ATRA mechanically reprograms pancreatic stellate cells to suppress matrix remodelling and inhibit cancer cell invasion

Chronopoulos, Antonios; Robinson, Benjamin; Sarper, Müge; Cortés, Ernesto; Auernheimer, Vera; Lachowski, Dariusz; Attwood, Simon J.; García, Reinaldo Menéndez; Ghassemi, Saba; Fabry, Ben; Hernández, Armando del Río

doi:10.1038/ncomms12630

Cited by 204 publications

(187 citation statements)

References 68 publications

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“…Using clinical specimen and experimental mouse models, Laklai et al identified a distinct, highly stiff, matricellular-stromal phenotype that was specifically associated with reduced epithelial transforming growth factor (TGF)-β signalling, elevated β-integrin mechano-signalling and Stat3 activation resulting in therapeutic resistance and significantly shortened survival in mice and humans 37. In line with these findings, ATRA, an active metabolite of vitamin A, was reported to reprogram mechanical quiescence in PSCs via a mechanism involving a retinoic acid receptor beta-dependent downregulation of actomyosin contractility 38. Furthermore, Rho kinase (ROCK) signalling, Yes-associated protein 1 and Janus kinase 2 and signal transducer and activator of transcription 3 signalling pathways have been associated with tissue tension and tumour cell contractility 39–41…”

Section: Introductionmentioning

confidence: 83%

Stromal biology and therapy in pancreatic cancer: ready for clinical translation?

Neeße

Bauer

Öhlund

et al. 2018

Gut

259

222

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Pancreatic ductal adenocarcinoma (PDA) is notoriously aggressive and hard to treat. The tumour microenvironment (TME) in PDA is highly dynamic and has been found to promote tumour progression, metastasis niche formation and therapeutic resistance. Intensive research of recent years has revealed an incredible heterogeneity and complexity of the different components of the TME, including cancer-associated fibroblasts, immune cells, extracellular matrix components, tumour vessels and nerves. It has been hypothesised that paracrine interactions between neoplastic epithelial cells and TME compartments may result in either tumour-promoting or tumour-restraining consequences. A better preclinical understanding of such complex and dynamic network systems is required to develop more powerful treatment strategies for patients. Scientific activity and the number of compelling findings has virtually exploded during recent years. Here, we provide an update of the most recent findings in this area and discuss their translational and clinical implications for basic scientists and clinicians alike.

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Section: Introductionmentioning

confidence: 83%

Stromal biology and therapy in pancreatic cancer: ready for clinical translation?

Neeße

Bauer

Öhlund

et al. 2018

Gut

259

222

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“…Agents targeting LOX activity could decrease collagen crosslinking, thereby reducing the density of the tumour stroma and increase the effectiveness of anticancer therapies 279–282 . The vitamin D receptor ligand calcipotriol 283 and all-trans retinoic acid (ATRA) 284 are other agents that reduced fibrosis in experiments with PDAC models.…”

Section: Tumour-stroma Targeting Strategiesmentioning

confidence: 99%

Targeting the tumour stroma to improve cancer therapy

2018

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Cancers are not merely composed of cancer cells alone and, instead, are complex ‘ecosystems’ comprising many different cell types and noncellular factors. The tumour stroma is a critical component of the tumour microenvironment, where it has crucial roles in tumour initiation, progression, and metastasis. Most anticancer therapies target cancer cells specifically, but the tumour stroma can promote resistance of cancer cells to such therapies, eventually resulting in fatal disease. Therefore, novel treatment strategies should combine anticancer and antistroma agents. Herein, we provide an overview of the advances in understanding the complex cancer cell–tumour stroma interactions, and discuss how this knowledge can result in more effective therapeutic strategies, which might ultimately improve patient outcomes.

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“…Similarly, all trans-retinoic acid (ATRA), the physiological active metabolite of vitamin A, restores mechanical quiescence in PSCs via activation of the retinoic acid receptor beta (RAR-β) and down regulation of actomyosin contractility, which suppresses the ability of PSCs to apply forces and mechanosense matrix rigidity. Mechanically quiescent PSCs are unable to remodel and stiffen the matrix, and this creates a microenvironment that is not favourable for pancreatic cancer cell invasion (figure 2) [35]. Notably, PSCs were removed from remodelled collagen/matrigel matrices before cancer cell invasion in these in vitro experiments; thus, the reduced ability of cancer cells to invade was related to the mechanical and/or topological changes in the ECM.…”

Section: Reprogramming Cell Mechanics Induces Quiescence In Pscs Supmentioning

confidence: 99%

“…Bottom, bright field images of PSC and its corresponding force map. Panel reproduced from [35]. CC BY 4.0.…”

Section: Atomic Force Microscopymentioning

confidence: 99%

Pancreatic cancer: a mechanobiology approach

Chronopoulos

Lieberthal

Hernández

2017

Converg. Sci. Phys. Oncol.

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Despite many years of effort from cancer biologists and clinical oncologists, pancreatic ductal adenocarcinoma (PDAC) remains a thoroughly recalcitrant disease, resisting both conventional forms of cancer treatment and radical innovative therapies. Perhaps driving the lack of success in PDAC is the underappreciation of the primary hallmark of the tumour: a fibrotic extracellular matrix (ECM) that composes a majority of the highly rigid solid carcinoma. In recent years we have come to understand that the homeostasis of ECM mechanics is pivotal for the homeostasis of cells and the progression or initiation of a malignant phenotype. This can be understood by way of mechanobiology, a field that attempts to understand how physical forces like ECM stiffness alter cell behaviour. In this review, we provide an overview of our understanding of PDAC from this perspective and the recent advances in biophysics and engineering that allow for new tools with which to investigate the mechanobiology of PDAC.

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ATRA mechanically reprograms pancreatic stellate cells to suppress matrix remodelling and inhibit cancer cell invasion

Cited by 204 publications

References 68 publications

Stromal biology and therapy in pancreatic cancer: ready for clinical translation?

Stromal biology and therapy in pancreatic cancer: ready for clinical translation?

Targeting the tumour stroma to improve cancer therapy

Pancreatic cancer: a mechanobiology approach

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