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Regional genomic instability predisposes to complex dystrophin gene rearrangements.

Authors :
Oshima, Junko
Magner, Daniel B.
Lee, Jennifer A.
Breman, Amy M.
Schmitt, Eric S.
White, Lisa D.
Crowe, Carol A.
Merrill, Michelle
Jayakar, Parul
Rajadhyaksha, Aparna
Eng, Christine M.
del Gaudio, Daniela
Source :
Human Genetics. Sep2009, Vol. 126 Issue 3, p411-423. 13p. 2 Diagrams, 3 Charts, 5 Graphs.
Publication Year :
2009

Abstract

Mutations in the dystrophin gene ( DMD) cause Duchenne and Becker muscular dystrophies and the majority of cases are due to DMD gene rearrangements. Despite the high incidence of these aberrations, little is known about their causative molecular mechanism(s). We examined 792 DMD/BMD clinical samples by oligonucleotide array-CGH and report on the junction sequence analysis of 15 unique deletion cases and three complex intragenic rearrangements to elucidate potential underlying mechanism(s). Furthermore, we present three cases with intergenic rearrangements involving DMD and neighboring loci. The cases with intragenic rearrangements include an inversion with flanking deleted sequences; a duplicated segment inserted in direct orientation into a deleted region; and a splicing mutation adjacent to a deletion. Bioinformatic analysis demonstrated that 7 of 12 breakpoints combined among 3 complex cases aligned with repetitive sequences, as compared to 4 of 30 breakpoints for the 15 deletion cases. Moreover, the inversion/deletion case may involve a stem-loop structure that has contributed to the initiation of this rearrangement. For the duplication/deletion and splicing mutation/deletion cases, the presence of the first mutation, either a duplication or point mutation, may have elicited the deletion events in an attempt to correct preexisting mutations. While NHEJ is one potential mechanism for these complex rearrangements, the highly complex junction sequence of the inversion/deletion case suggests the involvement of a replication-based mechanism. Our results support the notion that regional genomic instability, aided by the presence of repetitive elements, a stem-loop structure, and possibly preexisting mutations, may elicit complex rearrangements of the DMD gene. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
03406717
Volume :
126
Issue :
3
Database :
Academic Search Index
Journal :
Human Genetics
Publication Type :
Academic Journal
Accession number :
44206618
Full Text :
https://doi.org/10.1007/s00439-009-0679-9