Differential Effects of TNF (TNFSF2) and IFN-gamma on Intestinal Epithelial Cell Morphogenesis and Barrier Function in Three-Dimensional Culture

Kati Juuti-Uusitalo; Leon J. Klunder; Klaas A. Sjollema; Katarina Mackovicova; Ryuichi Ohgaki; Dick Hoekstra; Jan Dekker; Sven C. D. van Ijzendoorn

doi:10.1371/journal.pone.0022967

Differential Effects of TNF (TNFSF2) and IFN-gamma on Intestinal Epithelial Cell Morphogenesis and Barrier Function in Three-Dimensional Culture

Kati Juuti-Uusitalo^*, Leon J. Klunder, Klaas A. Sjollema, Katarina Mackovicova, Ryuichi Ohgaki, Dick Hoekstra, Jan Dekker, Sven C. D. van Ijzendoorn

^*Corresponding author for this work

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

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Abstract

Background: The cytokines TNF (TNFSF2) and IFN gamma are important mediators of inflammatory bowel diseases and contribute to enhanced intestinal epithelial permeability by stimulating apoptosis and/or disrupting tight junctions. Apoptosis and tight junctions are also important for epithelial tissue morphogenesis, but the effect of TNF and IFN gamma on the process of intestinal epithelial morphogenesis is unknown.

Methods/Principal Findings: We have employed a three-dimensional cell culture system, reproducing in vivo-like multicellular organization of intestinal epithelial cells, to study the effect of TNF on intestinal epithelial morphogenesis and permeability. We show that human intestinal epithelial cells in three-dimensional culture assembled into luminal spheres consisting of a single layer of cells with structural, internal, and planar cell polarity. Exposure of preformed luminal spheres to TNF or IFN gamma enhanced paracellular permeability, but via distinctive mechanisms. Thus, while both TNF and IFN gamma, albeit in a distinguishable manner, induced the displacement of selected tight junction proteins, only TNF increased paracellular permeability via caspase-driven apoptosis and cell shedding. Infliximab and adalumimab inhibited these effects of TNF. Moreover, we demonstrate that TNF via its stimulatory effect on apoptosis fundamentally alters the process of intestinal epithelial morphogenesis, which contributes to the de novo generation of intestinal epithelial monolayers with increased permeability. Also IFN gamma contributes to the de novo formation of monolayers with increased permeability, but in a manner that does not involve apoptosis.

Conclusions: Our study provides an optimized 3D model system for the integrated analysis of (real-time) intestinal epithelial paracellular permeability and morphogenesis, and reveals apoptosis as a pivotal mechanism underlying the enhanced permeability and altered morphogenesis in response to TNF, but not IFN gamma.

Original language	English
Article number	22967
Number of pages	12
Journal	PLoS ONE
Volume	6
Issue number	8
DOIs	https://doi.org/10.1371/journal.pone.0022967
Publication status	Published - 11-Aug-2011

Keywords

INFLAMMATORY-BOWEL-DISEASE
SPINDLE ORIENTATION
TIGHT JUNCTIONS
LUMEN FORMATION
APICAL SURFACE
MYOSIN-II
POLARITY
MECHANISMS
ALPHA
APOPTOSIS

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@article{1ea704365e734128a4fd124936d5c3bc,

title = "Differential Effects of TNF (TNFSF2) and IFN-gamma on Intestinal Epithelial Cell Morphogenesis and Barrier Function in Three-Dimensional Culture",

abstract = "Background: The cytokines TNF (TNFSF2) and IFN gamma are important mediators of inflammatory bowel diseases and contribute to enhanced intestinal epithelial permeability by stimulating apoptosis and/or disrupting tight junctions. Apoptosis and tight junctions are also important for epithelial tissue morphogenesis, but the effect of TNF and IFN gamma on the process of intestinal epithelial morphogenesis is unknown.Methods/Principal Findings: We have employed a three-dimensional cell culture system, reproducing in vivo-like multicellular organization of intestinal epithelial cells, to study the effect of TNF on intestinal epithelial morphogenesis and permeability. We show that human intestinal epithelial cells in three-dimensional culture assembled into luminal spheres consisting of a single layer of cells with structural, internal, and planar cell polarity. Exposure of preformed luminal spheres to TNF or IFN gamma enhanced paracellular permeability, but via distinctive mechanisms. Thus, while both TNF and IFN gamma, albeit in a distinguishable manner, induced the displacement of selected tight junction proteins, only TNF increased paracellular permeability via caspase-driven apoptosis and cell shedding. Infliximab and adalumimab inhibited these effects of TNF. Moreover, we demonstrate that TNF via its stimulatory effect on apoptosis fundamentally alters the process of intestinal epithelial morphogenesis, which contributes to the de novo generation of intestinal epithelial monolayers with increased permeability. Also IFN gamma contributes to the de novo formation of monolayers with increased permeability, but in a manner that does not involve apoptosis.Conclusions: Our study provides an optimized 3D model system for the integrated analysis of (real-time) intestinal epithelial paracellular permeability and morphogenesis, and reveals apoptosis as a pivotal mechanism underlying the enhanced permeability and altered morphogenesis in response to TNF, but not IFN gamma.",

keywords = "INFLAMMATORY-BOWEL-DISEASE, SPINDLE ORIENTATION, TIGHT JUNCTIONS, LUMEN FORMATION, APICAL SURFACE, MYOSIN-II, POLARITY, MECHANISMS, ALPHA, APOPTOSIS",

author = "Kati Juuti-Uusitalo and Klunder, {Leon J.} and Sjollema, {Klaas A.} and Katarina Mackovicova and Ryuichi Ohgaki and Dick Hoekstra and Jan Dekker and {van Ijzendoorn}, {Sven C. D.}",

year = "2011",

month = aug,

day = "11",

doi = "10.1371/journal.pone.0022967",

language = "English",

volume = "6",

journal = "PLoS ONE",

issn = "1932-6203",

publisher = "PUBLIC LIBRARY SCIENCE",

number = "8",

}

TY - JOUR

T1 - Differential Effects of TNF (TNFSF2) and IFN-gamma on Intestinal Epithelial Cell Morphogenesis and Barrier Function in Three-Dimensional Culture

AU - Juuti-Uusitalo, Kati

AU - Klunder, Leon J.

AU - Sjollema, Klaas A.

AU - Mackovicova, Katarina

AU - Ohgaki, Ryuichi

AU - Hoekstra, Dick

AU - Dekker, Jan

AU - van Ijzendoorn, Sven C. D.

PY - 2011/8/11

Y1 - 2011/8/11

N2 - Background: The cytokines TNF (TNFSF2) and IFN gamma are important mediators of inflammatory bowel diseases and contribute to enhanced intestinal epithelial permeability by stimulating apoptosis and/or disrupting tight junctions. Apoptosis and tight junctions are also important for epithelial tissue morphogenesis, but the effect of TNF and IFN gamma on the process of intestinal epithelial morphogenesis is unknown.Methods/Principal Findings: We have employed a three-dimensional cell culture system, reproducing in vivo-like multicellular organization of intestinal epithelial cells, to study the effect of TNF on intestinal epithelial morphogenesis and permeability. We show that human intestinal epithelial cells in three-dimensional culture assembled into luminal spheres consisting of a single layer of cells with structural, internal, and planar cell polarity. Exposure of preformed luminal spheres to TNF or IFN gamma enhanced paracellular permeability, but via distinctive mechanisms. Thus, while both TNF and IFN gamma, albeit in a distinguishable manner, induced the displacement of selected tight junction proteins, only TNF increased paracellular permeability via caspase-driven apoptosis and cell shedding. Infliximab and adalumimab inhibited these effects of TNF. Moreover, we demonstrate that TNF via its stimulatory effect on apoptosis fundamentally alters the process of intestinal epithelial morphogenesis, which contributes to the de novo generation of intestinal epithelial monolayers with increased permeability. Also IFN gamma contributes to the de novo formation of monolayers with increased permeability, but in a manner that does not involve apoptosis.Conclusions: Our study provides an optimized 3D model system for the integrated analysis of (real-time) intestinal epithelial paracellular permeability and morphogenesis, and reveals apoptosis as a pivotal mechanism underlying the enhanced permeability and altered morphogenesis in response to TNF, but not IFN gamma.

AB - Background: The cytokines TNF (TNFSF2) and IFN gamma are important mediators of inflammatory bowel diseases and contribute to enhanced intestinal epithelial permeability by stimulating apoptosis and/or disrupting tight junctions. Apoptosis and tight junctions are also important for epithelial tissue morphogenesis, but the effect of TNF and IFN gamma on the process of intestinal epithelial morphogenesis is unknown.Methods/Principal Findings: We have employed a three-dimensional cell culture system, reproducing in vivo-like multicellular organization of intestinal epithelial cells, to study the effect of TNF on intestinal epithelial morphogenesis and permeability. We show that human intestinal epithelial cells in three-dimensional culture assembled into luminal spheres consisting of a single layer of cells with structural, internal, and planar cell polarity. Exposure of preformed luminal spheres to TNF or IFN gamma enhanced paracellular permeability, but via distinctive mechanisms. Thus, while both TNF and IFN gamma, albeit in a distinguishable manner, induced the displacement of selected tight junction proteins, only TNF increased paracellular permeability via caspase-driven apoptosis and cell shedding. Infliximab and adalumimab inhibited these effects of TNF. Moreover, we demonstrate that TNF via its stimulatory effect on apoptosis fundamentally alters the process of intestinal epithelial morphogenesis, which contributes to the de novo generation of intestinal epithelial monolayers with increased permeability. Also IFN gamma contributes to the de novo formation of monolayers with increased permeability, but in a manner that does not involve apoptosis.Conclusions: Our study provides an optimized 3D model system for the integrated analysis of (real-time) intestinal epithelial paracellular permeability and morphogenesis, and reveals apoptosis as a pivotal mechanism underlying the enhanced permeability and altered morphogenesis in response to TNF, but not IFN gamma.

KW - INFLAMMATORY-BOWEL-DISEASE

KW - SPINDLE ORIENTATION

KW - TIGHT JUNCTIONS

KW - LUMEN FORMATION

KW - APICAL SURFACE

KW - MYOSIN-II

KW - POLARITY

KW - MECHANISMS

KW - ALPHA

KW - APOPTOSIS

U2 - 10.1371/journal.pone.0022967

DO - 10.1371/journal.pone.0022967

M3 - Article

SN - 1932-6203

VL - 6

JO - PLoS ONE

JF - PLoS ONE

IS - 8

M1 - 22967

ER -

Differential Effects of TNF (TNFSF2) and IFN-gamma on Intestinal Epithelial Cell Morphogenesis and Barrier Function in Three-Dimensional Culture

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