Genome editing reveals a role for OCT4 in human embryogenesis

Norah M.E. Fogarty; Afshan McCarthy; Kirsten E. Snijders; Benjamin E. Powell; Nada Kubikova; Paul Blakeley; Rebecca Lea; Kay Elder; Sissy E. Wamaitha; Daesik Kim; Valdone Maciulyte; Jens Kleinjung; Jin Soo Kim; Dagan Wells; Ludovic Vallier; Alessandro Bertero; James M.A. Turner; Kathy K. Niakan

doi:10.1038/nature24033

Genome editing reveals a role for OCT4 in human embryogenesis

Norah M.E. Fogarty
, Afshan McCarthy
, Kirsten E. Snijders
, Benjamin E. Powell
, Nada Kubikova
, Paul Blakeley
, Rebecca Lea
, Kay Elder
, Sissy E. Wamaitha
, Daesik Kim
, Valdone Maciulyte
, Jens Kleinjung
, Jin Soo Kim
, Dagan Wells
, Ludovic Vallier
, Alessandro Bertero
, James M.A. Turner
, Kathy K. Niakan

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

316 Scopus citations

Abstract

Despite their fundamental biological and clinical importance, the molecular mechanisms that regulate the first cell fate decisions in the human embryo are not well understood. Here we use CRISPR-Cas9-mediated genome editing to investigate the function of the pluripotency transcription factor OCT4 during human embryogenesis. We identified an efficient OCT4-targeting guide RNA using an inducible human embryonic stem cell-based system and microinjection of mouse zygotes. Using these refined methods, we efficiently and specifically targeted the gene encoding OCT4 (POU5F1) in diploid human zygotes and found that blastocyst development was compromised. Transcriptomics analysis revealed that, in POU5F1-null cells, gene expression was downregulated not only for extra-embryonic trophectoderm genes, such as CDX2, but also for regulators of the pluripotent epiblast, including NANOG. By contrast, Pou5f1-null mouse embryos maintained the expression of orthologous genes, and blastocyst development was established, but maintenance was compromised. We conclude that CRISPR-Cas9-mediated genome editing is a powerful method for investigating gene function in the context of human development.

Original language	English
Pages (from-to)	67-73
Number of pages	7
Journal	Nature
Volume	550
Issue number	7674
DOIs	https://doi.org/10.1038/nature24033
State	Published - 5 Oct 2017
Externally published	Yes

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Fogarty, N. M. E., McCarthy, A., Snijders, K. E., Powell, B. E., Kubikova, N., Blakeley, P., Lea, R., Elder, K., Wamaitha, S. E., Kim, D., Maciulyte, V., Kleinjung, J., Kim, J. S., Wells, D., Vallier, L., Bertero, A., Turner, J. M. A., & Niakan, K. K. (2017). Genome editing reveals a role for OCT4 in human embryogenesis. Nature, 550(7674), 67-73. https://doi.org/10.1038/nature24033

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title = "Genome editing reveals a role for OCT4 in human embryogenesis",

abstract = "Despite their fundamental biological and clinical importance, the molecular mechanisms that regulate the first cell fate decisions in the human embryo are not well understood. Here we use CRISPR-Cas9-mediated genome editing to investigate the function of the pluripotency transcription factor OCT4 during human embryogenesis. We identified an efficient OCT4-targeting guide RNA using an inducible human embryonic stem cell-based system and microinjection of mouse zygotes. Using these refined methods, we efficiently and specifically targeted the gene encoding OCT4 (POU5F1) in diploid human zygotes and found that blastocyst development was compromised. Transcriptomics analysis revealed that, in POU5F1-null cells, gene expression was downregulated not only for extra-embryonic trophectoderm genes, such as CDX2, but also for regulators of the pluripotent epiblast, including NANOG. By contrast, Pou5f1-null mouse embryos maintained the expression of orthologous genes, and blastocyst development was established, but maintenance was compromised. We conclude that CRISPR-Cas9-mediated genome editing is a powerful method for investigating gene function in the context of human development.",

author = "Fogarty, \{Norah M.E.\} and Afshan McCarthy and Snijders, \{Kirsten E.\} and Powell, \{Benjamin E.\} and Nada Kubikova and Paul Blakeley and Rebecca Lea and Kay Elder and Wamaitha, \{Sissy E.\} and Daesik Kim and Valdone Maciulyte and Jens Kleinjung and Kim, \{Jin Soo\} and Dagan Wells and Ludovic Vallier and Alessandro Bertero and Turner, \{James M.A.\} and Niakan, \{Kathy K.\}",

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AU - Fogarty, Norah M.E.

AU - McCarthy, Afshan

AU - Snijders, Kirsten E.

AU - Powell, Benjamin E.

AU - Kubikova, Nada

AU - Blakeley, Paul

AU - Lea, Rebecca

AU - Elder, Kay

AU - Wamaitha, Sissy E.

AU - Kim, Daesik

AU - Maciulyte, Valdone

AU - Kleinjung, Jens

AU - Kim, Jin Soo

AU - Wells, Dagan

AU - Vallier, Ludovic

AU - Bertero, Alessandro

AU - Turner, James M.A.

AU - Niakan, Kathy K.

PY - 2017/10/5

Y1 - 2017/10/5

N2 - Despite their fundamental biological and clinical importance, the molecular mechanisms that regulate the first cell fate decisions in the human embryo are not well understood. Here we use CRISPR-Cas9-mediated genome editing to investigate the function of the pluripotency transcription factor OCT4 during human embryogenesis. We identified an efficient OCT4-targeting guide RNA using an inducible human embryonic stem cell-based system and microinjection of mouse zygotes. Using these refined methods, we efficiently and specifically targeted the gene encoding OCT4 (POU5F1) in diploid human zygotes and found that blastocyst development was compromised. Transcriptomics analysis revealed that, in POU5F1-null cells, gene expression was downregulated not only for extra-embryonic trophectoderm genes, such as CDX2, but also for regulators of the pluripotent epiblast, including NANOG. By contrast, Pou5f1-null mouse embryos maintained the expression of orthologous genes, and blastocyst development was established, but maintenance was compromised. We conclude that CRISPR-Cas9-mediated genome editing is a powerful method for investigating gene function in the context of human development.

AB - Despite their fundamental biological and clinical importance, the molecular mechanisms that regulate the first cell fate decisions in the human embryo are not well understood. Here we use CRISPR-Cas9-mediated genome editing to investigate the function of the pluripotency transcription factor OCT4 during human embryogenesis. We identified an efficient OCT4-targeting guide RNA using an inducible human embryonic stem cell-based system and microinjection of mouse zygotes. Using these refined methods, we efficiently and specifically targeted the gene encoding OCT4 (POU5F1) in diploid human zygotes and found that blastocyst development was compromised. Transcriptomics analysis revealed that, in POU5F1-null cells, gene expression was downregulated not only for extra-embryonic trophectoderm genes, such as CDX2, but also for regulators of the pluripotent epiblast, including NANOG. By contrast, Pou5f1-null mouse embryos maintained the expression of orthologous genes, and blastocyst development was established, but maintenance was compromised. We conclude that CRISPR-Cas9-mediated genome editing is a powerful method for investigating gene function in the context of human development.

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DO - 10.1038/nature24033

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Genome editing reveals a role for OCT4 in human embryogenesis

Abstract

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