Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model
With their capability to self-renew and differentiate into derivatives of all three germ layers, human pluripotent stem cells (hPSCs) offer a unique model to study aspects of human development in vitro. Directed differentiation towards mesendodermal lineages is a complex process, involving transition through a primitive streak (PS)-like stage. We have recently shown PS-like patterning from hPSCs into definitive endoderm, cardiac as well as presomitic mesoderm by only modulating the bulk cell density and the concentration of the GSK3 inhibitor CHIR99021, a potent activator of the WNT pathway. The patterning process is modulated by a complex paracrine network, whose identity and mechanistic consequences are poorly understood. To study the underlying dynamics, we here applied mathematical modeling based on ordinary differential equations. We compared time-course data of early hPSC differentiation to increasingly complex model structures with incremental numbers of paracrine factors. Model simulations suggest at least three paracrine factors being required to recapitulate the experimentally observed differentiation kinetics. Feedback mechanisms from both undifferentiated and differentiated cells turned out to be crucial. Evidence from double knock-down experiments and secreted protein enrichment allowed us to hypothesize on the identity of two of the three predicted factors. From a practical perspective, the mathematical model predicts optimal settings for directing lineage-specific differentiation. This opens new avenues for rational stem cell bioprocessing in more advanced culture systems, e.g. in perfusion-fed bioreactors enabling cell therapies.
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| Format: | Article/Letter to editor biblioteca |
| Language: | English |
| Subjects: | Differentiation, Human pluripotent stem cells, Mathematical modeling, Paracrine effects, Primitive streak, |
| Online Access: | https://research.wur.nl/en/publications/paracrine-mechanisms-in-early-differentiation-of-human-pluripoten |
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dig-wur-nl-wurpubs-5408122024-12-04 Gaspari, Erika Franke, Annika Robles-Diaz, Diana Zweigerdt, Robert Roeder, Ingo Zerjatke, Thomas Kempf, Henning Article/Letter to editor Stem Cell Research 32 (2018) ISSN: 1873-5061 Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model 2018 With their capability to self-renew and differentiate into derivatives of all three germ layers, human pluripotent stem cells (hPSCs) offer a unique model to study aspects of human development in vitro. Directed differentiation towards mesendodermal lineages is a complex process, involving transition through a primitive streak (PS)-like stage. We have recently shown PS-like patterning from hPSCs into definitive endoderm, cardiac as well as presomitic mesoderm by only modulating the bulk cell density and the concentration of the GSK3 inhibitor CHIR99021, a potent activator of the WNT pathway. The patterning process is modulated by a complex paracrine network, whose identity and mechanistic consequences are poorly understood. To study the underlying dynamics, we here applied mathematical modeling based on ordinary differential equations. We compared time-course data of early hPSC differentiation to increasingly complex model structures with incremental numbers of paracrine factors. Model simulations suggest at least three paracrine factors being required to recapitulate the experimentally observed differentiation kinetics. Feedback mechanisms from both undifferentiated and differentiated cells turned out to be crucial. Evidence from double knock-down experiments and secreted protein enrichment allowed us to hypothesize on the identity of two of the three predicted factors. From a practical perspective, the mathematical model predicts optimal settings for directing lineage-specific differentiation. This opens new avenues for rational stem cell bioprocessing in more advanced culture systems, e.g. in perfusion-fed bioreactors enabling cell therapies. en application/pdf https://research.wur.nl/en/publications/paracrine-mechanisms-in-early-differentiation-of-human-pluripoten 10.1016/j.scr.2018.07.025 https://edepot.wur.nl/458621 Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak https://creativecommons.org/licenses/by-nc-nd/4.0/ Wageningen University & Research |
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Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak |
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Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak Gaspari, Erika Franke, Annika Robles-Diaz, Diana Zweigerdt, Robert Roeder, Ingo Zerjatke, Thomas Kempf, Henning Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| description |
With their capability to self-renew and differentiate into derivatives of all three germ layers, human pluripotent stem cells (hPSCs) offer a unique model to study aspects of human development in vitro. Directed differentiation towards mesendodermal lineages is a complex process, involving transition through a primitive streak (PS)-like stage. We have recently shown PS-like patterning from hPSCs into definitive endoderm, cardiac as well as presomitic mesoderm by only modulating the bulk cell density and the concentration of the GSK3 inhibitor CHIR99021, a potent activator of the WNT pathway. The patterning process is modulated by a complex paracrine network, whose identity and mechanistic consequences are poorly understood. To study the underlying dynamics, we here applied mathematical modeling based on ordinary differential equations. We compared time-course data of early hPSC differentiation to increasingly complex model structures with incremental numbers of paracrine factors. Model simulations suggest at least three paracrine factors being required to recapitulate the experimentally observed differentiation kinetics. Feedback mechanisms from both undifferentiated and differentiated cells turned out to be crucial. Evidence from double knock-down experiments and secreted protein enrichment allowed us to hypothesize on the identity of two of the three predicted factors. From a practical perspective, the mathematical model predicts optimal settings for directing lineage-specific differentiation. This opens new avenues for rational stem cell bioprocessing in more advanced culture systems, e.g. in perfusion-fed bioreactors enabling cell therapies. |
| format |
Article/Letter to editor |
| topic_facet |
Differentiation Human pluripotent stem cells Mathematical modeling Paracrine effects Primitive streak |
| author |
Gaspari, Erika Franke, Annika Robles-Diaz, Diana Zweigerdt, Robert Roeder, Ingo Zerjatke, Thomas Kempf, Henning |
| author_facet |
Gaspari, Erika Franke, Annika Robles-Diaz, Diana Zweigerdt, Robert Roeder, Ingo Zerjatke, Thomas Kempf, Henning |
| author_sort |
Gaspari, Erika |
| title |
Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| title_short |
Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| title_full |
Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| title_fullStr |
Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| title_full_unstemmed |
Paracrine mechanisms in early differentiation of human pluripotent stem cells : Insights from a mathematical model |
| title_sort |
paracrine mechanisms in early differentiation of human pluripotent stem cells : insights from a mathematical model |
| url |
https://research.wur.nl/en/publications/paracrine-mechanisms-in-early-differentiation-of-human-pluripoten |
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