miR-371-3 expression predicts neural differentiation propensity in human pluripotent stem cells

Hyesoo Kim; Gabsang Lee; Yosif Ganat; Eirini P. Papapetrou; Inna Lipchina; Nicholas D. Socci; Michel Sadelain; Lorenz Studer

doi:10.1016/j.stem.2011.04.002

miR-371-3 expression predicts neural differentiation propensity in human pluripotent stem cells

Hyesoo Kim, Gabsang Lee, Yosif Ganat, Eirini P. Papapetrou, Inna Lipchina, Nicholas D. Socci, Michel Sadelain, Lorenz Studer

Research output: Contribution to journal › Article › peer-review

99 Scopus citations

Abstract

The use of pluripotent stem cells in regenerative medicine and disease modeling is complicated by the variation in differentiation properties between lines. In this study, we characterized 13 human embryonic stem cell (hESC) and 26 human induced pluripotent stem cell (hiPSC) lines to identify markers that predict neural differentiation behavior. At a general level, markers previously known to distinguish mouse ESCs from epiblast stem cells (EPI-SCs) correlated with neural differentiation behavior. More specifically, quantitative analysis of miR-371-3 expression prospectively identified hESC and hiPSC lines with differential neurogenic differentiation propensity and in vivo dopamine neuron engraftment potential. Transient KLF4 transduction increased miR-371-3 expression and altered neurogenic behavior and pluripotency marker expression. Conversely, suppression of miR-371-3 expression in KLF4-transduced cells rescued neural differentiation propensity. miR-371-3 expression level therefore appears to have both a predictive and a functional role in determining human pluripotent stem cell neurogenic differentiation behavior.

Original language	English (US)
Pages (from-to)	695-706
Number of pages	12
Journal	Cell stem cell
Volume	8
Issue number	6
DOIs	https://doi.org/10.1016/j.stem.2011.04.002
State	Published - Jun 3 2011
Externally published	Yes

ASJC Scopus subject areas

Molecular Medicine
Genetics
Cell Biology

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title = "miR-371-3 expression predicts neural differentiation propensity in human pluripotent stem cells",

abstract = "The use of pluripotent stem cells in regenerative medicine and disease modeling is complicated by the variation in differentiation properties between lines. In this study, we characterized 13 human embryonic stem cell (hESC) and 26 human induced pluripotent stem cell (hiPSC) lines to identify markers that predict neural differentiation behavior. At a general level, markers previously known to distinguish mouse ESCs from epiblast stem cells (EPI-SCs) correlated with neural differentiation behavior. More specifically, quantitative analysis of miR-371-3 expression prospectively identified hESC and hiPSC lines with differential neurogenic differentiation propensity and in vivo dopamine neuron engraftment potential. Transient KLF4 transduction increased miR-371-3 expression and altered neurogenic behavior and pluripotency marker expression. Conversely, suppression of miR-371-3 expression in KLF4-transduced cells rescued neural differentiation propensity. miR-371-3 expression level therefore appears to have both a predictive and a functional role in determining human pluripotent stem cell neurogenic differentiation behavior.",

author = "Hyesoo Kim and Gabsang Lee and Yosif Ganat and Papapetrou, {Eirini P.} and Inna Lipchina and Socci, {Nicholas D.} and Michel Sadelain and Lorenz Studer",

note = "Funding Information: We would like to thank J. Hendrikx (SKI Flow Cytometry Core lab), A. Viale (SKI Genomics Core lab), and M. Leversha (Molecular Cytogenetics core) for excellent technical support. We also thank M. Tomishima for critical review of the manuscript, P. Tesar for providing mouse EPI-SCs, and C. Rohena for help with teratoma data. The work was supported by grants from the Kinetics Foundation, the Starr Foundation, NYSTEM, and the European Commission project NeuroStemCell. G.L. was supported by a NYSCF, Druckenmiller fellowship. ",

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AU - Kim, Hyesoo

AU - Lee, Gabsang

AU - Ganat, Yosif

AU - Papapetrou, Eirini P.

AU - Lipchina, Inna

AU - Socci, Nicholas D.

AU - Sadelain, Michel

AU - Studer, Lorenz

N1 - Funding Information: We would like to thank J. Hendrikx (SKI Flow Cytometry Core lab), A. Viale (SKI Genomics Core lab), and M. Leversha (Molecular Cytogenetics core) for excellent technical support. We also thank M. Tomishima for critical review of the manuscript, P. Tesar for providing mouse EPI-SCs, and C. Rohena for help with teratoma data. The work was supported by grants from the Kinetics Foundation, the Starr Foundation, NYSTEM, and the European Commission project NeuroStemCell. G.L. was supported by a NYSCF, Druckenmiller fellowship.

PY - 2011/6/3

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N2 - The use of pluripotent stem cells in regenerative medicine and disease modeling is complicated by the variation in differentiation properties between lines. In this study, we characterized 13 human embryonic stem cell (hESC) and 26 human induced pluripotent stem cell (hiPSC) lines to identify markers that predict neural differentiation behavior. At a general level, markers previously known to distinguish mouse ESCs from epiblast stem cells (EPI-SCs) correlated with neural differentiation behavior. More specifically, quantitative analysis of miR-371-3 expression prospectively identified hESC and hiPSC lines with differential neurogenic differentiation propensity and in vivo dopamine neuron engraftment potential. Transient KLF4 transduction increased miR-371-3 expression and altered neurogenic behavior and pluripotency marker expression. Conversely, suppression of miR-371-3 expression in KLF4-transduced cells rescued neural differentiation propensity. miR-371-3 expression level therefore appears to have both a predictive and a functional role in determining human pluripotent stem cell neurogenic differentiation behavior.

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miR-371-3 expression predicts neural differentiation propensity in human pluripotent stem cells

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