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Activation of SIRT1 ameliorates LPS-induced lung injury in mice via decreasing endothelial tight junction permeability

   
@article{APS9963,
	author = {Cui-ping Fu and Sheng-yu Hao and Xiao-bo Xu and Jian Zhou and Zi-long Liu and Huan Lu and Li-min Wang and Wei-zhong Jin and Shan-qun Li},
	title = {Activation  of SIRT1 ameliorates  LPS-induced lung injury in mice via decreasing endothelial  tight junction permeability},
	journal = {Acta Pharmacologica Sinica},
	volume = {40},
	number = {5},
	year = {2019},
	keywords = {},
	abstract = {The integrity of the endothelial barrier is a determinant of the prognosis of lipopolysaccharide  (LPS)-induced acute lung injury (ALI). In this study, we investigated whether and how Sirtuin 1 (SIRT1) maintained the vascular integrity during ALI. An experimental model of ALI was established in mice through intratracheal administration of LPS (10 mg/kg). LPS stimulation significantly increased the pulmonary permeability and decreased the expression of SIRT1 and tight junction proteins (TJs), including occludin, claudin-5, tight junction protein 1 and tight junction protein 2. Morphological studies showed that LPS induced obvious lung injury with inflammatory cell infiltration in the interstitial and alveolar space, hemorrhage,  edema, and the thickened alveolar wall compared to the control mice. Intratracheal administration  of the selective  SIRT1 activator SRT1720 (6.25 mg/kg) significantly  attenuated  LPS- induced lung injury, lung hyper-permeability and increased  TJs expression, whereas intratracheal administration  of the selective SIRT1 inhibitor EX527 (6.25 mg/kg) aggravated  LPS-induced ALI. Similar protective effects of SIRT1 on pulmonary cellular permeability were observed in primary human pulmonary microvascular endothelial cells treated with LPS (2 mg/mL) in vitro. We further demonstrated that the RhoA/ROCK signaling pathway was activated in SIRT1 regulation of tight junction permeability. The RhoA/ROCK inhibitor Y-27632 (10 μM) increased the expression of TJs and reversed  LPS- or EX527-induced hyper-permeability. In conclusion, SIRT1 ameliorates LPS-induced lung injury via decreasing endothelial tight junction permeability, possibly via RhoA/ ROCK signaling pathway. This finding may contribute to the development of new therapeutic approaches for lung injury.},
	issn = {1745-7254},	url = {http://www.chinaphar.com/article/view/9963}
}