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Longitudinal clonal tracking in humanized mice reveals sustained polyclonal repopulation of gene-modified human-HSPC despite vector integration bias.

Gajendra W SuryawanshiHubert ArokiumSanggu KimWannisa KhamaikawinSamantha LinSaki ShimizuKoollawat ChupraditYooJin LeeYiming XieXin GuanVasantika SuryawanshiAngela P PressonDong-Sung AnIrvin S Y Chen
Published in: Stem cell research & therapy (2021)
Human repopulation in mice is polyclonal and stabilizes more rapidly than that previously observed in humans. VIS preference for H3K36me3 has no apparent negative effects on HSPC repopulation. Our study provides a methodology to longitudinally track clonal repopulation in small animal models extensively used for stem cell and gene therapy research and with lentiviral vectors designed for clinical applications. Results of this study provide a framework for understanding the clonal behavior of human HPSC repopulating in a mouse environment, critical for translating results from humanized mice models to the human settings.
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