Caveolin1 and YAP drive mechanically induced mesothelial to mesenchymal transition and fibrosis

Despite their emerging relevance to fully understand disease pathogenesis, we have as yet a poor understanding as to how biomechanical signals are integrated with specific biochemical pathways to determine cell behaviour. Mesothelial-to-mesenchymal transition (MMT) markers colocalized with TGF-β1-de...

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Published in:	Cell death & disease Vol. 11; no. 8; p. 647
Main Authors:	Strippoli, Raffaele, Sandoval, Pilar, Moreno-Vicente, Roberto, Rossi, Lucia, Battistelli, Cecilia, Terri, Michela, Pascual-Antón, Lucía, Loureiro, Marta, Matteini, Francesca, Calvo, Enrique, Jiménez-Heffernan, José Antonio, Gómez, Manuel José, Jiménez-Jiménez, Victor, Sánchez-Cabo, Fátima, Vázquez, Jesús, Tripodi, Marco, López-Cabrera, Manuel, del Pozo, Miguel Ángel
Format:	Journal Article
Language:	English
Published:	London Nature Publishing Group UK 03-08-2020 Springer Nature B.V
Subjects:	101/58 13/1 13/21 14/19 38/89 631/80/304 64/60 692/420/256/2515 82/51 96/47 Adaptor Proteins, Signal Transducing - metabolism Adaptor Proteins, Signal Transducing - physiology Animal models Animals Antibodies Biochemistry Biomechanics Biomedical and Life Sciences Caveolin Caveolin 1 - metabolism Caveolin 1 - physiology Caveolin-1 Caveolins - metabolism Cell Biology Cell Culture Disease Models, Animal Epithelial Cells - metabolism Epithelial-Mesenchymal Transition - genetics Female Fibrosis Gene expression Humans Immunology Kinases Life Sciences Male Mechanotransduction Mesenchyme Mice Mice, Inbred C57BL Nuclear transport Peritoneal Dialysis - methods Peritoneal Fibrosis - genetics Peritoneal Fibrosis - metabolism Peritoneal Fibrosis - pathology Peritoneum Peritoneum - metabolism Proteomes Signal transduction Signal Transduction - drug effects Smad3 Protein - metabolism Tissue Adhesions - metabolism Transcription Transcription Factors - metabolism Transcription Factors - physiology Transcriptomes Transforming Growth Factor beta1 - metabolism Transforming growth factor-b1 Yes-associated protein
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Summary:	Despite their emerging relevance to fully understand disease pathogenesis, we have as yet a poor understanding as to how biomechanical signals are integrated with specific biochemical pathways to determine cell behaviour. Mesothelial-to-mesenchymal transition (MMT) markers colocalized with TGF-β1-dependent signaling and yes-associated protein (YAP) activation across biopsies from different pathologies exhibiting peritoneal fibrosis, supporting mechanotransduction as a central driving component of these class of fibrotic lesions and its crosstalk with specific signaling pathways. Transcriptome and proteome profiling of the response of mesothelial cells (MCs) to linear cyclic stretch revealed molecular changes compatible with bona fide MMT, which (i) overlapped with established YAP target gene subsets, and were largely dependent on endogenous TGF-β1 signaling. Importantly, TGF-β1 blockade blunts the transcriptional upregulation of these gene signatures, but not the mechanical activation and nuclear translocation of YAP per se. We studied the role therein of caveolin-1 (CAV1), a plasma membrane mechanotransducer. Exposure of CAV1-deficient MCs to cyclic stretch led to a robust upregulation of MMT-related gene programs, which was blunted upon TGF-β1 inhibition. Conversely, CAV1 depletion enhanced both TGF-β1 and TGFBRI expression, whereas its re-expression blunted mechanical stretching-induced MMT. CAV1 genetic deficiency exacerbated MMT and adhesion formation in an experimental murine model of peritoneal ischaemic buttons. Taken together, these results support that CAV1-YAP/TAZ fine-tune the fibrotic response through the modulation of MMT, onto which TGF-β1-dependent signaling coordinately converges. Our findings reveal a cooperation between biomechanical and biochemical signals in the triggering of MMT, representing a novel potential opportunity to intervene mechanically induced disorders coursing with peritoneal fibrosis, such as post-surgical adhesions.
Bibliography:	ObjectType-Article-1 SourceType-Scholarly Journals-1 ObjectType-Feature-2 content type line 23
ISSN:	2041-4889 2041-4889
DOI:	10.1038/s41419-020-02822-1