Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold
Generation of human organoids from induced pluripotent stem cells (iPSCs) offers exciting possibilities for developmental biology, disease modelling and cell therapy. Significant advances towards those goals have been hampered by dependence on animal derived matrices (e.g. Matrigel), immortalized ce...
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sg-ntu-dr.10356-898342023-07-14T15:44:42Z Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold Blackford, Samuel J. I. Ng, Soon Seng Saeb-Parsy, Kourosh Segal, Joe M. Serra, Maria Paola Horcas-Lopez, Marta No, Da Yoon Mastoridis, Sotiris Jassem, Wayel Frank, Curtis W. Cho, Nam Joon Nakauchi, Hiromitsu Glenn, Jeffrey S. Rashid, S. Tamir School of Materials Science & Engineering Biomimetic Materials Liver Stem Cells DRNTU::Engineering::Materials::Biomaterials Generation of human organoids from induced pluripotent stem cells (iPSCs) offers exciting possibilities for developmental biology, disease modelling and cell therapy. Significant advances towards those goals have been hampered by dependence on animal derived matrices (e.g. Matrigel), immortalized cell lines and resultant structures that are difficult to control or scale. To address these challenges, we aimed to develop a fully defined liver organoid platform using inverted colloid crystal (ICC) whose 3-dimensional mechanical properties could be engineered to recapitulate the extracellular niche sensed by hepatic progenitors during human development. iPSC derived hepatic progenitors (IH) formed organoids most optimally in ICC scaffolds constructed with 140 μm diameter pores coated with type I collagen in a two-step process mimicking liver bud formation. The resultant organoids were closer to adult tissue, compared to 2D and 3D controls, with respect to morphology, gene expression, protein secretion, drug metabolism and viral infection and could integrate, vascularise and function following implantation into livers of immune-deficient mice. Preliminary interrogation of the underpinning mechanisms highlighted the importance of TGFβ and hedgehog signalling pathways. The combination of functional relevance with tuneable mechanical properties leads us to propose this bioengineered platform to be ideally suited for a range of future mechanistic and clinical organoid related applications. Published version 2018-10-18T07:50:41Z 2019-12-06T17:34:33Z 2018-10-18T07:50:41Z 2019-12-06T17:34:33Z 2018 Journal Article Ng, S. S., Saeb-Parsy, K., Blackford, S. J., Segal, J. M., Serra, M. P., Horcas-Lopez, M., . . . Rashid, S. T. (2018). Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold. Biomaterials, 182, 299-311. doi:10.1016/j.biomaterials.2018.07.043 0142-9612 https://hdl.handle.net/10356/89834 http://hdl.handle.net/10220/46368 10.1016/j.biomaterials.2018.07.043 en Biomaterials © 2018 The Authors. Published by Elsevier Ltd. This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/). 13 p. application/pdf |
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Biomimetic Materials Liver Stem Cells DRNTU::Engineering::Materials::Biomaterials Blackford, Samuel J. I. Ng, Soon Seng Saeb-Parsy, Kourosh Segal, Joe M. Serra, Maria Paola Horcas-Lopez, Marta No, Da Yoon Mastoridis, Sotiris Jassem, Wayel Frank, Curtis W. Cho, Nam Joon Nakauchi, Hiromitsu Glenn, Jeffrey S. Rashid, S. Tamir Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| description |
Generation of human organoids from induced pluripotent stem cells (iPSCs) offers exciting possibilities for developmental biology, disease modelling and cell therapy. Significant advances towards those goals have been hampered by dependence on animal derived matrices (e.g. Matrigel), immortalized cell lines and resultant structures that are difficult to control or scale. To address these challenges, we aimed to develop a fully defined liver organoid platform using inverted colloid crystal (ICC) whose 3-dimensional mechanical properties could be engineered to recapitulate the extracellular niche sensed by hepatic progenitors during human development. iPSC derived hepatic progenitors (IH) formed organoids most optimally in ICC scaffolds constructed with 140 μm diameter pores coated with type I collagen in a two-step process mimicking liver bud formation. The resultant organoids were closer to adult tissue, compared to 2D and 3D controls, with respect to morphology, gene expression, protein secretion, drug metabolism and viral infection and could integrate, vascularise and function following implantation into livers of immune-deficient mice. Preliminary interrogation of the underpinning mechanisms highlighted the importance of TGFβ and hedgehog signalling pathways. The combination of functional relevance with tuneable mechanical properties leads us to propose this bioengineered platform to be ideally suited for a range of future mechanistic and clinical organoid related applications. |
| author2 |
School of Materials Science & Engineering |
| author_facet |
School of Materials Science & Engineering Blackford, Samuel J. I. Ng, Soon Seng Saeb-Parsy, Kourosh Segal, Joe M. Serra, Maria Paola Horcas-Lopez, Marta No, Da Yoon Mastoridis, Sotiris Jassem, Wayel Frank, Curtis W. Cho, Nam Joon Nakauchi, Hiromitsu Glenn, Jeffrey S. Rashid, S. Tamir |
| format |
Article |
| author |
Blackford, Samuel J. I. Ng, Soon Seng Saeb-Parsy, Kourosh Segal, Joe M. Serra, Maria Paola Horcas-Lopez, Marta No, Da Yoon Mastoridis, Sotiris Jassem, Wayel Frank, Curtis W. Cho, Nam Joon Nakauchi, Hiromitsu Glenn, Jeffrey S. Rashid, S. Tamir |
| author_sort |
Blackford, Samuel J. I. |
| title |
Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| title_short |
Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| title_full |
Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| title_fullStr |
Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| title_full_unstemmed |
Human iPS derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| title_sort |
human ips derived progenitors bioengineered into liver organoids using an inverted colloidal crystal poly (ethylene glycol) scaffold |
| publishDate |
2018 |
| url |
https://hdl.handle.net/10356/89834 http://hdl.handle.net/10220/46368 |
| _version_ |
1772827668823146496 |