Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration

Epithelial repair relies on the activation of stress signaling pathways to coordinate tissue repair. Their deregulation is implicated in chronic wound and cancer pathologies. Using TNF-α/Eiger-mediated inflammatory damage to Drosophila imaginal discs, we investigate how spatial patterns of signaling...

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Autores principales: Jaiswal, Janhvi, Egert, Janine, Engesser, Raphael, Peyrotón, Andrea Armengol, Nogay, Liyne, Weichselberger, Vanessa, Crucianelli, Carlo, Grass, Isabelle, Kreutz, Clemens, Timmer, Jens, Classen, Anne-Kathrin
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
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Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10228795/
https://www.ncbi.nlm.nih.gov/pubmed/37252939
http://dx.doi.org/10.1371/journal.pbio.3001665
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author Jaiswal, Janhvi
Egert, Janine
Engesser, Raphael
Peyrotón, Andrea Armengol
Nogay, Liyne
Weichselberger, Vanessa
Crucianelli, Carlo
Grass, Isabelle
Kreutz, Clemens
Timmer, Jens
Classen, Anne-Kathrin
author_facet Jaiswal, Janhvi
Egert, Janine
Engesser, Raphael
Peyrotón, Andrea Armengol
Nogay, Liyne
Weichselberger, Vanessa
Crucianelli, Carlo
Grass, Isabelle
Kreutz, Clemens
Timmer, Jens
Classen, Anne-Kathrin
author_sort Jaiswal, Janhvi
collection PubMed
description Epithelial repair relies on the activation of stress signaling pathways to coordinate tissue repair. Their deregulation is implicated in chronic wound and cancer pathologies. Using TNF-α/Eiger-mediated inflammatory damage to Drosophila imaginal discs, we investigate how spatial patterns of signaling pathways and repair behaviors arise. We find that Eiger expression, which drives JNK/AP-1 signaling, transiently arrests proliferation of cells in the wound center and is associated with activation of a senescence program. This includes production of the mitogenic ligands of the Upd family, which allows JNK/AP-1-signaling cells to act as paracrine organizers of regeneration. Surprisingly, JNK/AP-1 cell-autonomously suppress activation of Upd signaling via Ptp61F and Socs36E, both negative regulators of JAK/STAT signaling. As mitogenic JAK/STAT signaling is suppressed in JNK/AP-1-signaling cells at the center of tissue damage, compensatory proliferation occurs by paracrine activation of JAK/STAT in the wound periphery. Mathematical modelling suggests that cell-autonomous mutual repression between JNK/AP-1 and JAK/STAT is at the core of a regulatory network essential to spatially separate JNK/AP-1 and JAK/STAT signaling into bistable spatial domains associated with distinct cellular tasks. Such spatial stratification is essential for proper tissue repair, as coactivation of JNK/AP-1 and JAK/STAT in the same cells creates conflicting signals for cell cycle progression, leading to excess apoptosis of senescently stalled JNK/AP-1-signaling cells that organize the spatial field. Finally, we demonstrate that bistable separation of JNK/AP-1 and JAK/STAT drives bistable separation of senescent signaling and proliferative behaviors not only upon tissue damage, but also in Ras(V12), scrib tumors. Revealing this previously uncharacterized regulatory network between JNK/AP-1, JAK/STAT, and associated cell behaviors has important implications for our conceptual understanding of tissue repair, chronic wound pathologies, and tumor microenvironments.
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spelling pubmed-102287952023-05-31 Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration Jaiswal, Janhvi Egert, Janine Engesser, Raphael Peyrotón, Andrea Armengol Nogay, Liyne Weichselberger, Vanessa Crucianelli, Carlo Grass, Isabelle Kreutz, Clemens Timmer, Jens Classen, Anne-Kathrin PLoS Biol Research Article Epithelial repair relies on the activation of stress signaling pathways to coordinate tissue repair. Their deregulation is implicated in chronic wound and cancer pathologies. Using TNF-α/Eiger-mediated inflammatory damage to Drosophila imaginal discs, we investigate how spatial patterns of signaling pathways and repair behaviors arise. We find that Eiger expression, which drives JNK/AP-1 signaling, transiently arrests proliferation of cells in the wound center and is associated with activation of a senescence program. This includes production of the mitogenic ligands of the Upd family, which allows JNK/AP-1-signaling cells to act as paracrine organizers of regeneration. Surprisingly, JNK/AP-1 cell-autonomously suppress activation of Upd signaling via Ptp61F and Socs36E, both negative regulators of JAK/STAT signaling. As mitogenic JAK/STAT signaling is suppressed in JNK/AP-1-signaling cells at the center of tissue damage, compensatory proliferation occurs by paracrine activation of JAK/STAT in the wound periphery. Mathematical modelling suggests that cell-autonomous mutual repression between JNK/AP-1 and JAK/STAT is at the core of a regulatory network essential to spatially separate JNK/AP-1 and JAK/STAT signaling into bistable spatial domains associated with distinct cellular tasks. Such spatial stratification is essential for proper tissue repair, as coactivation of JNK/AP-1 and JAK/STAT in the same cells creates conflicting signals for cell cycle progression, leading to excess apoptosis of senescently stalled JNK/AP-1-signaling cells that organize the spatial field. Finally, we demonstrate that bistable separation of JNK/AP-1 and JAK/STAT drives bistable separation of senescent signaling and proliferative behaviors not only upon tissue damage, but also in Ras(V12), scrib tumors. Revealing this previously uncharacterized regulatory network between JNK/AP-1, JAK/STAT, and associated cell behaviors has important implications for our conceptual understanding of tissue repair, chronic wound pathologies, and tumor microenvironments. Public Library of Science 2023-05-30 /pmc/articles/PMC10228795/ /pubmed/37252939 http://dx.doi.org/10.1371/journal.pbio.3001665 Text en © 2023 Jaiswal et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Jaiswal, Janhvi
Egert, Janine
Engesser, Raphael
Peyrotón, Andrea Armengol
Nogay, Liyne
Weichselberger, Vanessa
Crucianelli, Carlo
Grass, Isabelle
Kreutz, Clemens
Timmer, Jens
Classen, Anne-Kathrin
Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title_full Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title_fullStr Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title_full_unstemmed Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title_short Mutual repression between JNK/AP-1 and JAK/STAT stratifies senescent and proliferative cell behaviors during tissue regeneration
title_sort mutual repression between jnk/ap-1 and jak/stat stratifies senescent and proliferative cell behaviors during tissue regeneration
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10228795/
https://www.ncbi.nlm.nih.gov/pubmed/37252939
http://dx.doi.org/10.1371/journal.pbio.3001665
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