Publications by authors named "Abbass Jaber"

Article Synopsis
  • * Recent advancements include the approval of the first gene therapy using a recombinant adeno-associated vector (rAAV) to deliver a microdystrophin, but significant therapeutic challenges remain.
  • * Major issues include potential immunotoxicity and hepatotoxicity from high doses of rAAV, as well as functional limitations and immunological risks associated with microdystrophin, prompting further exploration for improved treatment options.
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Duchenne Muscular dystrophy (DMD), a yet-incurable X-linked recessive disorder that results in muscle wasting and loss of ambulation is due to mutations in the dystrophin gene. Exonic duplications of dystrophin gene are a common type of mutations found in DMD patients. In this study, we utilized a single guide RNA CRISPR strategy targeting intronic regions to delete the extra duplicated regions in patient myogenic cells carrying duplication of exon 2, exons 2-9, and exons 8-9 in the DMD gene.

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Duchenne muscular dystrophy (DMD) is the most common and cureless muscle pediatric genetic disease, which is caused by the lack or the drastically reduced expression of dystrophin. Experimental therapeutic approaches for DMD have been mainly focused in recent years on attempts to restore the expression of dystrophin. While significant progress was achieved, the therapeutic benefit of treated patients is still unsatisfactory.

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