Plasticity of the inner cell mass in mouse blastocyst is restricted by the activity of FGF/MAPK pathway

M.  Wigger; K, Kisielewska; Katarzyna Teresa Filimonow; Berenika Plusa; M. Maleszewski; Aneta Suwinska

doi:10.1038/s41598-017-15427-0

Plasticity of the inner cell mass in mouse blastocyst is restricted by the activity of FGF/MAPK pathway

M. Wigger, K, Kisielewska, Katarzyna Teresa Filimonow, Berenika Plusa, M. Maleszewski, Aneta Suwinska

Division of Developmental Biology & Medicine (L5)

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

Abstract

In order to ensure successful development, cells of the early mammalian embryo must differentiate to either trophectoderm (TE) or inner cell mass (ICM), followed by epiblast (EPI) or primitive endoderm (PE) specification within the ICM. Here, we deciphered the mechanism that assures the correct order of these sequential cell fate decisions. We revealed that TE-deprived ICMs derived from 32-cell blastocysts are still able to reconstruct TE during in vitro culture, confirming totipotency of ICM cells at this stage. ICMs isolated from more advanced blastocysts no longer retain totipotency, failing to form TE and generating PE on their surface. We demonstrated that the transition from full potency to lineage priming is prevented by inhibition of the FGF/MAPK signalling pathway. Moreover, we found that after this first restriction step, ICM cells still retain fate flexibility, manifested by ability to convert their fate into an alternative lineage (PE towards EPI and vice versa), until peri-implantation stage

Original language	English
Journal	Scientific Reports
Early online date	9 Nov 2017
DOIs	https://doi.org/10.1038/s41598-017-15427-0
Publication status	Published - 2017

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title = "Plasticity of the inner cell mass in mouse blastocyst is restricted by the activity of FGF/MAPK pathway",

abstract = "In order to ensure successful development, cells of the early mammalian embryo must differentiate to either trophectoderm (TE) or inner cell mass (ICM), followed by epiblast (EPI) or primitive endoderm (PE) specification within the ICM. Here, we deciphered the mechanism that assures the correct order of these sequential cell fate decisions. We revealed that TE-deprived ICMs derived from 32-cell blastocysts are still able to reconstruct TE during in vitro culture, confirming totipotency of ICM cells at this stage. ICMs isolated from more advanced blastocysts no longer retain totipotency, failing to form TE and generating PE on their surface. We demonstrated that the transition from full potency to lineage priming is prevented by inhibition of the FGF/MAPK signalling pathway. Moreover, we found that after this first restriction step, ICM cells still retain fate flexibility, manifested by ability to convert their fate into an alternative lineage (PE towards EPI and vice versa), until peri-implantation stage",

author = "M. Wigger and K, Kisielewska and Filimonow, {Katarzyna Teresa} and Berenika Plusa and M. Maleszewski and Aneta Suwinska",

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doi = "10.1038/s41598-017-15427-0",

language = "English",

journal = "Scientific Reports",

issn = "2045-2322",

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TY - JOUR

T1 - Plasticity of the inner cell mass in mouse blastocyst is restricted by the activity of FGF/MAPK pathway

AU - Wigger, M.

AU - Kisielewska, K,

AU - Filimonow, Katarzyna Teresa

AU - Plusa, Berenika

AU - Maleszewski, M.

AU - Suwinska, Aneta

PY - 2017

Y1 - 2017

N2 - In order to ensure successful development, cells of the early mammalian embryo must differentiate to either trophectoderm (TE) or inner cell mass (ICM), followed by epiblast (EPI) or primitive endoderm (PE) specification within the ICM. Here, we deciphered the mechanism that assures the correct order of these sequential cell fate decisions. We revealed that TE-deprived ICMs derived from 32-cell blastocysts are still able to reconstruct TE during in vitro culture, confirming totipotency of ICM cells at this stage. ICMs isolated from more advanced blastocysts no longer retain totipotency, failing to form TE and generating PE on their surface. We demonstrated that the transition from full potency to lineage priming is prevented by inhibition of the FGF/MAPK signalling pathway. Moreover, we found that after this first restriction step, ICM cells still retain fate flexibility, manifested by ability to convert their fate into an alternative lineage (PE towards EPI and vice versa), until peri-implantation stage

AB - In order to ensure successful development, cells of the early mammalian embryo must differentiate to either trophectoderm (TE) or inner cell mass (ICM), followed by epiblast (EPI) or primitive endoderm (PE) specification within the ICM. Here, we deciphered the mechanism that assures the correct order of these sequential cell fate decisions. We revealed that TE-deprived ICMs derived from 32-cell blastocysts are still able to reconstruct TE during in vitro culture, confirming totipotency of ICM cells at this stage. ICMs isolated from more advanced blastocysts no longer retain totipotency, failing to form TE and generating PE on their surface. We demonstrated that the transition from full potency to lineage priming is prevented by inhibition of the FGF/MAPK signalling pathway. Moreover, we found that after this first restriction step, ICM cells still retain fate flexibility, manifested by ability to convert their fate into an alternative lineage (PE towards EPI and vice versa), until peri-implantation stage

U2 - 10.1038/s41598-017-15427-0

DO - 10.1038/s41598-017-15427-0

M3 - Article

SN - 2045-2322

JO - Scientific Reports

JF - Scientific Reports

ER -

Plasticity of the inner cell mass in mouse blastocyst is restricted by the activity of FGF/MAPK pathway

Abstract

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