热休克蛋白A12A改善内毒素血症肺损伤的实验研究

doi:10.3969/j.issn.1003-9198.2021.08.004

实用老年医学 ›› 2021, Vol. 35 ›› Issue (8): 803-806.doi: 10.3969/j.issn.1003-9198.2021.08.004

热休克蛋白A12A改善内毒素血症肺损伤的实验研究

戴媛, 刘嘉莉, 闵新栩, 李蕴凡, 毛芊, 丁正年

210029 江苏省南京市,南京医科大学第一附属医院麻醉科

收稿日期:2020-11-20 出版日期:2021-08-20 发布日期:2021-08-30
通讯作者: 丁正年,Email:zhengnianding@njmu.edu.cn
基金资助:
国家自然科学基金资助项目(81970692)

Heat shock protein A12A is necessary for pulmonary protection during endotoxemia

DAI Yuan, LIU Jia-li, MIN Xin-xu, LI Yun-fan, MAO Qian, DING Zheng-nian

Department of Anesthesiology, the First Affiliated Hospital of Nanjing Medical University, Nanjing 210029, China

Received:2020-11-20 Online:2021-08-20 Published:2021-08-30

摘要/Abstract

摘要： 目的研究热休克蛋白(HSP)A12A 在细菌脂多糖(LPS)诱导的内毒素血症肺损伤中的作用。方法采用8～10周龄的HSPA12A基因敲除鼠(Hspa12a^-/-)和野生型对照鼠(WT)进行实验,分别对小鼠腹腔注射LPS诱导内毒素血症,或腹腔注射生理盐水(NS)作为对照组,根据小鼠类型及处理方式将小鼠分为4组:NS-WT组、NS-Hspa12a^-/-组、LPS-WT组、LPS-Hspa12a^-/-组。腹腔注射6 h后取肺组织,检测肺组织中蛋白表达水平并制作肺组织石蜡切片;收集动脉血液用于动脉血气分析。通过免疫印迹检测蛋白表达水平;对肺组织石蜡切片行HE染色,评价肺组织的病理学变化得到肺损伤评分;通过血气分析评估肺功能。结果 LPS处理后, HSPA12A在LPS-WT组小鼠肺组织中的表达水平是NS-WT组的1.5倍 (P<0.05);LPS处理后,小鼠的肺组织出现了明显的病理变化,并且与WT鼠相比,HSPA12A基因敲除小鼠肺组织病理改变加重,肺损伤评分显著升高(P<0.01);与WT鼠相比,HSPA12A基因敲除小鼠动脉血中CO₂蓄积明显增加(P<0.05)。结论 HSPA12A在保护脓毒症/感染性休克肺损伤中具有重要作用。

关键词: 热休克蛋白A12A, 内毒素血症, 肺损伤

Abstract: Objective To investigate the effects of heat shock protein A12A (HSPA12A) on lung injury during endotoxemia. Methods HSPA12A knockout mice (Hspa12a^-/-) and wild type littermates (WT) mice aged 8-10 weeks were enrolled in this study. The mice were injected with lipopolysaccharide (LPS) intraperitoneally to induce endotoxemia, while normal saline (NS)-treated mice served as the controls. According to the type of mice and treatment mode, the mice were divided into NS-WT group, NS-Hspa12a^-/- group, LPS-WT group and LPS-Hspa12a^-/- group. Six hours after LPS or NS treatment, the lung tissues were harvested for the detection of protein levels and paraffin sections. The arterial blood was collected for arterial blood gas analysis. Protein expression levels were detected by immunoblotting. Pulmonary injury scores were obtained according to the histopathological changes of the lung tissues by H&E staining, and the pulmonary function was evaluated by blood gas analysis. Results The expression level of HSPA12A in the lungs of LPS-treated mice was 150% of that in NS-treated mice (P<0.05). After LPS treatment, the lung tissues showed obvious pathological changes, and Hspa12a^-/- mice showed severer pulmonary histological abnormalities and higher injury scores than those in WT mice (P<0.01). Hspa12a^-/- mice showed increased CO₂ accumulation in arterial blood than WT mice during endotoxemia (P<0.05). Conclusions HSPA12A plays an important role in the protection against sepsis/septic shock-induced lung injury.

Key words: heat shock protern A12A, endotoxemia, lung injury

中图分类号:

R 563

戴媛, 刘嘉莉, 闵新栩, 李蕴凡, 毛芊, 丁正年. 热休克蛋白A12A改善内毒素血症肺损伤的实验研究[J]. 实用老年医学, 2021, 35(8): 803-806.

DAI Yuan, LIU Jia-li, MIN Xin-xu, LI Yun-fan, MAO Qian, DING Zheng-nian. Heat shock protein A12A is necessary for pulmonary protection during endotoxemia[J]. Practical Geriatrics, 2021, 35(8): 803-806.

参考文献

[1] LIU Z, MAHALE P, ENGELS E A. Sepsis and risk of cancer among elderly adults in the united states[J]. Clin Infect Dis, 2019, 68(5): 717-724.
[2] SHAH D, DAS P, ACHARYA S, et al. Small immunomodulatory molecules as potential therapeutics in experimental murine models of acute lung injury (ALI)/acute respiratory distress syndrome (ARDS)[J]. Int J Mol Sci, 2021,22(5):2573.
[3] VILLAR J, BLANCO J, KACMAREK R M. Current incidence and outcome of the acute respiratory distress syndrome[J]. Curr Opin Crit Care, 2016, 22(1): 1-6.
[4] VOS M J, HAGEMAN J, CARRA S, et al. Structural and functional diversities between members of the human HSPB, HSPH, HSPA, and DNAJ chaperone families[J]. Biochemistry, 2008, 47(27):7001-7011.
[5] YOMBO D, MENTINK-KANE M, WILSON M, et al. Heat shock protein 70 is a positive regulator of airway inflammation and goblet cell hyperplasia in a mouse model of allergic airway inflammation[J]. J Biol Chem, 2019, 294(41):15082-15094.
[6] CHATTERJEE A, SNEAD C, YETIK-ANACAK G, et al. Heat shock protein 90 inhibitors attenuate LPS-induced endothelial hyperpermeability[J]. Am J Physiol Lung Cell Mol Physiol, 2008, 294(4): L755-L763.
[7] MIN X, ZHANG X, LI Y, et al. HSPA12A unstabilizes CD147 to inhibit lactate export and migration in human renal cell carcinoma[J]. Theranostics, 2020, 10(19): 8573-8590.
[8] ZHANG X, CHEN X, QI T, et al. HSPA12A is required for adipocyte differentiation and diet-induced obesity through a positive feedback regulation with PPARgamma[J]. Cell Death Differ, 2019, 26(11): 2253-2267.
[9] MAO Y, KONG Q, LI R, et al. Heat shock protein A12A encodes a novel prosurvival pathway during ischaemic stroke[J]. Biochim Biophys Acta Mol Basis Dis, 2018, 1864(5 Pt A): 1862-1872.
[10] MATUTE-BELLO G, DOWNEY G, MOORE B B, et al. An official American Thoracic Society workshop report: features and measurements of experimental acute lung injury in animals[J]. Am J Respir Cell Mol Biol, 2011, 44(5): 725-738.
[11] KAWASAKI T, CHEN W, HTWE Y M, et al. DPP4 inhibition by sitagliptin attenuates LPS-induced lung injury in mice[J]. Am J Physiol Lung Cell Mol Physiol, 2018, 315(5): L834-L845.
[12] MATTHAY M A, ZEMANS R L, ZIMMERMAN G A, et al. Acute respiratory distress syndrome[J]. Nat Rev Dis Primers, 2019, 5(1): 18.
[13] PFALZGRAFF A, WEINDL G. Intracellular lipopolysaccharide sensing as a potential therapeutic target for sepsis[J]. Trends Pharmacol Sci, 2019, 40(3): 187-197.
[14] WU J, LI X, HUANG L, et al. HSPA12B inhibits lipopolysaccharide-induced inflammatory response in human umbilical vein endothelial cells[J]. J Cell Mol Med, 2015, 19(3): 544-554.

热休克蛋白A12A改善内毒素血症肺损伤的实验研究

Heat shock protein A12A is necessary for pulmonary protection during endotoxemia

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