Efficient, continuous mutagenesis in human cells using a pseudo-random DNA editor.

Haiqi Chen Sophia LiuSamuel PadulaDaniel LesmanKettner GriswoldAllen Z LinTongtong ZhaoJamie L Marshall Fei Chen

Published in: Nature biotechnology (2019)

Here we describe TRACE (T7 polymerase-driven continuous editing), a method that enables continuous, targeted mutagenesis in human cells using a cytidine deaminase fused to T7 RNA polymerase. TRACE induces high rates of mutagenesis over multiple cell generations in genes under the control of a T7 promoter integrated in the genome. We used TRACE in a MEK1 inhibitor-resistance screen, and identified functionally correlated mutations.

Keyphrases

crispr cas
heavy metals
genome wide
dna methylation
gene expression
single cell
transcription factor
high throughput
cancer therapy
single molecule
risk assessment
cell free
cell proliferation
drug delivery
mesenchymal stem cells
genome wide identification