An error in dystrophin mRNA processing in golden retriever muscular dystrophy, an animal homologue of Duchenne muscular dystrophy
NJH Sharp, JN Kornegay, SD Van Camp… - Genomics, 1992 - Elsevier
NJH Sharp, JN Kornegay, SD Van Camp, MH Herbstreith, SL Secore, S Kettle, WY Hung…
Genomics, 1992•ElsevierGolden retriever muscular dystrophy (GRMD) is a spontaneous, X-linked, progressively fatal
disease of dogs and is also a homologue of Duchenne muscular dystrophy (DMD). Two-
thirds of DMD patients carry detectable deletions in their dystrophin gene in normal and
GRMD dogs has failed to demonstrate any detectable loss of exons. Here, we have
demonstrated a RNA processing error in GRMD that results from a single base change in
the 3′ consensus splice site of intron 6. The seventh exon is then skipped, which predicts a …
disease of dogs and is also a homologue of Duchenne muscular dystrophy (DMD). Two-
thirds of DMD patients carry detectable deletions in their dystrophin gene in normal and
GRMD dogs has failed to demonstrate any detectable loss of exons. Here, we have
demonstrated a RNA processing error in GRMD that results from a single base change in
the 3′ consensus splice site of intron 6. The seventh exon is then skipped, which predicts a …
Abstract
Golden retriever muscular dystrophy (GRMD) is a spontaneous, X-linked, progressively fatal disease of dogs and is also a homologue of Duchenne muscular dystrophy (DMD). Two-thirds of DMD patients carry detectable deletions in their dystrophin gene in normal and GRMD dogs has failed to demonstrate any detectable loss of exons. Here, we have demonstrated a RNA processing error in GRMD that results from a single base change in the 3′ consensus splice site of intron 6. The seventh exon is then skipped, which predicts a termination of the dystrophin reading frame within its N-terminal domain in exon 8. This is the first example of dystrophin deficiency caused by a splice-site mutation.
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