Somatic Coding Mutations in Human Induced Pluripotent Stem Cells

Overview

Journal Nature

Specialty Science

Date 2011 Mar 4

PMID 21368825

Citations 602

Authors

Athurva Gore

Zhe Li

Ho-Lim Fung

Jessica E Young

Suneet Agarwal

Jessica Antosiewicz-Bourget

Isabel Canto

Alessandra Giorgetti

Mason A Israel

Evangelos Kiskinis

Je-Hyuk Lee

Yuin-Han Loh

Philip D Manos

Nuria Montserrat

Athanasia D Panopoulos

Sergio Ruiz

Melissa L Wilbert

Junying Yu

Ewen F Kirkness

Juan Carlos Izpisua Belmonte

Derrick J Rossi

James A Thomson

Kevin Eggan

George Q Daley

Lawrence S B Goldstein

Kun Zhang

Affiliations

Soon will be listed here.

Abstract

Defined transcription factors can induce epigenetic reprogramming of adult mammalian cells into induced pluripotent stem cells. Although DNA factors are integrated during some reprogramming methods, it is unknown whether the genome remains unchanged at the single nucleotide level. Here we show that 22 human induced pluripotent stem (hiPS) cell lines reprogrammed using five different methods each contained an average of five protein-coding point mutations in the regions sampled (an estimated six protein-coding point mutations per exome). The majority of these mutations were non-synonymous, nonsense or splice variants, and were enriched in genes mutated or having causative effects in cancers. At least half of these reprogramming-associated mutations pre-existed in fibroblast progenitors at low frequencies, whereas the rest occurred during or after reprogramming. Thus, hiPS cells acquire genetic modifications in addition to epigenetic modifications. Extensive genetic screening should become a standard procedure to ensure hiPS cell safety before clinical use.

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