Effect of SIRT1 weakening on inflammation in mice with acute respiratory distress syndrome induced by lipopolysaccharide

doi:10.3877/cma.j.issn.1674-6902.2017.02.010

Abstract

Abstract:

Objective

To investigate the effect and mechanism of SIRT1 on inflammation in acute respiratory distress syndrome (ARDS) mice induced by lipopolysaccharide(LPS) .

Methods

The differences of related gene expression of lung tissues in two mice, including the SIRT1^{+ /-} mice with SIRT1 gene is knocked down and the wild-type mice, were detected by qRT-PCR and Western Blot. Then the ARDS model was induced in two kinds of mice by intraperitoneal injection of LPS, and the control group were injected with equal volume of saline. The pathological changes of lung tissue were observed by HE staining and the lung W/D ratio were calculated, the total protein concentration in BALF were detected by BCA, the levels of inflammatory factor tumour necrosis factor-α(TNF-α) and interleukin-6(IL-6) in bronchoalveolar lavage fluid (BALF) and plasma were tested by ELISA, the expression of p38 MAPK, p-p38 MAPK and p-ATF2 in lung tissue were detected by Western Blot.

Results

Compared with wild-type mice, the mRNA and protein expression of SIRT1 in lung tissue in SIRT1^{+ /-} were significantly decreased, The difference was statistically significant(P<0.01). After ARDS induced by LPS, The pathological observation about two kinds of mice both showed infiltration of inflammatory cells in lung tissue, destruction of alveolar structure, edema of interstitial, thickening of alveolar septum, and SIRT1^{+ /-} mice were more severely damaged than wild-type mice. In SIRT1^{+ /-} mice, lung W/D ratio, total protein concentration in BALF, the levels of inflammatory factors TNF-α and IL-6 in BALF and plasma were significantly increased(P<0.05), the expression of p-p38 MAPK/p38 MAPK and p-ATF2 in lung tissues were increased more significantly than in wild-type mice(P<0.05).

Conclusion

The SIRT1 gene plays an important role in the inflammatory process of mice with ARDS induced by LPS, which may be related to the increased activity of p38 MAPK-p-ATF2 signaling pathway.

Key words: Acute respiratory distress syndrome, SIRT1, p38 MAPK, p-ATF2

Wei Zhao, Junyan Liu, Yuying Li. Effect of SIRT1 weakening on inflammation in mice with acute respiratory distress syndrome induced by lipopolysaccharide[J]. Chinese Journal of Lung Diseases(Electronic Edition), 2017, 10(02): 163-167.

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https://zhfbjbzz.cma-cmc.com.cn/EN/Y2017/V10/I02/163

Figures/Tables 6

References 15

1	宋旸，蒋昊翔，张永红，等. 急性呼吸窘迫综合征药物研究进展[J/CD]. 中华肺部疾病杂志(电子版), 2015, 8(6): 769-772.
2	Silva PL, Rocco PR, Pelosi P. FG-4497: a new target for acute respiratory distress syndrome？[J]. Expert Rev Respir Med, 2015, 9(4): 405-409.
3	Ivy JM, Klar AJ, Hicks JB. Cloning and characterization of four SIR genes of saccharomyces cerevisiae[J]. Mol Cell Biol, 1986, 6(2): 688-702.
4	Yang H, Bi Y, Xue L, et al. Multifaceted modulation of SIRT1 in cancer and inflammation[J]. Crit Rev Oncog, 2015, 20(1-2): 49-64.
5	Ma Y, Nie H, Chen H, et al. NAD^＋/NADH metabolism and NAD^＋-dependent enzymes in cell death and ischemic brain injury: current advances and therapeutic implications[J]. Curr Med Chem, 2015, 22(10): 1239-1247.
6	Xie J, Zhang X, Zhang L. Negative regulation of inflammation by SIRT1[J]. Pharmacol Res, 2013, 67(1): 60-67.
7	Vachharajani VT, Liu T, Wang X, et al. Sirtuins link inflammation and metabolism[J]. J Immunol Res, 2016, 2016: 8167273.
8	Archer SL. Pre-B-cell colony-enhancing factor regulates vascular smooth muscle maturation through a NAD^＋-dependent mechanism: recognition of a new mechanism for cell diversity and redox regulation of vascular tone and remodeling[J]. Circ Res, 2005, 97(1): 4-7.
9	Shinozaki S, Chang K, Sakai M, et al. Inflammatory stimuli induce inhibitory S-nitrosylation of the deacetylase SIRT1 to increase acetylation and activation of p53 and p65[J]. Sci Signal, 2014, 7(351): ra106-ra106.
10	Rajendrasozhan S, Yang SR, Kinnula VL, et al. SIRT1, an antiinflammatory and antiaging protein, is decreased in lungs of patients with chronic obstructive pulmonary disease[J]. Am J Respir Crit Care Med, 2008, 177(8): 861-870.
11	Johnson GL, Lapadat R. Mitogen-activated protein kinase pathways mediated by ERK, JNK, and p38 protein kinases[J]. Science, 2002, 298(5600): 1911-1912.
12	Han J, Sun P. The pathways to tumor suppression via route p38[J]. Trends Biochem Sci, 2007, 32(8): 364-371.
13	Raman M, Chen W, Cobb MH. Differential regulation and properties of MAPKs[J]. Oncogene, 2007, 26(26): 3100-3112.
14	张琳，姜勇，张璐. p38蛋白激酶不同亚型在RAW264.7细胞中的定位[J]. 南方医科大学学报，2000, 20(3): 193-196.
15	Dodeller F, Skapenko A, Kalden JP, et al. The p38 mitogen-activated protein kinase regulates effector functions of primary human CD4 T cells[J]. Eur J Immunol, 2005, 35(12): 3631-3642.

组　别	W/D(mg/mg)	BALF中总蛋白浓度(g/L)
WT control	4.11±0.18	372.82±125.49
HET control	3.89±0.28	334.38±74.95
WT＋LPS	6.17±0.30^a	863.80±100.96^a
HET＋LPS	7.13±0.25^ab	1 288.82±96.10^ab

组　别	W/D(mg/mg)	BALF中总蛋白浓度(g/L)
WT control	4.11±0.18	372.82±125.49
HET control	3.89±0.28	334.38±74.95
WT＋LPS	6.17±0.30^a	863.80±100.96^a
HET＋LPS	7.13±0.25^ab	1 288.82±96.10^ab

分　组	TNF-α(ng/L)		IL-6(ng/L)
分　组	血浆	BALF	血浆	BALF
WT control	113.42±13.40	133.17±16.95	27.27±11.15	16.11±2.28
HET control	105.98±15.64	124.52±21.76	25.38±11.10	16.04±4.37
WT＋LPS	511.34±26.50^a	207.18±20.30^a	832.52±53.97^a	314.41±32.63^a
HET＋LPS	624.67±47.60^ab	290.81±26.78^ab	1 175.18±117.28^ab	450.84±36.43^ab

分　组	TNF-α(ng/L)		IL-6(ng/L)
分　组	血浆	BALF	血浆	BALF
WT control	113.42±13.40	133.17±16.95	27.27±11.15	16.11±2.28
HET control	105.98±15.64	124.52±21.76	25.38±11.10	16.04±4.37
WT＋LPS	511.34±26.50^a	207.18±20.30^a	832.52±53.97^a	314.41±32.63^a
HET＋LPS	624.67±47.60^ab	290.81±26.78^ab	1 175.18±117.28^ab	450.84±36.43^ab

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