Correction of the Mutation Responsible for Sickle Cell Anemia by an RNA-DNA Oligonucleotide
Allyson Cole-Strauss(Thomas Jefferson University), Kyonggeun Yoon(Thomas Jefferson University), Yufei Xiang(Thomas Jefferson University), Bruce C. Byrne(Cooper University Hospital), Michael C. Rice(Thomas Jefferson University), Jeff Gryn(Cooper University Hospital), William K. Holloman(Cornell University), Eric B. Kmiec(Thomas Jefferson University)
Cited by 319
Abstract
A chimeric oligonucleotide composed of DNA and modified RNA residues was used to direct correction of the mutation in the hemoglobin betaS allele. After introduction of the chimeric molecule into lymphoblastoid cells homozygous for the betaS mutation, there was a detectable level of gene conversion of the mutant allele to the normal sequence. The efficient and specific conversion directed by chimeric molecules may hold promise as a therapeutic method for the treatment of genetic diseases.
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