Publication:
A micropatterned human-specific neuroepithelial tissue for modeling gene and drug-induced neurodevelopmental defects

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SCHOOL OF MEDICINE
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Sahni, Geetika
Chang, Shu-Yung
Meng, Jeremy Teo Choon
Tan, Jerome Zu Yao
Fatien, Jean Jacques Clement
Bonnard, Carine
Utami, Kagistia Hana
Chan, Puck Wee
Tan, Thong Teck
Altunoglu, Umut

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Abstract

The generation of structurally standardized human pluripotent stem cell (hPSC)-derived neural embryonic tissues has the potential to model genetic and environmental mediators of early neurodevelopmental defects. Current neural patterning systems have so far focused on directing cell fate specification spatio-temporally but not morphogenetic processes. Here, the formation of a structurally reproducible and highly-organized neuroepithelium (NE) tissue is directed from hPSCs, which recapitulates morphogenetic cellular processes relevant to early neurulation. These include having a continuous, polarized epithelium and a distinct invagination-like folding, where primitive ectodermal cells undergo E-to-N-cadherin switching and apical constriction as they acquire a NE fate. This is accomplished by spatio-temporal patterning of the mesoendoderm, which guides the development and self-organization of the adjacent primitive ectoderm into the NE. It is uncovered that TGF beta signaling emanating from endodermal cells support tissue folding of the prospective NE. Evaluation of NE tissue structural dysmorphia, which is uniquely achievable in the model, enables the detection of apical constriction and cell adhesion dysfunctions in patient-derived hPSCs as well as differentiating between different classes of neural tube defect-inducing drugs.

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Wiley

Subject

Chemistry, Nanoscience and nanotechnology, Materials science

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Source

Advanced Science

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DOI

10.1002/advs.202001100

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