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Functional genomic screening in human pluripotent stem cells reveals new roadblocks in early pancreatic endoderm formation

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peer-reviewed

Erstveröffentlichung
2022-02-08
Authors
Krüger, Jana
Breunig, Markus
Pasquini, Lino Pascal
Morawe, Mareen
Groß, Alexander
et al.
Editor
Russ, Holger
Wissenschaftlicher Artikel


Published in
Cells ; 11 (2022), 3. - Art.-Nr. 582. - eISSN 2073-4409
Link to original publication
https://dx.doi.org/10.3390/cells11030582
Faculties
Medizinische Fakultät
Institutions
UKU. Klinik für Innere Medizin I
Institut für Medizinische Systembiologie
External cooperations
Université de Paris
Document version
published version (publisher's PDF)
Abstract
Human pluripotent stem cells, with their ability to proliferate indefinitely and to differentiate into virtually all cell types of the human body, provide a novel resource to study human development and to implement relevant disease models. Here, we employed a human pancreatic differentiation platform complemented with an shRNA screen in human pluripotent stem cells (PSCs) to identify potential drivers of early endoderm and pancreatic development. Deep sequencing followed by abundancy ranking pinpointed six top hit genes potentially associated with either improved or impaired endodermal differentiation, which were selected for functional validation in CRISPR-Cas9 mediated knockout (KO) lines. Upon endoderm differentiation (DE), particularly the loss of SLC22A1 and DSC2 led to impaired differentiation efficiency into CXCR4/KIT-positive DE cells. qPCR analysis also revealed changes in differentiation markers CXCR4, FOXA2, SOX17, and GATA6. Further differentiation of PSCs to the pancreatic progenitor (PP) stage resulted in a decreased proportion of PDX1/NKX6-1-positive cells in SLC22A1 KO lines, and in DSC2 KO lines when differentiated under specific culture conditions. Taken together, our study reveals novel genes with potential roles in early endodermal development.
DFG Project THU
GRK 2254 / HEIST / Heterogenität und Evolution in soliden Tumoren (HEIST) / DFG / 288342734
Monogenetische Formen des juvenil sich manifestierenden Diabetes: neue Schritte in Richtung β-Zellentwicklung, -funktion und -überleben / DFG / 406674944 [KL 2544/5-1]
Zelluläre Plastizität im Pankreas - vom Krankheitsmodell über Gewebserneuerung zur personalisierten Medizin / DFG / 426789149 [KL 2544/6-1]
Project uulm
International PhD Programme in Molecular Medicine / IGradU, Universität Ulm
Publication funding
Open-Access-Förderung durch die Medizinische Fakultät der Universität Ulm
Gefördert durch die Deutsche Forschungsgemeinschaft (DFG) - 491116205
Is supplemented by
https://www.mdpi.com/article/10.3390/cells11030582/s1
Subject headings
[GND]: Krebs <Medizin> | Blutstammzelle | Pluripotente Stammzelle | RNS | Genomik
[MeSH]: Stem cells | Pluripotent stem cells | RNA | Mutation | Organic cation transport proteins | Cardiomyopathies | Genomics
[Free subject headings]: stem cells | pancreatic development | definitive endoderm | shRNA | CATION TRANSPORTER 1 | IN-VITRO | EXPRESSION | DESMOCOLLIN-2 | CARDIOMYOPATHY | CARCINOMA | MOUSE
[DDC subject group]: DDC 570 / Life sciences | DDC 610 / Medicine & health
License
CC BY 4.0 International
https://creativecommons.org/licenses/by/4.0/

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DOI & citation

Please use this identifier to cite or link to this item: http://dx.doi.org/10.18725/OPARU-43260

Krüger, Jana et al. (2022): Functional genomic screening in human pluripotent stem cells reveals new roadblocks in early pancreatic endoderm formation. Open Access Repositorium der Universität Ulm und Technischen Hochschule Ulm. http://dx.doi.org/10.18725/OPARU-43260
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