AKT2 Regulates Pulmonary Inflammation and Fibrosis via Modulating Macrophage Activation

Nie, Yunjuan; Sun, Lei; Wu, Yaxian; Yang, Yeming; Wang, Jun; He, Huiqiong; Hu, Yudong; Chang, Yanhua; Qi, Liang; Zhu, Jianwei; Ye, Richard D.; Christman, John W.; Qian, Feng

doi:10.4049/jimmunol.1601503

Cited by 62 publications

(59 citation statements)

References 55 publications

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“…BLM causes damage to the alveolar epithelial cells, leading to an interstitial inflammatory response within the first week after its administration. 19,30 However, we found there were few significant and pathological conditions. 32,33 One important downstream target protein is FoxO1, which can be deactivated through phosphorylation at its three putative phosphorylation sites for Akt.…”

Section: Discussionmentioning

confidence: 70%

“…Inflammatory responses are a critical mechanism for PF progression. BLM causes damage to the alveolar epithelial cells, leading to an interstitial inflammatory response within the first week after its administration . However, we found there were few significant changes in BLM‐induced inflammation after lanatoside C administration (Figure A‐D) and that the effect of lanatoside C in regulating the development of BLM‐induced PF is not through suppressing the inflammatory response.…”

Section: Discussionmentioning

confidence: 71%

“…17,18 To verify this hypothesis, we assessed the impact of lanatoside C in a BLM-induced mouse model of pulmonary fibrosis. 19 We found that treatment with lanatoside C protected mice against pulmonary F I G U R E 1 Lanatoside C attenuated pathological changes and reduced mortality in bleomycin-induced pulmonary fibrosis of mice. A, Chemical structure of lanatoside C (LanC).…”

mentioning

confidence: 85%

“…To verify this hypothesis, we assessed the impact of lanatoside C in a BLM‐induced mouse model of pulmonary fibrosis . We found that treatment with lanatoside C protected mice against pulmonary fibrosis in a dose‐dependent manner and reduced fibroblast proliferation, differentiation and migration in lung tissue.…”

Section: Introductionmentioning

confidence: 98%

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Lanatoside C protects mice against bleomycin‐induced pulmonary fibrosis through suppression of fibroblast proliferation and differentiation

Nie

Zhang

Jin

et al. 2019

Clin Exp Pharma Physio

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Summary It has been established that lanatoside C, a FDA‐approved cardiac glycoside, reduces proliferation of cancer cell lines. The proliferation of fibroblasts is critical to the pathogenesis of pulmonary fibrosis (PF), a progressive and fatal fibrotic lung disease lacking effective treatment. In this study we have investigated the impact of lanatoside C on a bleomycin (BLM)‐induced mouse model of PF and through the evaluation of fibroblast proliferation and activation in vitro. We evaluated explanted lung tissue by histological staining, western blot analysis, qRT‐PCR and survival analysis, demonstrating that lanatoside C was able to protect mice against BLM‐induced pulmonary fibrosis. The proliferation of cultured pulmonary fibroblasts isolated from BLM‐induced PF mice was suppressed by lanatoside C, as hypothesized, through the induction of cell apoptosis and cell cycle arrest at the G2/M phase. The Akt signalling pathway was involved in this process. Interestingly, the production of α‐SMA, fibronectin, and collagen I and III in response to TGF‐β1 in healthy mouse fibroblasts was suppressed following lanatoside C administration by inhibition of TGF‐β1/Smad signalling. In addition, TGF‐β1‐induced migration in lung fibroblasts was also impeded after lanatoside C treatment. Together, our data revealed that lanatoside C alleviated BLM‐induced pulmonary fibrosis in mice via attenuation of growth and differentiation of fibroblasts, suggesting that it has potential as a candidate therapy for PF patients.

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Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 71%

mentioning

confidence: 85%

Section: Introductionmentioning

confidence: 98%

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Lanatoside C protects mice against bleomycin‐induced pulmonary fibrosis through suppression of fibroblast proliferation and differentiation

Nie

Zhang

Jin

et al. 2019

Clin Exp Pharma Physio

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“…17 Nie et al have demonstrated that FOXO3a represses interleukin-13 transcription in macrophages to protect against bleomycin-induced pulmonary inflammation and fibrosis. 18 In addition, it has been shown that FOXO3a is capable of inhibiting the NLRP3 inflammasome by potentiating the transcription of Bim in liver macrophages (Kupffer cells). 19 Recently, genome-wide meta-analysis indicates that interplay between FOXO3a and certain MHC II molecules (e.g.…”

Section: Introductionmentioning

confidence: 99%

Forkhead transcription factor FOXO3a mediates interferon‐γ‐induced MHC II transcription in macrophages

Fan

Chen

et al. 2019

Immunology

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Summary Macrophages are professional antigen‐presenting cells relying on the expression of class II major histocompatibility complex (MHC II) genes. Interferon‐γ (IFN‐γ) activates MHC II transcription via the assembly of an enhanceosome centred on class II trans‐activator (CIITA). In the present study, we investigated the role of the forkhead transcription factor FOXO3a in IFN‐ γ‐induced MHC II transcription in macrophages. Knockdown of FOXO3a, but not FOXO1 or FOXO4, diminished IFN‐γ‐induced MHC II expression in RAW cells. On the contrary, over‐expression of FOXO3a, but neither FOXO1 nor FOXO4, enhanced CIITA‐mediated trans‐activation of the MHC II promoter. IFN‐γ treatment promoted the recruitment of FOXO3a to the MHC II promoter. Co‐immunoprecipitation and RE‐ChIP assays showed that FOXO3a was a component of the MHC II enhanceosome forming interactions with CIITA, RFX5, RFXB and RFXAP. FOXO3a contributed to MHC II transcription by altering histone modifications surrounding the MHC II promoter. Of interest, FOXO3a was recruited to the type IV CIITA promoter and directly activated CIITA transcription by interacting with signal transducer of activation and transcription 1 in response to IFN‐γ stimulation. In conclusion, our data unveil a novel role for FOXO3a in the regulation of MHC II transcription in macrophages.

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C‐C motif chemokine ligand 5 confines liver regeneration by down‐regulating reparative macrophage‐derived hepatocyte growth factor in a forkhead box O 3a–dependent manner

et al. 2022

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Background and Aims: Liver regeneration (LR) is vital for the recovery of liver function after hepatectomy. Limited regeneration capacity, together with insufficient remnant liver volume, is a risk factor for posthepatectomy liver failure (PHLF) resulting from small-for-size syndrome. Although inflammation plays an important role in controlling LR, the underlying mechanisms still remain obscure. Approach and Results:We identified C-C motif chemokine ligand (CCL) 5 as an important negative regulator for LR. CCL5 levels were elevated after partial hepatectomy (PHx), both in healthy donors of living donor liver transplantation (LT) and PHx mouse models. Ccl5 knockout mice displayed

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AKT2 Regulates Pulmonary Inflammation and Fibrosis via Modulating Macrophage Activation

Cited by 62 publications

References 55 publications

Lanatoside C protects mice against bleomycin‐induced pulmonary fibrosis through suppression of fibroblast proliferation and differentiation

Lanatoside C protects mice against bleomycin‐induced pulmonary fibrosis through suppression of fibroblast proliferation and differentiation

Forkhead transcription factor FOXO3a mediates interferon‐γ‐induced MHC II transcription in macrophages

C‐C motif chemokine ligand 5 confines liver regeneration by down‐regulating reparative macrophage‐derived hepatocyte growth factor in a forkhead box O 3a–dependent manner

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