Reprogramming of DNA Replication Timing

Author:

Shufaro Yoel1,Lacham-Kaplan Orly2,Tzuberi Ben-Zion3,McLaughlin John4,Trounson Alan2,Cedar Howard3,Reubinoff Benjamin E.1

Affiliation:

1. The Hadassah Human Embryonic Stem Cells Research Center, the Goldyne-Savad Institute of Gene Therapy, and the Department of OB & GYN, Hadassah University Hospital, Jerusalem 91120, Israel

2. Monash Immunology and Stem Cell Laboratories, Monash University, Melbourne, Australia

3. Department of Developmental Biology and Cancer Research, Israel-Canada Institute for Medical Research, Hebrew University Medical School, Ein-Kerem, Jerusalem 91120, Israel

4. The Research Institute at Nationwide Children's Hospital Columbus, Ohio 43205, USA

Abstract

Abstract Replication timing is an important developmentally regulated regional property that is correlated with chromosome structure and gene expression, but little is known about the establishment and maintenance of these patterns. Here we followed the fate of replication timing patterns in cells that undergo reprogramming either through somatic-cell nuclear transplantation or by the generation of induced pluripotential stem cells. We have investigated three different paradigms, stage-specific replication timing, parental allele-specific asynchrony (imprinted regions), and random allelic asynchronous replication. In all cases, somatic replication timing patterns were reset exactly at the appropriate stage in early development and could be properly established upon re-differentiation. Taken together, these results suggest that, unlike DNA methylation, the molecular mechanisms governing replication timing are not only stable but can also be easily reprogrammed.

Publisher

Oxford University Press (OUP)

Subject

Cell Biology,Developmental Biology,Molecular Medicine

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