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Epithelial-mesenchymal interaction protects normal colonocytes from 4-HNE-induced phenotypic transformation

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  • Jacques Dupuy
  • Emma Cogo
  • Edwin Fouché
  • Françoise Guéraud
  • Fabrice Pierre
  • Pascale Plaisancié

Abstract

Introduction: Recent studies have shown that epithelial-stromal interactions could play a role in the development of colorectal cancer. Here, we investigated the role of fibroblasts in the transformation of normal colonocytes induced by 4-HNE. Methods: Normal Co colonocytes and nF fibroblasts from the same mouse colon were exposed, in monoculture (m) or coculture (c), to 4-HNE (5 μM) twice weekly for 3 weeks. Gene expression was then analysed and the ability of Co colonocytes to grow in anchorage-independent conditions was tested in soft agar. Fibroblasts previously treated or not with 4-HNE were also seeded in culture inserts positioned above the agar layers to allow paracrine exchanges with colonocytes. Results: First, 60% of the genes studied were modulated by coculture in Co colonocytes, with notably increased expression of BMP receptors. Furthermore, while 4-HNE increased the ability of monoculture-treated Co colonocytes to form colonies, this effect was not observed in coculture-treated Co colonocytes. Adding a selective BMPR1 inhibitor during the treatment phase abolished the protective effect of coculture. Conversely, addition of a BMP4 agonist to the medium of monoculture-treated Co colonocytes prevented phenotypic transformation by 4-HNE. Second, the presence of nF(m)-HNE fibroblasts during the soft agar assay increased the number and size of Co(m) colonocyte colonies, regardless of whether these cells had been previously treated with 4-HNE in monoculture. For soft agar assays performed with nF(c) and Co(c) cells initially treated in coculture, only the reassociation between Co(c)-HNE and nF(c)-HNE resulted in a small increase in the number of colonies. Conclusions: During the exposure phase, the epithelial-mesenchymal interaction protected colonocytes from 4-HNE-induced phenotypic transformation via activation of the BMP pathway. This intercellular dialogue also limited the ability of fibroblasts to subsequently promote colonocyte-anchorage-independent growth. In contrast, fibroblasts pre-exposed to 4-HNE in monoculture strongly increased the ability of Co(m) colonocytes to form colonies.

Suggested Citation

  • Jacques Dupuy & Emma Cogo & Edwin Fouché & Françoise Guéraud & Fabrice Pierre & Pascale Plaisancié, 2024. "Epithelial-mesenchymal interaction protects normal colonocytes from 4-HNE-induced phenotypic transformation," PLOS ONE, Public Library of Science, vol. 19(4), pages 1-28, April.
    • Handle: RePEc:plo:pone00:0302932
    DOI: 10.1371/journal.pone.0302932
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    1. Manolis Roulis & Aimilios Kaklamanos & Marina Schernthanner & Piotr Bielecki & Jun Zhao & Eleanna Kaffe & Laura-Sophie Frommelt & Rihao Qu & Marlene S. Knapp & Ana Henriques & Niki Chalkidi & Vasiliki, 2020. "Paracrine orchestration of intestinal tumorigenesis by a mesenchymal niche," Nature, Nature, vol. 580(7804), pages 524-529, April.
    2. Zhen Qi & Yehua Li & Bing Zhao & Chi Xu & Yuan Liu & Haonan Li & Bingjie Zhang & Xinquan Wang & Xiao Yang & Wei Xie & Baojie Li & Jing-Dong Jackie Han & Ye-Guang Chen, 2017. "BMP restricts stemness of intestinal Lgr5+ stem cells by directly suppressing their signature genes," Nature Communications, Nature, vol. 8(1), pages 1-14, April.
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