Pleural mesothelial cell transformation into myofibroblasts and haptotactic migration in response to TGF-β1 in vitro

Nasreen, Najmunnisa; Mohammed, Kamal A.; Mubarak, Kamal K.; Baz, Maher A.; Akindipe, Olufemi; Fernández-Bussy, Sebastián; Antony, Veena B.

doi:10.1152/ajplung.90587.2008

Cited by 99 publications

(103 citation statements)

References 46 publications

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“…TGF-b is most efficiently secreted as a large latent complex and most TGF-b is stored in the extracellular matrix before activation [19]. A key feature of IPF is the presence of high levels of inactive precursor form TGF-b1 in the lung parenchyma [27].…”

Section: Pulmonary Fibrosismentioning

confidence: 99%

A neutrophil elastase inhibitor prevents bleomycin-induced pulmonary fibrosis in mice

2012

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Neutrophil elastase plays pivotal roles in the pathogenesis of pulmonary fibrosis. The neutrophil elastase inhibitor, sivelestat, could alleviate pulmonary fibrosis; however, the antifibrotic mechanisms have not yet been clarified. We examined the antifibrotic mechanisms, mainly focusing on a key fibrotic cytokine, transforming growth factor (TGF)-b1, in this study.To elucidate the antifibrotic mechanisms of sivelestat, we examined a murine model of bleomycin-induced early-stage pulmonary fibrosis. After intratracheal instillation of bleomycin, sivelestat was administered intraperitoneally once a day for 7 or 14 days. Bronchoalveolar lavage fluid and lung samples were examined on day 7 or day 14 after bleomycin instillation.In the bleomycin-induced early-stage pulmonary fibrosis model, the neutrophil elastase level was increased in the lungs. Sivelestat significantly inhibited the increase in lung collagen content, fibrotic changes, the numbers of total cells (including macrophages, neutrophils and lymphocytes), the levels of the active form of TGF-b1 and phospho-Smad2 in bleomycin-induced earlystage pulmonary fibrosis. The total TGF-b1 levels and relative changes of TGF-b1 mRNA expression, however, were not decreased significantly by sivelestat.These results suggest that sivelestat alleviated bleomycin-induced pulmonary fibrosis via inhibition of both TGF-b activation and inflammatory cell recruitment in the lung.

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Section: Pulmonary Fibrosismentioning

confidence: 99%

A neutrophil elastase inhibitor prevents bleomycin-induced pulmonary fibrosis in mice

2012

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“…However, our current understanding of DC chemotaxis is largely qualitative and limited to 2D (16)(17)(18)(19). Furthermore, while it is well established that cell migration requires different mechanisms in 3D vs. 2D (20)(21)(22)(23)(24)(25), nearly all chemotaxis studies to date have been performed in 2D or 2.5D conditions largely because of the lack of model systems in which well defined gradients can be created in 3D while evaluating cell invasion (especially because DC migration is relatively fast compared to the time scale of diffusion for gradient establishment).…”

mentioning

confidence: 99%

Dendritic cell chemotaxis in 3D under defined chemokine gradients reveals differential response to ligands CCL21 and CCL19

Haessler

Pisano

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

184

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Dendritic cell (DC) homing to the lymphatics and positioning within the lymph node is important for adaptive immunity, and is regulated by gradients of CCL19 and CCL21, ligands for CCR7. Despite the importance of DC chemotaxis, it is not well understood how DCs interpret gradients of these chemokines in a complex 3D microenvironment. Here, we use a microfluidic device that allows rapid establishment of stable gradients in 3D matrices to show that DC chemotaxis in 3D can respond to CCR7 ligand gradients as small as 0.4%, which helps explain how DCs sense lymphatic vessels in an environment where broadcast distance for chemokine diffusion is hindered by convective flows into the vessel. Interestingly, DCs displayed similar sensitivities to both chemokines at small gradients (≤60 nM∕mm), but migrated more efficiently towards higher gradients of CCL21, which unlike CCL19 binds strongly to matrix proteoglycans and signals without the need for internalization. Furthermore, cells preferentially migrated towards CCL21 when exposed to equal and opposite gradients of CCL21 and CCL19 simultaneously, even when matrix-binding of CCL21 was prevented. Although these ligands have similar binding affinity to CCR7, our results demonstrate that, in a 3D environment, CCL21 is a more potent directional cue for DC migration than CCL19. These findings provide new quantitative insight into DC chemotaxis in a physiological 3D environment and suggest how CCL19 and CCL21 may signal differently to fine-tune DC homing and positioning within the lymphatic system. These results also have broad relevance to other systems of cell chemotaxis, which remain poorly understood in the 3D context.D endritic cells (DCs) are considered the most potent and professional antigen-presenting cells. DCs are positioned throughout the periphery, and when activated, migrate to lymphatic vessels and into lymph nodes, where they can direct antigen-specific Tcell responses. Upon activation or maturation, DCs upregulate the C-C chemokine-receptor CCR7, which allows them to sense and home towards CCR7 ligand-secreting lymphatic vessels and lymph nodes (1). The two known ligands for CCR7 are the C-C chemokines CCL21 and CCL19 (2); both are secreted by stromal cells in the lymph node paracortex to properly position DCs with CCR7 þ naïve T cells for their activation. CCL21, but not CCL19, is also expressed by the endothelium of lymphatic vessels in the periphery (1). Thus, CCR7-mediated chemotaxis is critical for DC homing to, and positioning within, lymph nodes and for T cell activation there (3).CCL19 and CCL21 function as directional signals presumably by virtue of concentration gradients (∇C) that guide DCs towards areas of increasing concentrations. Interestingly, CCL19 and CCL21 have similar binding affinities for CCR7 (4-6) and similar chemotactic potential for DCs and T cells under 2D conditions (7,8), but differ in their internalization (8, 9) as well as their binding affinity to extracellular matrix (ECM) proteoglycans. Specifically, the positively charged C t...

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“…3 Nasreen et al 9 reported that TGF-b1 induces PMC EMT, and PMCs are a source of myofibroblasts in IPF. PMCs undergoing EMT produce large amount of collagen and contribute to the overdeposition of ECM in sub-pleural fibrosis.…”

Section: Discussionmentioning

confidence: 99%

“…5,7,8 PMCs with EMT are considered a source of myofibroblasts, which are the key cells within fibroproliferative foci. 3,8,9 Bleomycin is a classical inducer of pulmonary fibrosis model. In animal models, lung fibrosis induced by intraperitoneal bleomycin injection exhibits a sub-pleural fibrotic distribution similar to what is seen in human IPF.…”

Section: Introductionmentioning

confidence: 99%

miR-18a-5p Inhibits Sub-pleural Pulmonary Fibrosis by Targeting TGF-β Receptor II

Zhang

Yue²,

Fei³

et al. 2017

Molecular Therapy

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Pleural mesothelial cell transformation into myofibroblasts and haptotactic migration in response to TGF-β1 in vitro

Cited by 99 publications

References 46 publications

A neutrophil elastase inhibitor prevents bleomycin-induced pulmonary fibrosis in mice

A neutrophil elastase inhibitor prevents bleomycin-induced pulmonary fibrosis in mice

Dendritic cell chemotaxis in 3D under defined chemokine gradients reveals differential response to ligands CCL21 and CCL19

miR-18a-5p Inhibits Sub-pleural Pulmonary Fibrosis by Targeting TGF-β Receptor II

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