长链非编码RNA在脓毒症肺损伤中作用的研究进展

详细信息    查看全文 | 推荐本文 |

	作者：戴巍 ; 胡世林 ; 钱克俭 关键词：急性呼吸窘迫综合征 ; 肺损伤 ; 长链非编码RNA ; 脓毒症 中文刊名：JXYY 英文刊名：Jiangxi Medical Journal 机构：南昌大学第一附属医院重症医学科;江西省上饶市第五人民医院; 出版日期：2019-04-20 出版单位：江西医药 年：2019 期：v.54 基金：国家自然科学基金项目,编号81560306 语种：中文; 页：JXYY201904045 页数：3 CN：04 ISSN：36-1094/R 分类号：136-138

摘要

长链非编码RNA(LncRNA)的生物功能多种多样,在转录的招募、表达、转录后修饰及表观遗传等过程中调控特异性基因的表达,广泛参与机体各种生理和病理过程。脓毒症是一种以器官功能障碍和对感染的异常免疫反应为特征的综合征。脓毒症引起的急性肺损伤/急性呼吸窘迫综合征(ALI/ARDS)发病率和死亡率较高。发生于肺部感染或肺外感染后,宿主对感染的异常反应导致肺泡毛细血管屏障破裂,导致肺损伤,表现为低氧血症、炎症和非心源性肺水肿。目前ALI/ARDS的发病机制尚不清楚,缺乏特异性的治疗方法。本文综述lncRNA在调控巨噬细胞、上皮细胞、内皮细胞、成纤维细胞等方面的研究进展,以期为lncRNA在脓毒症肺损伤的研究提供参考。
        

引文

[1]Singer M,Deutschman CS,Seymour CW,et al. The Third International Consensus Definitions for Sepsis and Septic Shock(Sepsis-3)[J]. J the American Medical Association,2016,315(8):801.
    [2]Bellani G,Laffey JG,Pham T,et al. Epidemiology,Patterns of Care,and Mortality for Patients With Acute Respiratory Distress Syndrome in Intensive Care Units in 50 Countries[J]. JAMA,2016,315(8):788.
    [3]Calfee CS,Janz DR,Bernard GR,et al. Distinct molecular phenotypes of direct vs indirect ARDS in single-center and multicenter studies[J]. Chest,2015,147(6):1539-1548.
    [4]Chen ZJMM. Progress and prospects of long noncoding RNAs in lipid homeostasis[J]. Molecular Metabolism,2016,5(3):164-170.
    [5]王俊,周凯.长链非编码RNA在结直肠癌中的研究进展[J].江西医药,2014,49(10):1118-1120.
    [6]Cui H,Banerjee S,Guo S,et al. Long noncoding RNA Malat1regulates differential activation of macrophage and response to lung injury[J]. JCI Insight,2019,4(4):e124522.
    [7]Dai L,Zhang G,Cheng Z,et al. Knockdown of LncRNA MALAT1contributes to the suppression of inflammatory responses by upregulating miR-146a in LPS-induced acute lung injury[J].Connect Tissue Res,2018,59(6):581-592.
    [8]Jia Y,Li Z,Cai W,et al. SIRT1 regulates inflammation response of macrophages in sepsis mediated by long noncoding RNA[J].Biochim Biophys Acta Mol Basis Dis,2018,1864(3):784-792.
    [9]Scacalossi KR,van Solingen C,Moore KJ. Long non-coding RNAs regulating macrophage functions in homeostasis and disease[J].Vascul Pharmacol,2019,114:122-130.
    [10]Zhang D,Lee H,Haspel JA,et al. Long noncoding RNA FOXD3-AS1 regulates oxidative stress-induced apoptosis via sponging microRNA-150[J]. Faseb J,2017,31(10):4472-4481.
    [11]Li H,Shi H,Gao M,et al. Long non-coding RNA CASC2improved acute lung injury by regulating miR-144-3p/AQP1 axis to reduce lung epithelial cell apoptosis[J]. Cell Biosci,2018,8:15.
    [12]Liu M,Han T,Shi S,et al. Long noncoding RNA HAGLROS regulates cell apoptosis and autophagy in lipopolysaccharidesinduced WI-38cells via modulating miR-100/NF-kappaB axis[J].Biochem Biophys Res Commun,2018,500(3):589-596.
    [13]Li H,Shi H,Ma N,et al. BML-111 alleviates acute lung injury through regulating the expression of lncRNA MALAT1[J]. Arch Biochem Biophys,2018,649:15-21.
    [14]Wang D,Gu C,Liu M,et al. Analysis of Long Noncoding RNA Expression Profile in Human Pulmonary Microvascular Endothelial Cells Exposed to Lipopolysaccharide[J]. Cell Physiol Biochem,2019,52(4):653-667.
    [15]Rapicavoli NA,Qu K,Zhang J,et al. A mammalian pseudogene lncRNA at the interface of inflammation and anti-inflammatory therapeutics[J]. Elife,2013,2:e00762.
    [16]Zhou Z,Zhu Y,Gao G,et al. Long noncoding RNA SNHG16targets miR-146a-5p/CCL5 to regulate LPS-induced WI-38 cell apoptosis and inflammation in acute pneumonia[J]. Life Sci,2019,228:189-197.
    [17]Hu G,Tang Q,Sharma S,et al. Expression and regulation of intergenic long noncoding RNAs during T cell development and differentiation[J]. Nat Immunol,2013,14(11):1190-1198.
    [18]蒋光辉,刘素芸,陶文强,等. SP-D、KL-6评价呼吸机相关性肺损伤的初步研究[J].江西医药,2017,52(12):1268-1270,1288.
    [19]Wang L,Zhang N,Zhang Y,et al. Landscape of transcription and long non-coding RNAs reveals new insights into the inflammatory and fibrotic response following ventilator-induced lung injury[J].Respir Res,2018,19(1):122.