PSC-derived intestinal organoids with apical-out orientation as a tool to study nutrient uptake, drug absorption and metabolism

P. Kakni; C. Lopez-Iglesias; R. Truckenmuller; P. Habibovic; S. Giselbrecht

doi:10.3389/fmolb.2023.1102209

PSC-derived intestinal organoids with apical-out orientation as a tool to study nutrient uptake, drug absorption and metabolism

P. Kakni, C. Lopez-Iglesias, R. Truckenmuller, P. Habibovic, S. Giselbrecht^*

^*Corresponding author for this work

Research output: Contribution to journal › Article › Academic › peer-review

Abstract

Intestinal organoids recapitulate many features of the in vivo gastrointestinal tract and have revolutionized in vitro studies of intestinal function and disease. However, the restricted accessibility of the apical surface of the organoids facing the central lumen (apical-in) limits studies related to nutrient uptake and drug absorption and metabolism. Here, we demonstrate that pluripotent stem cell (PSC)-derived intestinal organoids with reversed epithelial polarity (apical-out) can successfully recapitulate tissue-specific functions. In particular, these apical-out organoids show strong epithelial barrier formation with all the major junctional complexes, nutrient transport and active lipid metabolism. Furthermore, the organoids express drug-metabolizing enzymes and relevant apical and basolateral transporters. The scalable and robust generation of functional, apical-out intestinal organoids lays the foundation for a completely new range of organoid-based high-throughput/high-content in vitro applications in the fields of nutrition, metabolism and drug discovery.

Original language	English
Article number	1102209
Number of pages	13
Journal	Frontiers in Molecular Biosciences
Volume	10
DOIs	https://doi.org/10.3389/fmolb.2023.1102209
Publication status	Published - 18 Jan 2023

Keywords

intestinal organoids
epithelial polarity
drug discovery
nutrient uptake
barrier integrity
gastrointestinal model
IN-VITRO
EXPRESSION
TRANSPORTERS
INHIBITOR
CULTURE
MODELS
CYP3A4
MRP2

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10.3389/fmolb.2023.1102209Licence: CC BY

Cite this

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title = "PSC-derived intestinal organoids with apical-out orientation as a tool to study nutrient uptake, drug absorption and metabolism",

abstract = "Intestinal organoids recapitulate many features of the in vivo gastrointestinal tract and have revolutionized in vitro studies of intestinal function and disease. However, the restricted accessibility of the apical surface of the organoids facing the central lumen (apical-in) limits studies related to nutrient uptake and drug absorption and metabolism. Here, we demonstrate that pluripotent stem cell (PSC)-derived intestinal organoids with reversed epithelial polarity (apical-out) can successfully recapitulate tissue-specific functions. In particular, these apical-out organoids show strong epithelial barrier formation with all the major junctional complexes, nutrient transport and active lipid metabolism. Furthermore, the organoids express drug-metabolizing enzymes and relevant apical and basolateral transporters. The scalable and robust generation of functional, apical-out intestinal organoids lays the foundation for a completely new range of organoid-based high-throughput/high-content in vitro applications in the fields of nutrition, metabolism and drug discovery.",

keywords = "intestinal organoids, epithelial polarity, drug discovery, nutrient uptake, barrier integrity, gastrointestinal model, IN-VITRO, EXPRESSION, TRANSPORTERS, INHIBITOR, CULTURE, MODELS, CYP3A4, MRP2",

author = "P. Kakni and C. Lopez-Iglesias and R. Truckenmuller and P. Habibovic and S. Giselbrecht",

note = "Funding Information: This study was financially supported by the Dutch Province of Limburg (program “Limburg INvesteert in haar Kenniseconomie/LINK”; SAS-2014–00837 and SAS-2018–02477). The authors gratefully acknowledge the Gravitation Program “Materials Driven Regeneration”, funded by the Netherlands Organization for Scientific Research (024.003.013). Publisher Copyright: Copyright {\textcopyright} 2023 Kakni, L{\'o}pez-Iglesias, Truckenm{\"u}ller, Habibovi{\'c} and Giselbrecht.",

year = "2023",

month = jan,

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doi = "10.3389/fmolb.2023.1102209",

language = "English",

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journal = "Frontiers in Molecular Biosciences",

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TY - JOUR

T1 - PSC-derived intestinal organoids with apical-out orientation as a tool to study nutrient uptake, drug absorption and metabolism

AU - Kakni, P.

AU - Lopez-Iglesias, C.

AU - Truckenmuller, R.

AU - Habibovic, P.

AU - Giselbrecht, S.

N1 - Funding Information: This study was financially supported by the Dutch Province of Limburg (program “Limburg INvesteert in haar Kenniseconomie/LINK”; SAS-2014–00837 and SAS-2018–02477). The authors gratefully acknowledge the Gravitation Program “Materials Driven Regeneration”, funded by the Netherlands Organization for Scientific Research (024.003.013). Publisher Copyright: Copyright © 2023 Kakni, López-Iglesias, Truckenmüller, Habibović and Giselbrecht.

PY - 2023/1/18

Y1 - 2023/1/18

N2 - Intestinal organoids recapitulate many features of the in vivo gastrointestinal tract and have revolutionized in vitro studies of intestinal function and disease. However, the restricted accessibility of the apical surface of the organoids facing the central lumen (apical-in) limits studies related to nutrient uptake and drug absorption and metabolism. Here, we demonstrate that pluripotent stem cell (PSC)-derived intestinal organoids with reversed epithelial polarity (apical-out) can successfully recapitulate tissue-specific functions. In particular, these apical-out organoids show strong epithelial barrier formation with all the major junctional complexes, nutrient transport and active lipid metabolism. Furthermore, the organoids express drug-metabolizing enzymes and relevant apical and basolateral transporters. The scalable and robust generation of functional, apical-out intestinal organoids lays the foundation for a completely new range of organoid-based high-throughput/high-content in vitro applications in the fields of nutrition, metabolism and drug discovery.

AB - Intestinal organoids recapitulate many features of the in vivo gastrointestinal tract and have revolutionized in vitro studies of intestinal function and disease. However, the restricted accessibility of the apical surface of the organoids facing the central lumen (apical-in) limits studies related to nutrient uptake and drug absorption and metabolism. Here, we demonstrate that pluripotent stem cell (PSC)-derived intestinal organoids with reversed epithelial polarity (apical-out) can successfully recapitulate tissue-specific functions. In particular, these apical-out organoids show strong epithelial barrier formation with all the major junctional complexes, nutrient transport and active lipid metabolism. Furthermore, the organoids express drug-metabolizing enzymes and relevant apical and basolateral transporters. The scalable and robust generation of functional, apical-out intestinal organoids lays the foundation for a completely new range of organoid-based high-throughput/high-content in vitro applications in the fields of nutrition, metabolism and drug discovery.

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KW - nutrient uptake

KW - barrier integrity

KW - gastrointestinal model

KW - IN-VITRO

KW - EXPRESSION

KW - TRANSPORTERS

KW - INHIBITOR

KW - CULTURE

KW - MODELS

KW - CYP3A4

KW - MRP2

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