Apoptosis, G1 Phase Stall, and Premature Differentiation Account for Low Chimeric Competence of Human and Rhesus Monkey Naive Pluripotent Stem Cells
Author(s) -
Irène Aksoy,
Cloé Rognard,
Anaïs Moulin,
Guillaume Marcy,
Etienne Masfaraud,
Florence Wianny,
Véronique Cortay,
Angèle Bellemin-Ménard,
Nathalie Doerflinger,
Ma Dirheimer,
Chloé Mayère,
Pierre-Yves Bourillot,
Cian J. Lynch,
Olivier Raineteau,
Thierry Joly,
Colette Dehay,
Manuel Serrano,
Marielle Afanassieff,
Pierre Savatier
Publication year - 2020
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.2020.12.004
Subject(s) - biology , embryonic stem cell , induced pluripotent stem cell , chimera (genetics) , reprogramming , microbiology and biotechnology , stem cell , embryo , genetics , cell , gene
After reprogramming to naive pluripotency, human pluripotent stem cells (PSCs) still exhibit very low ability to make interspecies chimeras. Whether this is because they are inherently devoid of the attributes of chimeric competency or because naive PSCs cannot colonize embryos from distant species remains to be elucidated. Here, we have used different types of mouse, human, and rhesus monkey naive PSCs and analyzed their ability to colonize rabbit and cynomolgus monkey embryos. Mouse embryonic stem cells (ESCs) remained mitotically active and efficiently colonized host embryos. In contrast, primate naive PSCs colonized host embryos with much lower efficiency. Unlike mouse ESCs, they slowed DNA replication after dissociation and, after injection into host embryos, they stalled in the G1 phase and differentiated prematurely, regardless of host species. We conclude that human and non-human primate naive PSCs do not efficiently make chimeras because they are inherently unfit to remain mitotically active during colonization.
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