期刊
AMERICAN JOURNAL OF PATHOLOGY
卷 186, 期 10, 页码 2614-2622出版社
ELSEVIER SCIENCE INC
DOI: 10.1016/j.ajpath.2016.06.018
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资金
- NIH [ES023438, DK083952]
- National Natural Science Foundation of China Youth Science Fund Project [81402641]
- China Scholarship Council [201506275099]
Liver X receptors (LXRs) were identified as receptors that sense oxidized cholesterol derivatives. LXRs are best known for their hepatic functions in regulating cholesterol metabolism and triglyceride synthesis, but whether and how LXRs play a role in the lung diseases is less understood. To study the function of LXRs in acute respiratory distress syndrome (ARDS), we applied the oleic acid (OA) model of ARDS to mice whose LXR was genetically or pharmacologically activated. The VP-LXR alpha knock-in (LXR-KI) mice, in which a constitutively activated LXR alpha (VP-LXR alpha) was inserted into the mouse LXR alpha. locus, were used as the genetic gain-of-function model. We showed that the OA-induced lung damages, including the cytokine levels and total cell numbers and neutrophil numbers in the bronchoalveolar lavage fluid, the wet/dry weight ratio, and morphological abnormalities were reduced in the LXR-KI mice and wild-type mice treated with the LXR agonist GW3965. The pulmonoprotective effect of GW3965 was abolished in the LXR-null mice. Consistent with the pulmonoprotective effect of LXR and the induction of antioxidant enzymes by LXR, the OA-induced suppression of superoxide dismutase and catalase was attenuated in LXR-KI mice and GW3965-treated wild-type mice. Taken together, our results demonstrate that activation of LXRs can alleviate OA-induced ARDS by attenuating the inflammatory response and enhancing antioxidant capacity.
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