Generation of disease-specific and CRISPR/Cas9-mediated gene-corrected iPS cells from a patient with adult progeria Werner syndrome

Hisaya Kato,Yoshiro Maezawa,Yasuo Ouchi,Naoya Takayama,Masamitsu Sone,Kanako Sone,Aki Takada-Watanabe,Kyoko Tsujimura,Masaya Koshizaka,Sayaka Nagasawa,Hisako Saitoh,Manami Ohtaka,Mahito Nakanishi,Hidetoshi Tahara,Akira Shimamoto,Atsushi Iwama,Koji Eto,Koutaro Yokote

Generation of disease-specific and CRISPR/Cas9-mediated gene-corrected iPS cells from a patient with adult progeria Werner syndrome

2021

Hisaya Kato
Yoshiro Maezawa
Yasuo Ouchi
Naoya Takayama
Masamitsu Sone
Kanako Sone
Aki Takada-Watanabe
Kyoko Tsujimura
Masaya Koshizaka
Sayaka Nagasawa
Hisako Saitoh
Manami Ohtaka
Mahito Nakanishi
Hidetoshi Tahara
Akira Shimamoto
Atsushi Iwama
Koji Eto
Koutaro Yokote

Abstract Adult progeria Werner syndrome (WS), a rare autosomal recessive disorder, is characterized by accelerated aging symptoms after puberty. The causative gene, WRN, is a member of the RecQ DNA helicase family and is predominantly involved in DNA replication, repair, and telomere maintenance. Here, we report the generation of iPS cells from a patient with WS and correction of the WRN gene by the CRISPR/Cas9-mediated method. These iPSC lines would be a valuable resource for deciphering the pathogenesis of WS.

Keywords:

CRISPR
Genetics
Helicase
Gene
DNA replication
Telomere
Biology
Induced pluripotent stem cell
Progeria
Werner syndrome

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