Abstract:Homozygous E6V alleles in the beta globin gene cause disease in the majority of sickle cell patients and the use of gene editing technologies to correct this mutation in hematopoietic stem cells offers the potential to cure disease. Approaches utilizing viral transduction or exogenous nucleases to facilitate gene editing merit consideration, but also invoke a number of safety and manufacturing concerns that are avoided through use of peptide-nucleic acids (PNAs) for triplex gene editing.
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