Failure to Down-Regulate <i>miR-154</i> Expression in Early Postnatal Mouse Lung Epithelium Suppresses Alveologenesis, with Changes in Tgf-β Signaling Similar to those Induced by Exposure to Hyperoxia - Forschungsportal der Justus-Liebig-Universität Gießen:

Journalartikel

Failure to Down-Regulate miR-154 Expression in Early Postnatal Mouse Lung Epithelium Suppresses Alveologenesis, with Changes in Tgf-β Signaling Similar to those Induced by Exposure to Hyperoxia

Autorenliste: Chao, Cho-Ming; Carraro, Gianni; Rako, Zvonimir A.; Kolck, Johannes; Sedighi, Jamschid; Zimmermann, Volker; Moiseenko, Alena; Wilhelm, Jochen; Young, Brittany M.; Chong, Lei; Wu, Jin; Contreras, Adriana; Minoo, Parviz; Barreto, Guillermo; Warburton, David; Bellusci, Saverio

Jahr der Veröffentlichung: 2020

Zeitschrift: Cells

Bandnummer: 9

Heftnummer: 4

eISSN: 2073-4409

Open Access Status: Gold

DOI Link: https://doi.org/10.3390/cells9040859

Verlag: MDPI

Abstract:
Background: Bronchopulmonary dysplasia (BPD) is a lung disease of preterm born infants, characterized by alveolar simplification. MicroRNA (miR) are known to be involved in many biological and pathological processes in the lung. Although a changed expression has been described for several miR in BPD, a causal role remains to be established. Results: Our results showed that the expression level of miR-154 increases during lung development and decreases postnatally. Further, hyperoxia treatment maintains high levels of miR-154 in alveolar type 2 cells (AT2). We hypothesized that the decrease in miR-154 expression in AT2 cells is required for normal alveologenesis. To test this hypothesis, we generated a novel transgenic mouse allowing doxycycline-based miR-154 overexpression. Maintenance of miR-154 expression in the postnatal distal lung epithelium under normoxia conditions is sufficient to reproduce the hypoalveologenesis phenotype triggered by hyperoxia. Using a pull-down assay, we identified Caveolin1 as a key downstream target of miR-154. Caveolin1 protein is downregulated in response to overexpression of miR-154. This is associated with increased phosphorylation of Smad3 and Tgf-ss signaling. We found that AT2 cells overexpressing miR-154 display decreased expression of AT2 markers and increased expression of AT1 markers. Conclusion: Our results suggest that down-regulation of miR-154 in postnatal lung may function as an important physiological switch that permits the induction of the correct alveolar developmental program, while conversely, failure to down-regulate miR-154 suppresses alveolarization, leading to the common clinically observed phenotype of alveolar simplification.

Zitierstile

Harvard-Zitierstil: Chao, C., Carraro, G., Rako, Z., Kolck, J., Sedighi, J., Zimmermann, V., et al. (2020) Failure to Down-Regulate miR-154 Expression in Early Postnatal Mouse Lung Epithelium Suppresses Alveologenesis, with Changes in Tgf-β Signaling Similar to those Induced by Exposure to Hyperoxia, Cells, 9(4), Article 859. https://doi.org/10.3390/cells9040859

APA-Zitierstil: Chao, C., Carraro, G., Rako, Z., Kolck, J., Sedighi, J., Zimmermann, V., Moiseenko, A., Wilhelm, J., Young, B., Chong, L., Wu, J., Contreras, A., Minoo, P., Barreto, G., Warburton, D., & Bellusci, S. (2020). Failure to Down-Regulate miR-154 Expression in Early Postnatal Mouse Lung Epithelium Suppresses Alveologenesis, with Changes in Tgf-β Signaling Similar to those Induced by Exposure to Hyperoxia. Cells. 9(4), Article 859. https://doi.org/10.3390/cells9040859

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