscular dystrophy germ line mosaicism recurrence risk |
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