Single-cell analysis reveals that expression of nanog is biallelic and equally variable as that of other pluripotency factors in mouse escs

Dina A. Faddah; Haoyi Wang; Albert Wu Cheng; Yarden Katz; Yosef Buganim; Rudolf Jaenisch

doi:10.1016/j.stem.2013.04.019

Single-cell analysis reveals that expression of nanog is biallelic and equally variable as that of other pluripotency factors in mouse escs

Dina A. Faddah, Haoyi Wang, Albert Wu Cheng, Yarden Katz, Yosef Buganim, Rudolf Jaenisch

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

Abstract

The homeodomain transcription factor Nanog is a central part of the core pluripotency transcriptional network and plays a critical role in embryonic stem cell (ESC) self-renewal. Several reports have suggested that Nanog expression is allelically regulated and that transient downregulation of Nanog in a subset of pluripotent cells predisposes them toward differentiation. Using single-cell gene expression analyses combined with different reporters for the two alleles of Nanog, we show that Nanog is biallelically expressed in ESCs independently of culture condition. We also show that the overall variation in endogenous Nanog expression inESCs is very similar to that of several other pluripotency markers. Our analysis suggests that reporter-based studies of gene expression in pluripotent cells can be significantly influenced by the gene-targeting strategy and genetic background employed. 2013

Original language	English
Pages (from-to)	23-29
Number of pages	7
Journal	Cell Stem Cell
Volume	13
Issue number	1
DOIs	https://doi.org/10.1016/j.stem.2013.04.019
State	Published - 3 Jul 2013
Externally published	Yes

All Science Journal Classification (ASJC) codes

Molecular Medicine
Genetics
Cell Biology

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10.1016/j.stem.2013.04.019

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title = "Single-cell analysis reveals that expression of nanog is biallelic and equally variable as that of other pluripotency factors in mouse escs",

abstract = "The homeodomain transcription factor Nanog is a central part of the core pluripotency transcriptional network and plays a critical role in embryonic stem cell (ESC) self-renewal. Several reports have suggested that Nanog expression is allelically regulated and that transient downregulation of Nanog in a subset of pluripotent cells predisposes them toward differentiation. Using single-cell gene expression analyses combined with different reporters for the two alleles of Nanog, we show that Nanog is biallelically expressed in ESCs independently of culture condition. We also show that the overall variation in endogenous Nanog expression inESCs is very similar to that of several other pluripotency markers. Our analysis suggests that reporter-based studies of gene expression in pluripotent cells can be significantly influenced by the gene-targeting strategy and genetic background employed. 2013",

author = "Faddah, \{Dina A.\} and Haoyi Wang and Cheng, \{Albert Wu\} and Yarden Katz and Yosef Buganim and Rudolf Jaenisch",

note = "Funding Information: We thank A. Smith for sharing TNGA cells; B. Carey, M. Dawlaty, F. Soldner, and A. Salama for helpful discussions; T. Theunissen for help with sorting; and A. van Oudenaarden and S. Klemm for insightful discussions and Stella probe. D.A.F. is a Vertex scholar and was supported by a National Science Foundation Graduate Research Fellowship and a Jerome and Florence Brill Graduate Student Fellowship. A.W.C. was supported by a Croucher and Ludwig Research Fellowship. Y.B. was supported by a National Institutes of Health (NIH) Kirschstein National Research Service Award (1 F32 GM099153-01A1). This work was supported by NIH grants HD 045022 and R37CA084198 to R.J. R.J. is a cofounder of Fate Therapeutics and an advisor to Stemgent.",

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AU - Faddah, Dina A.

AU - Wang, Haoyi

AU - Cheng, Albert Wu

AU - Katz, Yarden

AU - Buganim, Yosef

AU - Jaenisch, Rudolf

N1 - Funding Information: We thank A. Smith for sharing TNGA cells; B. Carey, M. Dawlaty, F. Soldner, and A. Salama for helpful discussions; T. Theunissen for help with sorting; and A. van Oudenaarden and S. Klemm for insightful discussions and Stella probe. D.A.F. is a Vertex scholar and was supported by a National Science Foundation Graduate Research Fellowship and a Jerome and Florence Brill Graduate Student Fellowship. A.W.C. was supported by a Croucher and Ludwig Research Fellowship. Y.B. was supported by a National Institutes of Health (NIH) Kirschstein National Research Service Award (1 F32 GM099153-01A1). This work was supported by NIH grants HD 045022 and R37CA084198 to R.J. R.J. is a cofounder of Fate Therapeutics and an advisor to Stemgent.

PY - 2013/7/3

Y1 - 2013/7/3

N2 - The homeodomain transcription factor Nanog is a central part of the core pluripotency transcriptional network and plays a critical role in embryonic stem cell (ESC) self-renewal. Several reports have suggested that Nanog expression is allelically regulated and that transient downregulation of Nanog in a subset of pluripotent cells predisposes them toward differentiation. Using single-cell gene expression analyses combined with different reporters for the two alleles of Nanog, we show that Nanog is biallelically expressed in ESCs independently of culture condition. We also show that the overall variation in endogenous Nanog expression inESCs is very similar to that of several other pluripotency markers. Our analysis suggests that reporter-based studies of gene expression in pluripotent cells can be significantly influenced by the gene-targeting strategy and genetic background employed. 2013

AB - The homeodomain transcription factor Nanog is a central part of the core pluripotency transcriptional network and plays a critical role in embryonic stem cell (ESC) self-renewal. Several reports have suggested that Nanog expression is allelically regulated and that transient downregulation of Nanog in a subset of pluripotent cells predisposes them toward differentiation. Using single-cell gene expression analyses combined with different reporters for the two alleles of Nanog, we show that Nanog is biallelically expressed in ESCs independently of culture condition. We also show that the overall variation in endogenous Nanog expression inESCs is very similar to that of several other pluripotency markers. Our analysis suggests that reporter-based studies of gene expression in pluripotent cells can be significantly influenced by the gene-targeting strategy and genetic background employed. 2013

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Single-cell analysis reveals that expression of nanog is biallelic and equally variable as that of other pluripotency factors in mouse escs

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