Molecular therapy. Nucleic acids

Prime editing fixes heart muscle disease caused by RBM20-P633L mutation in human heart cells

Updated

Abstract

Essence

Prime editing corrected an RBM20-P633L cardiomyopathy mutation in human iPSC-derived cardiomyocytes and rescued RBM20 localization and CAMK2D splicing phenotypes in vitro.

Evidence

A cell-model study screened pegRNAs in HEK293T target arrays and then used PE4 in homozygous P633L/P633L human iPSC-derived cardiomyocytes, reaching 34.8% average T-to-C editing with low off-target editing.

Caveat

The evidence comes from engineered screening cells and iPSC-derived cardiomyocytes, not an in vivo cardiac therapy.

Simplified

Full Text

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