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Generation of a Panel of Induced Pluripotent Stem Cells From Chimpanzees: a Resource for Comparative Functional Genomics

Irene Gallego Romero, Bryan J Pavlovic, Irene Hernando-Herraez, Nicholas E Banovich, Courtney L Kagan, Jonathan E Burnett, Constance H Huang, Amy Mitrano, Claudia I Chavarria, Inbar F Ben-Nun, Yingchun Li, Karen Sabatini, Trevor R Leonardo, Mana Parast, Tomas Marques-Bonet, Louise C Laurent, Jeanne F Loring, Yoav Gilad
doi: https://doi.org/10.1101/008862
Irene Gallego Romero
University of Chicago;
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  • For correspondence: ireneg@uchicago.edu
Bryan J Pavlovic
University of Chicago;
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Irene Hernando-Herraez
Institute of Evolutionary Biology;
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Nicholas E Banovich
University of Chicago;
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Courtney L Kagan
University of Chicago;
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Jonathan E Burnett
University of Chicago;
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Constance H Huang
University of Chicago;
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Amy Mitrano
University of Chicago;
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Claudia I Chavarria
University of Chicago;
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Inbar F Ben-Nun
The Scripps Research Institute;
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Yingchun Li
University of California San Diego;
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Karen Sabatini
University of California San Diego;
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Trevor R Leonardo
University of California San Diego;
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Mana Parast
University of California San Diego;
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Tomas Marques-Bonet
Centro Nacional de Análisis Genómico
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Louise C Laurent
University of California San Diego;
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Jeanne F Loring
The Scripps Research Institute;
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Yoav Gilad
University of Chicago;
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Abstract

Comparative genomics studies in primates are extremely restricted because we only have access to a few types of cell lines from non-human apes and to a limited collection of frozen tissues. In order to gain better insight into regulatory processes that underlie variation in complex phenotypes, we must have access to faithful model systems for a wide range of tissues and cell types. To facilitate this, we have generated a panel of 7 fully characterized chimpanzee (Pan troglodytes) induced pluripotent stem cell (iPSC) lines derived from fibroblasts of healthy donors. All lines appear to be free of integration from exogenous reprogramming vectors, can be maintained using standard iPSC culture techniques, and have proliferative and differentiation potential similar to human and mouse lines. To begin demonstrating the utility of comparative iPSC panels, we collected RNA sequencing data and methylation profiles from the chimpanzee iPSCs and their corresponding fibroblast precursors, as well as from 7 human iPSCs and their precursors, which were of multiple cell type and population origins. Overall, we observed much less regulatory variation within species in the iPSCs than in the somatic precursors, indicating that the reprogramming process has erased many of the differences observed between somatic cells of different origins. We identified 4,918 differentially expressed genes and 3,598 differentially methylated regions between iPSCs of the two species, many of which are novel inter-species differences that were not observed between the somatic cells of the two species. Our panel will help realise the potential of iPSCs in primate studies, and in combination with genomic technologies, transform studies of comparative evolution.

Copyright 
The copyright holder for this preprint is the author/funder. It is made available under a CC-BY-ND 4.0 International license.
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  • Posted September 8, 2014.

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Generation of a Panel of Induced Pluripotent Stem Cells From Chimpanzees: a Resource for Comparative Functional Genomics
Irene Gallego Romero, Bryan J Pavlovic, Irene Hernando-Herraez, Nicholas E Banovich, Courtney L Kagan, Jonathan E Burnett, Constance H Huang, Amy Mitrano, Claudia I Chavarria, Inbar F Ben-Nun, Yingchun Li, Karen Sabatini, Trevor R Leonardo, Mana Parast, Tomas Marques-Bonet, Louise C Laurent, Jeanne F Loring, Yoav Gilad
bioRxiv 008862; doi: https://doi.org/10.1101/008862
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Generation of a Panel of Induced Pluripotent Stem Cells From Chimpanzees: a Resource for Comparative Functional Genomics
Irene Gallego Romero, Bryan J Pavlovic, Irene Hernando-Herraez, Nicholas E Banovich, Courtney L Kagan, Jonathan E Burnett, Constance H Huang, Amy Mitrano, Claudia I Chavarria, Inbar F Ben-Nun, Yingchun Li, Karen Sabatini, Trevor R Leonardo, Mana Parast, Tomas Marques-Bonet, Louise C Laurent, Jeanne F Loring, Yoav Gilad
bioRxiv 008862; doi: https://doi.org/10.1101/008862

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