Association of Human iPSC Gene Signatures and X Chromosome Dosage with Two Distinct Cardiac Differentiation Trajectories
Author(s) -
Agnieszka D’AntonioChronowska,
Margaret K. R. Donovan,
William W. Greenwald,
Jennifer Nguyen,
Kyohei Fujita,
Sherin I. Hashem,
Hiroko Matsui,
Francesca Soncin,
Mana M. Parast,
Michelle C. Ward,
Florence Coulet,
Erin N. Smith,
Eric Adler,
Matteo D’Antonio,
Kelly A. Frazer
Publication year - 2019
Publication title -
stem cell reports
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 3.207
H-Index - 76
ISSN - 2213-6711
DOI - 10.1016/j.stemcr.2019.09.011
Subject(s) - biology , genetics , gene , chromosome , association (psychology) , x chromosome , computational biology , evolutionary biology , philosophy , epistemology
Despite the importance of understanding how variability across induced pluripotent stem cell (iPSC) lines due to non-genetic factors (clone and passage) influences their differentiation outcome, large-scale studies capable of addressing this question have not yet been conducted. Here, we differentiated 191 iPSC lines to generate iPSC-derived cardiovascular progenitor cells (iPSC-CVPCs). We observed cellular heterogeneity across the iPSC-CVPC samples due to varying fractions of two cell types: cardiomyocytes (CMs) and epicardium-derived cells (EPDCs). Comparing the transcriptomes of CM-fated and EPDC-fated iPSCs, we discovered that 91 signature genes and X chromosome dosage differences are associated with these two distinct cardiac developmental trajectories. In an independent set of 39 iPSCs differentiated into CMs, we confirmed that sex and transcriptional differences affect cardiac-fate outcome. Our study provides novel insights into how iPSC transcriptional and X chromosome gene dosage differences influence their response to differentiation stimuli and, hence, cardiac cell fate.
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