Induction of a Mesenchymal Expression Program in Lung Epithelial Cells by Wingless Protein (Wnt)/β-Catenin Requires the Presence of c-Jun N-Terminal Kinase–1 (JNK1)

Velden, Jos van der; Guala, Amy S.; Leggett, Susan E.; Sluimer, Jasper D.; Badura, Elsbeth C. H. L.; Janssen–Heininger, Yvonne M. W.

doi:10.1165/rcmb.2011-0297oc

Cited by 28 publications

(26 citation statements)

References 48 publications

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“…Similarly, cigarette smoke has been shown to induce EMT in alveolar epithelial cells (61)(62)(63), which may impair alveolar re-epithelization upon damage (64,65), thus also having implications for the development of emphysema. Cigarette smoke affects WNT/b-catenin signaling and EMT in alveolar epithelial cells (66,67), although these studies show an inhibition of b-catenin signaling, which is not in line with previous studies showing the induction of EMT (68,69).…”

Section: Epithelial To Mesenchymal Transitioncontrasting

confidence: 97%

Airway Epithelial Barrier Dysfunction in Chronic Obstructive Pulmonary Disease: Role of Cigarette Smoke Exposure

Aghapour¹,

Raee

Moghaddam

et al. 2018

Am J Respir Cell Mol Biol

228

216

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The epithelial lining of the airway forms the first barrier against environmental insults, such as inhaled cigarette smoke, which is the primary risk factor for the development of chronic obstructive pulmonary disease (COPD). The barrier is formed by airway epithelial junctions, which are interconnected structures that restrict permeability to inhaled pathogens and environmental stressors. Destruction of the epithelial barrier not only exposes subepithelial layers to hazardous agents in the inspired air, but also alters the normal function of epithelial cells, which may eventually contribute to the development of COPD. Of note, disruption of epithelial junctions may lead to modulation of signaling pathways involved in differentiation, repair, and proinflammatory responses. Epithelial barrier dysfunction may be particularly relevant in COPD, where repeated injury by cigarette smoke exposure, pathogens, inflammatory mediators, and impaired epithelial regeneration may compromise the barrier function. In the current review, we discuss recent advances in understanding the mechanisms of barrier dysfunction in COPD, as well as the molecular mechanisms that underlie the impaired repair response of the injured epithelium in COPD and its inability to redifferentiate into a functionally intact epithelium.

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Section: Epithelial To Mesenchymal Transitioncontrasting

confidence: 97%

Airway Epithelial Barrier Dysfunction in Chronic Obstructive Pulmonary Disease: Role of Cigarette Smoke Exposure

Aghapour¹,

Raee

Moghaddam

et al. 2018

Am J Respir Cell Mol Biol

228

216

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“…Even with siRNA knockdown of b-catenin, TGFb1 exposure still reduced E-cadherin and zonula occludens 1 (ZO-1) expression and increased S100A4 expression. In contrast, TGFb1-induced expression of aSMA was attenuated with siRNA knockdown of b-catenin ( Figure E14), complementing recent studies by other investigators (26,27). Confocal immunofluorescence on lung sections from cell fate mapping mice revealed that total S100A41 and EMT-derived bgal1/S100A41 lung fibroblasts increased at 2 weeks after bleomycin ( Figure E15A).…”

Section: Mice With Deficiency Of B-catenin In the Alveolar Epitheliumsupporting

confidence: 84%

β-Catenin in the Alveolar Epithelium Protects from Lung Fibrosis after Intratracheal Bleomycin

Tanjore

Degryse

Crossno

et al. 2013

Am J Respir Crit Care Med

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Rationale: Alveolar epithelial cells (AECs) play central roles in the response to lung injury and the pathogenesis of pulmonary fibrosis. Objectives: We aimed to determine the role of b-catenin in alveolar epithelium during bleomycin-induced lung fibrosis. Methods: Genetically modified mice were developed to selectively delete b-catenin in AECs and were crossed to cell fate reporter mice that express b-galactosidase (bgal) in cells of AEC lineage. Mice were given intratracheal bleomycin (0.04 units) and assessed for AEC death, inflammation, lung injury, and fibrotic remodeling. Mouse lung epithelial cells (MLE12) with small interfering RNA knockdown of b-catenin underwent evaluation for wound closure, proliferation, and bleomycin-induced cytotoxicity. Measurements and Main Results: Increased b-catenin expression was noted in lung parenchyma after bleomycin. Mice with selective deletion of b-catenin in AECs had greater AEC death at 1 week after bleomycin, followed by increased numbers of fibroblasts and enhanced lung fibrosis as determined by semiquantitative histological scoring and total collagen content. However, no differences in lung inflammation or protein levels in bronchoalveolar lavage were noted. In vitro, b-catenin-deficient AECs showed increased bleomycininduced cytotoxicity as well as reduced proliferation and impaired wound closure. Consistent with these findings, mice with AEC b-catenin deficiency showed delayed recovery after bleomycin.Conclusions: b-Catenin in the alveolar epithelium protects against bleomycin-induced fibrosis. Our studies suggest that AEC survival and wound healing are enhanced through b-catenin-dependent mechanisms. Activation of the developmentally important b-catenin pathway in AECs appears to contribute to epithelial repair after epithelial injury.

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“…Mechanical stress caused by excessive contractility leads to an aberrant wound-healing response and fibrosis [33]. In epithelial-mesenchymal cell transition (EMT), which occurs in pulmonary fibrosis, is seen the concomitant increased amounts of mRNA levels of α-SMA, FSP1 and vimentin [55]. According with this, our study showed enhanced immunolabeling of α-SMA in the subcutaneous AT of cancer cachectic group, as well as increased mRNA expression of FSP1.…”

Section: Discussionsupporting

confidence: 55%

Adipose tissue fibrosis in human cancer cachexia: the role of TGFβ pathway

et al. 2017

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BackgroundCancer cachexia is a multifactorial syndrome that dramatically decreases survival. Loss of white adipose tissue (WAT) is one of the key characteristics of cachexia. WAT wasting is paralleled by microarchitectural remodeling in cachectic cancer patients. Fibrosis results from uncontrolled ECM synthesis, a process in which, transforming growth factor-beta (TGFβ) plays a pivotal role. So far, the mechanisms involved in adipose tissue (AT) re-arrangement, and the role of TGFβ in inducing AT remodeling in weight-losing cancer patients are poorly understood. This study examined the modulation of ECM components mediated by TGFβ pathway in fibrotic AT obtained from cachectic gastrointestinal cancer patients.MethodsAfter signing the informed consent form, patients were enrolled into the following groups: cancer cachexia (CC, n = 21), weight-stable cancer (WSC, n = 17), and control (n = 21). The total amount of collagen and elastic fibers in the subcutaneous AT was assessed by histological analysis and by immunohistochemistry. TGFβ isoforms expression was analyzed by Multiplex assay and by immunohistochemistry. Alpha-smooth muscle actin (αSMA), fibroblast-specific protein (FSP1), Smad3 and 4 were quantified by qPCR and/or by immunohistochemistry. Interleukin (IL) 2, IL5, IL8, IL13 and IL17 content, cytokines known to be associated with fibrosis, was measured by Multiplex assay.ResultsThere was an accumulation of collagen and elastic fibers in the AT of CC, as compared with WSC and controls. Collagens type I, III, VI, and fibronectin expression was enhanced in the tissue of CC, compared with both WSC and control. The pronounced expression of αSMA in the surrounding of adipocytes, and the increased mRNA content for FSP1 (20-fold) indicate the presence of activated myofibroblasts; particularly in CC. TGFβ1 and TGFβ3 levels were up-regulated by cachexia in AT, as well in the isolated adipocytes. Smad3 and Smad4 labeling was found to be more evident in the fibrotic areas of CC adipose tissue.ConclusionsCancer cachexia promotes the development of AT fibrosis, in association with altered TGFβ signaling, compromising AT organization and function.

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Induction of a Mesenchymal Expression Program in Lung Epithelial Cells by Wingless Protein (Wnt)/β-Catenin Requires the Presence of c-Jun N-Terminal Kinase–1 (JNK1)

Cited by 28 publications

References 48 publications

Airway Epithelial Barrier Dysfunction in Chronic Obstructive Pulmonary Disease: Role of Cigarette Smoke Exposure

Airway Epithelial Barrier Dysfunction in Chronic Obstructive Pulmonary Disease: Role of Cigarette Smoke Exposure

β-Catenin in the Alveolar Epithelium Protects from Lung Fibrosis after Intratracheal Bleomycin

Adipose tissue fibrosis in human cancer cachexia: the role of TGFβ pathway

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