| Literature DB >> 2900805 |
M C Wapenaar1, T Kievits, K A Hart, S Abbs, L A Blonden, J T den Dunnen, P M Grootscholten, E Bakker, C Verellen-Dumoulin, M Bobrow.
Abstract
We have made a detailed study of a deletion hot spot in the distal half of the Duchenne muscular dystrophy (DMD) gene, using intragenic probe P20 (DXS269), isolated by a hybrid cell-mediated cloning procedure. P20 detects 16% deletions in patients suffering from either DMD or Becker muscular dystrophy (BMD), in sharp contrast to the adjacent intragenic markers JBir (7%) and J66 (less than 1%), mapping respectively 200-320 kb proximal and 380-500 kb distal to P20. Of the P20 deletions, 30% start within a region of 25-40 kb, the majority extending distally. P20 was confirmed to map internal to a distal intron of the DMD gene. This region was recently shown by both cDNA analysis (M. Koenig et al., 1987; Cell 50: 509-517), and field inversion electrophoresis studies (J.T. Den Dunnen et al., 1987, Nature (London) 329: 640-642) to be specifically prone to deletions. In addition, P20 detects MspI and EcoRV RFLPs, informative in 48% of the carrier females. Together, these properties make P20 useful for carrier detection, prenatal diagnosis, and the study of deletion induction in both DMD and BMD.Entities:
Mesh:
Year: 1988 PMID: 2900805 DOI: 10.1016/0888-7543(88)90090-0
Source DB: PubMed Journal: Genomics ISSN: 0888-7543 Impact factor: 5.736