4.4 Article

D-4F decreases the expression of Aβ protein through up-regulating long non coding RNA sirt1-as in SAMP8 mice

期刊

SAUDI PHARMACEUTICAL JOURNAL
卷 25, 期 4, 页码 517-522

出版社

ELSEVIER SCIENCE BV
DOI: 10.1016/j.jsps.2017.04.017

关键词

D-4F; Sirt1-as; SAMP8; A beta protein; Long non coding RNA

资金

  1. National Nature Science Foundation of China [81270941]
  2. Key National Basic Research Program of China [2013CB530804]

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Background and objective: Cholesterol plays key roles on (A beta) metabolism and production. D-4F is the apolipoprotein A-I mimetic peptide which has been revealed a critical role in regulation cholesterol. We aimed at identifying the effects of D-4F on A beta production in SAMP8 and the underlying mechanisms. Methods: SAMP8 mice (n = 15) were randomized into three groups for treatment with D-4F given in drinking water: high-dose group (0.5 mg/ml), low-dose group (0.3 mg/ml) and control group (just drinking water). The heart, kidney, liver and brain were obtained from SAMP8 (9 of them included in the analysis). The long non-coding RNA sirt1-as was measured in all tissues. The immunohistochemistry, western blot qRT-PCR were performed to determine the sirt1-as and the relevant proteins or RNAs levels. Results: After treated with D-4F, the sirt1-as has been significantly upregulated in brain, rather than heart, kidney or liver. Specially, sirt1-as was significantly up-regulated by high dose of D-4F in the hippocampus area (p = 0.007) compared with control group. Further analysis revealed that D-4F up-regulates the expression of SIRT1. We also found that D-4F treatment significantly increased the reverse cholesterol transport related proteins liver X receptor alpha (LXR alpha) and ATP-binding cassette transporter A1 (ABCA1, p < 0.05). Finally, the amyloid beta-protein (A beta protein) was statistically lower than that in the control group (p < 0.05). Conclusion: Our observation indicated that D-4F decreases the expression of A beta protein through up-regulating long non coding RNA sirt1-as and its downstream proteins which may involve in reverse cholesterol transport. (C) 2017 Production and hosting by Elsevier B.V.

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