ICM-autonomous regulation of mouse blastocyst primitive endoderm formation by p38-MAPK is independent of cavity expansion

Bohuslavová Née Stiborová, Martina; Hauserová, Andrea; Collier, Rebecca; Lilao Garzón,Joaquín; Muñoz Descalzo, Silvia; Bruce, Alexander W

Identificador persistente para citar o vincular este elemento: https://accedacris.ulpgc.es/jspui/handle/10553/160273

Campo DC	Valor	idioma
dc.contributor.author	Bohuslavová Née Stiborová, Martina	-
dc.contributor.author	Hauserová, Andrea	-
dc.contributor.author	Collier, Rebecca	-
dc.contributor.author	Lilao Garzón,Joaquín	-
dc.contributor.author	Muñoz Descalzo, Silvia	-
dc.contributor.author	Bruce, Alexander W	-
dc.date.accessioned	2026-03-10T09:42:13Z	-
dc.date.available	2026-03-10T09:42:13Z	-
dc.date.issued	2026	-
dc.identifier.issn	1470-1626	-
dc.identifier.other	WoS	-
dc.identifier.uri	https://accedacris.ulpgc.es/jspui/handle/10553/160273	-
dc.description.abstract	During early mouse blastocyst ICM maturation, we previously described that pharmacological inhibition of p38-MAPK (p38-MAPKi) significantly impairs primitive endoderm (PrE) differentiation from an initially uncommitted population of ICM cells but does not affect pluripotent epiblast (EPI) specification. A recent report details a positive role for blastocyst cavity expansion in assisting ICM lineage formation and marker gene expression. As p38-MAPKi also results in smaller cavity volumes, we addressed to what extent p38-MAPKi mediated impaired PrE differentiation is driven by ICM autonomous or cavity expansion mechanisms. We compared ICM differentiation phenotypes associated with either chemically inhibited cavity volume expansion and p38-MAPKi, on the individual cell and ICM lineage population levels. Whilst recapitulating previously observed decreases in expression of both EPI and PrE markers, we discovered cavity expansion phenotypes are manifest in impaired numbers of specified EPI and increased numbers of uncommitted cells; rather than impaired PrE differentiation, as observed after p38-MAPKi. Moreover, using both 2D ES-cell and 3D ICM organoid models, we show PrE differentiation is also significantly impaired by p38-MAPKi in the absence of a blastocyst cavity; a result recapitulated in cultured immuno-surgically isolated early blastocyst ICMs, in which an outer PrE and inner EPI population are ordinarily formed. These data confirm the early blastocyst requirement for p38-MAPK activity to permit PrE differentiation from uncommitted ICM progenitors is primarily ICM autonomous rather than caused by impaired cavity expansion.	-
dc.language	eng	-
dc.relation	‘‘Viera y Clavijo’’ Program 2016	-
dc.relation	Estudio de la calidad de los embriones preimplantacionales de hembras de edad avanzada en un modelo murino. ACIISI (ULPGC2018-14/CEI2019-02)	-
dc.relation	ProID2020010013	-
dc.relation.ispartof	Reproduction	-
dc.source	Reproduction[ISSN 1470-1626],v. 171 (3), (Marzo 2026)	-
dc.subject	32 Ciencias médicas	-
dc.subject	2407 Biología celular	-
dc.subject.other	Ouabain	-
dc.subject.other	ATP1	-
dc.subject.other	Blastocyst cavity expansion	-
dc.subject.other	SB220025	-
dc.subject.other	p38-MAPK	-
dc.subject.other	ICM cell-fate	-
dc.subject.other	Epiblast	-
dc.subject.other	Primitive endoderm	-
dc.subject.other	Mouse ES-cell and ICM organoids	-
dc.title	ICM-autonomous regulation of mouse blastocyst primitive endoderm formation by p38-MAPK is independent of cavity expansion	-
dc.type	Article	-
dc.identifier.doi	10.1093/reprod/xaag023	-
dc.identifier.isi	001721882600001	-
dc.identifier.eissn	1741-7899	-
dc.identifier.issue	3	-
dc.relation.volume	171	-
dc.investigacion	Ciencias de la Salud	-
dc.type2	Artículo	-
dc.contributor.daisngid	No ID	-
dc.contributor.daisngid	No ID	-
dc.contributor.daisngid	No ID	-
dc.contributor.daisngid	No ID	-
dc.contributor.daisngid	No ID	-
dc.contributor.daisngid	No ID	-
dc.description.numberofpages	17	-
dc.utils.revision	Sí	-
dc.contributor.wosstandard	WOS:Bohuslavová, M	-
dc.contributor.wosstandard	WOS:Hauserová, A	-
dc.contributor.wosstandard	WOS:Collier, R	-
dc.contributor.wosstandard	WOS:Lilao-Garzón, J	-
dc.contributor.wosstandard	WOS:Muñoz-Descalzo, S	-
dc.contributor.wosstandard	WOS:Bruce, AW	-
dc.date.coverdate	Febrero 2026	-
dc.identifier.ulpgc	Sí	-
dc.contributor.buulpgc	BU-MED	-
dc.description.sjr	1,096	-
dc.description.jcr	3,7	-
dc.description.sjrq	Q1	-
dc.description.jcrq	Q1	-
dc.description.scie	SCIE	-
dc.description.miaricds	10,8	-
item.fulltext	Sin texto completo	-
item.grantfulltext	none	-
crisitem.author.dept	GIR IUIBS: Diabetes y endocrinología aplicada	-
crisitem.author.dept	IU de Investigaciones Biomédicas y Sanitarias	-
crisitem.author.dept	GIR IUIBS: Diabetes y endocrinología aplicada	-
crisitem.author.dept	IU de Investigaciones Biomédicas y Sanitarias	-
crisitem.author.dept	Departamento de Morfología	-
crisitem.author.orcid	0000-0002-9971-2459	-
crisitem.author.orcid	0000-0003-0939-7721	-
crisitem.author.parentorg	IU de Investigaciones Biomédicas y Sanitarias	-
crisitem.author.parentorg	IU de Investigaciones Biomédicas y Sanitarias	-
crisitem.author.fullName	Lilao Garzón,Joaquín	-
crisitem.author.fullName	Muñoz Descalzo, Silvia	-
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