Genetic aberrations in iPSCs are introduced by a transient G1/S cell cycle checkpoint deficiency

Author:

Araki Ryoko,Hoki Yuko,Suga Tomo,Obara ChizukaORCID,Sunayama Misato,Imadome Kaori,Fujita Mayumi,Kamimura Satoshi,Nakamura Miki,Wakayama Sayaka,Nagy AndrasORCID,Wakayama TeruhikoORCID,Abe Masumi

Abstract

AbstractA number of point mutations have been identified in reprogrammed pluripotent stem cells such as iPSCs and ntESCs. The molecular basis for these mutations has remained elusive however, which is a considerable impediment to their potential medical application. Here we report a specific stage at which iPSC generation is not reduced in response to ionizing radiation, i.e. radio-resistance. Quite intriguingly, a G1/S cell cycle checkpoint deficiency occurs in a transient fashion at the initial stage of the genome reprogramming process. These cancer-like phenomena, i.e. a cell cycle checkpoint deficiency resulting in the accumulation of point mutations, suggest a common developmental pathway between iPSC generation and tumorigenesis. This notion is supported by the identification of specific cancer mutational signatures in these cells. We describe efficient generation of human integration-free iPSCs using erythroblast cells, which have only a small number of point mutations and INDELs, none of which are in coding regions.

Funder

Mitsubishi Foundation

Uehara Memorial Foundation

Takeda Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry

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