HEIDI: Vanova, Tereza: Tyrosine kinase expressed in hepatocellular carcinoma, TEC, controls pluripotency and early cell fate decisions of human pluripotent stem cells via regulation of fibroblast growth factor-2 secretion

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Status: Bibliographieeintrag

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	Online-Ressource
Verfasst von:	Vanova, Tereza [VerfasserIn]
	La Venuta, Giuseppe [VerfasserIn]
	Nickel, Walter [VerfasserIn]
Titel:	Tyrosine kinase expressed in hepatocellular carcinoma, TEC, controls pluripotency and early cell fate decisions of human pluripotent stem cells via regulation of fibroblast growth factor-2 secretion
Verf.angabe:	Tereza Vanova, Zaneta Konecna, Zuzana Zbonakova, Giuseppe La Venuta, Karolina Zoufalova, Sarka Jelinkova, Miroslav Varecha, Vladimir Rotrekl, Pavel Krejci, Walter Nickel, Petr Dvorak, Michaela Kunova Bosakova
Umfang:	10 S.
Fussnoten:	Gesehen am 27.09.2018
Titel Quelle:	Enthalten in: Stem cells
Jahr Quelle:	2017
Band/Heft Quelle:	35(2017), 9, S. 2050-2059
ISSN Quelle:	1549-4918
Abstract:	Human pluripotent stem cells (hPSC) require signaling provided by fibroblast growth factor (FGF) receptors. This can be initiated by the recombinant FGF2 ligand supplied exogenously, but hPSC further support their niche by secretion of endogenous FGF2. In this study, we describe a role of tyrosine kinase expressed in hepatocellular carcinoma (TEC) kinase in this process. We show that TEC-mediated FGF2 secretion is essential for hPSC self-renewal, and its lack mediates specific differentiation. Following both short hairpin RNA- and small interfering RNA-mediated TEC knockdown, hPSC secretes less FGF2. This impairs hPSC proliferation that can be rescued by increasing amounts of recombinant FGF2. TEC downregulation further leads to a lower expression of the pluripotency markers, an improved priming towards neuroectodermal lineage, and a failure to develop cardiac mesoderm. Our data thus demonstrate that TEC is yet another regulator of FGF2-mediated hPSC pluripotency and differentiation. Stem Cells 2017;35:2050-2059
DOI:	doi:10.1002/stem.2660
URL:	Bitte beachten Sie: Dies ist ein Bibliographieeintrag. Ein Volltextzugriff für Mitglieder der Universität besteht hier nur, falls für die entsprechende Zeitschrift/den entsprechenden Sammelband ein Abonnement besteht oder es sich um einen OpenAccess-Titel handelt. Verlag: http://dx.doi.org/10.1002/stem.2660
	Verlag: https://stemcellsjournals.onlinelibrary.wiley.com/doi/abs/10.1002/stem.2660
	DOI: https://doi.org/10.1002/stem.2660
Datenträger:	Online-Ressource
Sprache:	eng
K10plus-PPN:	1581356676
Verknüpfungen:	→ Zeitschrift

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