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A pluripotent developmental state confers a low fidelity of chromosome segregation

Chenhui Deng, Amanda Ya, Duane A. Compton, Kristina Godek

2023Stem Cell Reports16 citationsDOIOpen Access PDF

Abstract

During in vitro propagation, human pluripotent stem cells (hPSCs) frequently become aneuploid with incorrect chromosome numbers due to mitotic chromosome segregation errors. Yet, it is not understood why hPSCs exhibit a low mitotic fidelity. Here, we investigate the mechanisms responsible for mitotic errors in hPSCs and show that the primary cause is lagging chromosomes in anaphase with improper merotelic microtubule attachments. Accordingly, short-term treatment (<24 h) with small molecules that prolong mitotic duration or destabilize chromosome microtubule attachments reduces merotelic errors and lagging chromosome rates, although hPSCs adapt and lagging chromosome rates rebound upon long-term (>24 h) microtubule destabilization. Strikingly, we also demonstrate that mitotic error rates correlate with developmental potential decreasing or increasing upon loss or gain of pluripotency, respectively. Thus, a low mitotic fidelity is an inherent and conserved phenotype of hPSCs. Moreover, chromosome segregation fidelity depends on developmental state in normal human cells.

Topics & Concepts

BiologyMitosisAnaphaseChromosome segregationInduced pluripotent stem cellChromosomeCell biologyGeneticsEmbryonic stem cellGeneMicrotubule and mitosis dynamicsPluripotent Stem Cells ResearchRenal and related cancers