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. 2010 Aug 6;7(2):225-39.
doi: 10.1016/j.stem.2010.06.018.

Molecular pathway and cell state responsible for dissociation-induced apoptosis in human pluripotent stem cells

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Molecular pathway and cell state responsible for dissociation-induced apoptosis in human pluripotent stem cells

Masatoshi Ohgushi et al. Cell Stem Cell. .
Free article

Abstract

Human embryonic stem cells (hESCs), unlike mouse ones (mESCs), are vulnerable to apoptosis upon dissociation. Here, we show that the apoptosis, which is of a nonanoikis type, is caused by ROCK-dependent hyperactivation of actomyosin and efficiently suppressed by the myosin inhibitor Blebbistatin. The actomyosin hyperactivation is triggered by the loss of E-cadherin-dependent intercellular contact and also observed in dissociated mouse epiblast-derived pluripotent cells but not in mESCs. We reveal that Abr, a unique Rho-GEF family factor containing a functional Rac-GAP domain, is an indispensable upstream regulator of the apoptosis and ROCK/myosin hyperactivation. Rho activation coupled with Rac inhibition is induced in hESCs upon dissociation, but not in Abr-depleted hESCs or mESCs. Furthermore, artificial Rho or ROCK activation with Rac inhibition restores the vulnerability of Abr-depleted hESCs to dissociation-induced apoptosis. Thus, the Abr-dependent "Rho-high/Rac-low" state plays a decisive role in initiating the dissociation-induced actomyosin hyperactivation and apoptosis in hESCs.

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  • Dying alone: a tale of rho.
    Samuel MS, Olson MF. Samuel MS, et al. Cell Stem Cell. 2010 Aug 6;7(2):135-6. doi: 10.1016/j.stem.2010.07.002. Cell Stem Cell. 2010. PMID: 20682437

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