SIRT3通过调节FoxO3a的去乙酰化抑制焦亡,减轻脓毒症诱导的急性肺损伤

IF 3.3 3区 医学 Q2 PHARMACOLOGY & PHARMACY
Zheqian Wu , Yong Wang , Shijie Lu, Lili Yin, Lihua Dai
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引用次数: 0

摘要

本研究主要分析SIRT3通过调节FoxO3a的脱乙酰化和抑制pyroptosis来减轻败血症诱导的急性肺损伤(ALI)的机制。方法采用SIRT3过表达和沉默的BEAS-2B细胞,观察SIRT3对LPS处理的肺上皮细胞凋亡的影响。FoxO3a沉默的BEAS-2B细胞也用于验证SIRT3在ALI体外抑制氧化应激和焦下垂的机制。3-TYP在体内抑制SIRT3的脱乙酰功能。通过检测GSDMD-N和LDH流出来评估Pyroposis。结果CLP诱导的ALI小鼠GSDMD-N和LDH水平升高,诱发pyroptosis。SIRT3的沉默加剧了氧化应激、NLRP3活化和焦下垂,并抑制了FoxO3a的脱乙酰化。SIRT3的过表达减弱了pyroptosis,诱导了脱乙酰化,并恢复了FoxO3a和MnSOD的表达。沉默的FoxO3a加重了焦下垂。SIRT3的过表达恢复了FoxO3a表达的降低并抑制了pyroptosis。3-TYP阻断SIRT3对FoxO3a的促进作用和SIRT3对pyroptosis的抑制作用。结论脓毒症SIRT3的降低导致FoxO3a的高乙酰化,进而加剧氧化应激并诱导ALI的pyroptosis。提高SIRT3水平可通过脱乙酰作用促进FoxO3a,从而抑制pyroptosis和缓解ALI。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
SIRT3 alleviates sepsis-induced acute lung injury by inhibiting pyroptosis via regulating the deacetylation of FoxO3a

Objective

This study mainly analyzes the mechanism of SIRT3 alleviating sepsis-induced acute lung injury (ALI) by regulating the deacetylation of FoxO3a and inhibiting pyroptosis.

Methods

SIRT3-overexpressing and silenced BEAS-2B cells were used to evaluate the effect of SIRT3 on apoptosis in LPS-treated lung epithelial cells. FoxO3a-silenced BEAS-2B cells were also used to verify the mechanism by which SIRT3 inhibited oxidative stress and pyroptosis in vitro in ALI. 3-TYP was used to inhibit the deacetylation function of SIRT3 in vivo. Pyroptosis was assessed by detecting GSDMD-N and LDH efflux.

Results

In CLP-induced ALI mice, GSDMD-N and LDH levels were elevated, pyroptosis was induced. Silencing of SIRT3 exacerbated oxidative stress, NLRP3 activation and pyroptosis, and inhibited the deacetylation of FoxO3a. Overexpression of SIRT3 attenuated pyroptosis, induced deacetylation and restored the expression of FoxO3a and MnSOD. Silencing FoxO3a aggravated pyroptosis. Overexpression of SIRT3 restored the reduced FoxO3a expression and suppressed pyroptosis. 3-TYP blocked the promotion of FoxO3a by SIRT3 and the inhibitory effect of SIRT3 on pyroptosis.

Conclusion

The reduction of SIRT3 in sepsis caused hyperacetylation of FoxO3a, which in turn exacerbates oxidative stress and induces pyroptosis of ALI. Increasing the level of SIRT3 promotes FoxO3a through deacetylation, thereby inhibiting pyroptosis and relieving ALI.

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来源期刊
CiteScore
6.20
自引率
0.00%
发文量
41
审稿时长
42 days
期刊介绍: Pulmonary Pharmacology and Therapeutics (formerly Pulmonary Pharmacology) is concerned with lung pharmacology from molecular to clinical aspects. The subject matter encompasses the major diseases of the lung including asthma, cystic fibrosis, pulmonary circulation, ARDS, carcinoma, bronchitis, emphysema and drug delivery. Laboratory and clinical research on man and animals will be considered including studies related to chemotherapy of cancer, tuberculosis and infection. In addition to original research papers the journal will include review articles and book reviews. Research Areas Include: • All major diseases of the lung • Physiology • Pathology • Drug delivery • Metabolism • Pulmonary Toxicology.
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