Interstrand crosslinking of homologous repair template DNA enhances gene editing in human cells.

Hannah I GhasemiJulien BacalAmanda C YoonKatherine U TavasoliCarmen CruzJonathan T VuBrooke M GardnerChristopher D Richardson

Published in: Nature biotechnology (2023)

We describe a strategy to boost the efficiency of gene editing via homology-directed repair (HDR) by covalently modifying the template DNA with interstrand crosslinks. Crosslinked templates (xHDRTs) increase Cas9-mediated editing efficiencies by up to fivefold in K562, HEK293T, U2OS, iPS and primary T cells. Increased editing from xHDRTs is driven by events on the template molecule and requires ataxia telangiectasia and Rad3-related (ATR) kinase and components of the Fanconi anemia pathway.

Keyphrases

crispr cas
genome editing
circulating tumor
molecularly imprinted
dna repair
cell free
dna damage
single molecule
chronic kidney disease
nucleic acid
early onset
dna damage response
protein kinase
hyaluronic acid
oxidative stress
iron deficiency