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Dissecting the Structure and Mechanism of a Complex Duplication–Triplication Rearrangement in the DMD Gene
Authors:Aliya Ishmukhametova  Jian‐Min Chen  Rafaëlle Bernard  Bernard de Massy  Frédéric Baudat  Amandine Boyer  Déborah Méchin  Delphine Thorel  Brigitte Chabrol  Marie‐Claire Vincent  Mireille Claustres  Sylvie Tuffery‐Giraud
Affiliation:1. Université Montpellier 1, UFR médecine, , Montpellier, F‐34000 France;2. CHU Montpellier, H?pital Arnaud de Villeneuve, Laboratoire de Génétique Moléculaire, , Montpellier, F‐34000 France;3. INSERM U1078 and établissement Fran?ais du Sang (EFS) – Bretagne, , Brest, F‐29218 France;4. Laboratoire de Génétique Moléculaire, H?pital de la Timone CHU, , Marseille, F‐13385 France;5. Institut de Génétique Humaine, UPR1142, CNRS, , Montpellier, France;6. CHU La Timone, Service de Neurologie Pédiatrique, , Marseille, F‐13385 France;7. INSERM, U827, , Montpellier, F‐34000 France
Abstract:
Pathogenic complex genomic rearrangements are being increasingly characterized at the nucleotide level, providing unprecedented opportunities to evaluate the complexities of mutational mechanisms. Here, we report the molecular characterization of a complex duplication–triplication rearrangement involving exons 45–60 of the DMD gene. Inverted repeats facilitated this complex rearrangement, which shares common genomic organization with the recently described duplication‐inverted triplication–duplication (DUP–TRP/INV‐DUP) events; specifically, a 690‐kb region comprising DMD exons from 45 to 60 was duplicated in tandem, and another 46‐kb segment containing exon 51 was inserted inversely in between them. Taking into consideration (1) the presence of a predicted PRDM9 binding site in the near vicinity of the junction involving two inverted L1 elements and (2) the inherent properties of X–Y chromosome recombination during male meiosis, we proposed an alternative two‐step model for the generation of this X‐linked DMD DUP–TRP/INV‐DUP event.
Keywords:DMD  complex rearrangements  inverted repeats  PRDM9
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