A large CRISPR-induced bystander mutation causes immune dysregulation.

Dimitre R SimeonovAlexander J BrandtAlice Y ChanJessica T CortezZhongmei LiJonathan M WooYoujin LeeClaudia M B CarvalhoAlyssa C IndartTheodore L RothJames Y ZouAndrew P MayJames R LupskiMark S AndersonF William BuaasDaniel S RokhsarAlexander Marson

Published in: Communications biology (2019)

A persistent concern with CRISPR-Cas9 gene editing has been the potential to generate mutations at off-target genomic sites. While CRISPR-engineering mice to delete a ~360 bp intronic enhancer, here we discovered a founder line that had marked immune dysregulation caused by a 24 kb tandem duplication of the sequence adjacent to the on-target deletion. Our results suggest unintended repair of on-target genomic cuts can cause pathogenic "bystander" mutations that escape detection by routine targeted genotyping assays.

Keyphrases

crispr cas
genome editing
genome wide
copy number
high throughput
dna methylation
high glucose
type diabetes
clinical practice
diabetic rats
cancer therapy
adipose tissue
quantum dots
label free
wild type
amino acid
stress induced