RNAi and expression of retrotransposons MuERV-L and IAP in preimplantation mouse embryos

Petr Svoboda; Paula Stein; Martin Anger; Emily Bernstein; Gregory J. Hannon; Richard M. Schultz

doi:10.1016/j.ydbio.2004.01.028

RNAi and expression of retrotransposons MuERV-L and IAP in preimplantation mouse embryos

Petr Svoboda, Paula Stein, Martin Anger, Emily Bernstein, Gregory J. Hannon, Richard M. Schultz

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

175 Scopus citations

Abstract

Both murine endogenous retrovirus-L (MuERV-L) and intracisternal A particle (IAP), two autonomous long terminal repeat (LTR) retrotransposons, are activated during genome activation in the preimplantation mouse embryo, and both sense and antisense transcripts are detected in 2-cell and 8-cell stage embryos. Because RNA interference (RNAi) functions in the preimplantation mouse embryo, we analyzed the relationship between RNAi and MuERV-L and IAP expression by inhibiting RNAi and measuring relative changes of the levels of these transcripts. We inhibited the initial step in the RNAi pathway by injecting 1-cell embryos with mDicer siRNA or long mDicer dsRNA and analyzed MuERV-L and IAP expression at the 8-cell stage. This approach resulted in the targeted destruction of mDicer mRNA, but not Hdac1 mRNA, inhibited the RNAi pathway, and resulted in a 50% increase in IAP and MuERV-L transcript abundance. These results suggest that RNAi constrains expression of repetitive parasitic sequences in preimplantation embryos, and thereby contributes to preserving genomic integrity at a stage of development when the organism consists of only a few cells.

Original language	English
Pages (from-to)	276-285
Number of pages	10
Journal	Developmental Biology
Volume	269
Issue number	1
DOIs	https://doi.org/10.1016/j.ydbio.2004.01.028
State	Published - 1 May 2004
Externally published	Yes

Keywords

Dicer
Genome activation
Preimplantation embryo
RNAi
Retrotransposon

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10.1016/j.ydbio.2004.01.028

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title = "RNAi and expression of retrotransposons MuERV-L and IAP in preimplantation mouse embryos",

abstract = "Both murine endogenous retrovirus-L (MuERV-L) and intracisternal A particle (IAP), two autonomous long terminal repeat (LTR) retrotransposons, are activated during genome activation in the preimplantation mouse embryo, and both sense and antisense transcripts are detected in 2-cell and 8-cell stage embryos. Because RNA interference (RNAi) functions in the preimplantation mouse embryo, we analyzed the relationship between RNAi and MuERV-L and IAP expression by inhibiting RNAi and measuring relative changes of the levels of these transcripts. We inhibited the initial step in the RNAi pathway by injecting 1-cell embryos with mDicer siRNA or long mDicer dsRNA and analyzed MuERV-L and IAP expression at the 8-cell stage. This approach resulted in the targeted destruction of mDicer mRNA, but not Hdac1 mRNA, inhibited the RNAi pathway, and resulted in a 50% increase in IAP and MuERV-L transcript abundance. These results suggest that RNAi constrains expression of repetitive parasitic sequences in preimplantation embryos, and thereby contributes to preserving genomic integrity at a stage of development when the organism consists of only a few cells.",

keywords = "Dicer, Genome activation, Preimplantation embryo, RNAi, Retrotransposon",

author = "Petr Svoboda and Paula Stein and Martin Anger and Emily Bernstein and Hannon, {Gregory J.} and Schultz, {Richard M.}",

note = "Funding Information: This research was supported by grants from the NIH (HD 22681 to R.M.S. and GM 62534 to G.J.H.) and by an Innovator award from the U.S. Army Breast Cancer Research Program to G.J.H., who is also a Rita Allen Foundation scholar. P. Svoboda thanks Raymond W. Rose for comments and criticisms, and P. Svoboda and P. Stein thank Zhe Xu for help with the microinjection experiments. Portions of this work were submitted by P. Svoboda in partial fulfillment for the PhD requirements at the University of Pennsylvania.",

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AU - Stein, Paula

AU - Anger, Martin

AU - Bernstein, Emily

AU - Hannon, Gregory J.

AU - Schultz, Richard M.

N1 - Funding Information: This research was supported by grants from the NIH (HD 22681 to R.M.S. and GM 62534 to G.J.H.) and by an Innovator award from the U.S. Army Breast Cancer Research Program to G.J.H., who is also a Rita Allen Foundation scholar. P. Svoboda thanks Raymond W. Rose for comments and criticisms, and P. Svoboda and P. Stein thank Zhe Xu for help with the microinjection experiments. Portions of this work were submitted by P. Svoboda in partial fulfillment for the PhD requirements at the University of Pennsylvania.

PY - 2004/5/1

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N2 - Both murine endogenous retrovirus-L (MuERV-L) and intracisternal A particle (IAP), two autonomous long terminal repeat (LTR) retrotransposons, are activated during genome activation in the preimplantation mouse embryo, and both sense and antisense transcripts are detected in 2-cell and 8-cell stage embryos. Because RNA interference (RNAi) functions in the preimplantation mouse embryo, we analyzed the relationship between RNAi and MuERV-L and IAP expression by inhibiting RNAi and measuring relative changes of the levels of these transcripts. We inhibited the initial step in the RNAi pathway by injecting 1-cell embryos with mDicer siRNA or long mDicer dsRNA and analyzed MuERV-L and IAP expression at the 8-cell stage. This approach resulted in the targeted destruction of mDicer mRNA, but not Hdac1 mRNA, inhibited the RNAi pathway, and resulted in a 50% increase in IAP and MuERV-L transcript abundance. These results suggest that RNAi constrains expression of repetitive parasitic sequences in preimplantation embryos, and thereby contributes to preserving genomic integrity at a stage of development when the organism consists of only a few cells.

AB - Both murine endogenous retrovirus-L (MuERV-L) and intracisternal A particle (IAP), two autonomous long terminal repeat (LTR) retrotransposons, are activated during genome activation in the preimplantation mouse embryo, and both sense and antisense transcripts are detected in 2-cell and 8-cell stage embryos. Because RNA interference (RNAi) functions in the preimplantation mouse embryo, we analyzed the relationship between RNAi and MuERV-L and IAP expression by inhibiting RNAi and measuring relative changes of the levels of these transcripts. We inhibited the initial step in the RNAi pathway by injecting 1-cell embryos with mDicer siRNA or long mDicer dsRNA and analyzed MuERV-L and IAP expression at the 8-cell stage. This approach resulted in the targeted destruction of mDicer mRNA, but not Hdac1 mRNA, inhibited the RNAi pathway, and resulted in a 50% increase in IAP and MuERV-L transcript abundance. These results suggest that RNAi constrains expression of repetitive parasitic sequences in preimplantation embryos, and thereby contributes to preserving genomic integrity at a stage of development when the organism consists of only a few cells.

KW - Dicer

KW - Genome activation

KW - Preimplantation embryo

KW - RNAi

KW - Retrotransposon

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ER -

RNAi and expression of retrotransposons MuERV-L and IAP in preimplantation mouse embryos

Abstract

Keywords

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