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摘要: 柯萨奇B3病毒 (CVB3) 是小RNA病毒科肠道病毒属的一员, 是急性和慢性病毒性心肌炎的主要致病原。虽然经过大量动物实验、人体心肌活检以及体外实验研究, 病毒性心肌炎的发病机制逐渐清晰, 但目前临床仍缺乏有效的预防手段与特异的治疗药物。近年来microRNAs (miRNAs) 成为基因水平的研究热点, 而宿主miRNAs与CVB3之间的密切关系也逐渐被科学家们发掘, 可能为病毒性心肌炎的治疗和预防提供新方向。Abstract: Coxsackievirus B3 (CVB3) is a member of the genus enterovirus within the family picornaviridae.It is an important causative agent of virus-induced acute and chronic heart disease.Although many animal experiments, myocardial biopsy and in vitro experiments have indicated the pathogenesis of viral myocarditis, there were no effective prevention and treatment strategies.In recent years, microRNAs (miRNAs) has become a hotspot in gene level research, and the close relationship between host miRNA and CVB3 has been gradually explored by scientists.It may provide new directions for the treatment and prevention of viral myocarditis.
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Key words:
- coxsackievirus B3 /
- microRNA /
- viral myocarditis
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[1] Hammond SM.MicroRNAs as oncogenes[J].Curr Opin Genet Dev, 2006, 16 (1):4-9.
[2] Bartel DP.MicroRNAs:target recognition and regulatory functions[J].Cell, 2009, 136 (2):215-33.
[3] Cullen BR.Transcription and processing of human microRNA precursors[J].Mol Cell, 2004, 16 (6):861-865.
[4] Borchert GM, Lanier W, Davidson BL.RNA polymerase Ⅲ transcribes human microRNAs[J].Mol Biol, 2006, 13 (12):1097-1101.
[5] Hutvágner G, McLachlan J, Pasquinelli AE.A cellular function for the RNA-interference enzyme Dicer in the maturation of the let-7small temporal RNA[J].Science, 2001, 293 (5531):834-838.
[6] Bernstein E, Caudy AA, Hammond SM, et al.Role for a bidentate ribonuclease in the initiation step of RNA interference[J].Nature, 2001, 409 (6818):363-366.
[7] Grishok A, Pasquinelli AE, Conte D, et al.Genes and mechanisms related to RNA interference regulate expression of the small temporal RNAs that control C.elegans developmental timing[J].Cell, 2001, 106 (1):23-34.
[8] Hammond SM, Bernstein E, Beach D, et al.An RNAdirected nuclease mediates post-transcriptional gene silencing in Drosophila cells[J].Nature, 2000, 404 (6775):293-296.
[9] Wu L, Fan J, Belasco JG.MicroRNAs direct rapid deadenylation of Mrna[J].Proc Natl Acad Sci USA, 2006, 103 (11):4034-4039.
[10] Standart N, Jackson RJ.GENES DEV.MicroRNAs repress translation of m7Gppp-capped target mRNAs in vitro by inhibiting initiation and promoting deadenylation[J].2007, 21 (16):1975-1982.
[11] Duursma AM, Kedde M, Schrier M, et al.miR-148targets human DNMT3b protein coding region[J].RNA, 2008, 14 (5):872-877.
[12] Rigoutsos I.New tricks for animal microRNAS:targeting of amino acid coding regions at conserved and nonconserved site[J].Cancer Res, 2009, 69 (8):3245-3248.
[13] Lee I, Ajay SS, Yook JI, et al.New class of microRNA targets containing simultaneous 5'-UTR and 3'-UTR interaction sites[J].Genome Res, 2009, 19 (7):1175-1183.
[14] Grey F, Tirabassi R, Meyers H, et al.A viral microRNA down-regulates multiple cell cycle genes through mRNA 5'UTRs[J].PLoS Pathog, 2010, 6 (6):e1000967.
[15] Lewis BP, Burge CB, Bartel DP.Conserved seed pairing, often flanked by adenosines, indicates that thousands of human genes are microRNA targets[J].Cell, 2005, 120 (1):15-20.
[16] Croce CM.Causes and consequences of microRNA dysregulation in cancer[J].Nat Rev Genet, 2009, 10 (10):704-714.
[17] Umbach JL, Cullen BR.The role of RNAi and microRNAs in animal virus replication and antiviral immunity[J].Genes Dev, 2009, 23 (10):1151-1164.
[18] Winter J, Jung S, Keller S, et al.Many roads to maturity:microRNA biogenesis pathways and their regulation[J].Nat Cell Biol, 2009, 11 (3):228-234.
[19] Umbach JL, Kramer MF, Jurak I, et al.MicroRNAs expressed by herpes simplex virus 1during latent infection regulate viral mRNAs[J].Nature, 2008, 454 (7205):780-783.
[20] Pfeffer S, Zavolan M, Grässer FA, et al.Identification of virus-encoded microRNAs[J].Science, 2004, 304 (5671):734-736.
[21] Gottwein E, Mukherjee N, Sachse C, et al.A viral microRNA functions as an orthologue of cellular miR-155[J].Nature, 2007, 450 (7172):1096-1099.
[22] Triboulet R, Mari B, Lin YL, et al.Suppression of microRNA-silencing pathway by HIV-1 during virus replication[J].Science, 2007, 315 (5818):1579-1582.
[23] Jopling CL, Yi M, Lancaster AM, et al.Modulation of hepatitis C virus RNA abundance by a liver-specific MicroRNA[J].Science, 2005, 309 (5740):1577-1581
[24] Wang L, Qin Y, Tong L, et al.MiR-342-5p suppress coxackievirus B3 biosynthesis by targeting the 2C-coding region[J].Antiviral Res, 2012, 93 (2):270-279.
[25] Ye X, Hemida MG, Qiu Y, et al.MiR-126promotes coxsackievirus replication by mediating cross-talk of ERK1/2 and Wnt/β-catenin signal pathways[J].Cell Mol Life Sci, 2013, 70 (23):4631-4644.
[26] Tong L, Lin L, Wu S, et al.MiR-10*up-regulates coxckievirus B3 biosynthesis by targrting the 3D-coding sequence[J].Nucleic Acids Res, 2013, 41 (6):3760-3771.
[27] Liu N, Okamura K, Tyler DM, et al.The evolution and functional diversification of animal microRNA genes[J].Cell Res, 2008, 18 (10):985-996.
[28] Corsten M, Heggermont W, Papageorgiou AP, et al.The microRNA-221/-222cluster balances the antiviral and inflammatory response in viral myocarditis[J].Eur Heart J, 2015, 36 (42):2909-2919.
[29] Bao JL, Lin L.MiR-155and miR-148areduce cardiac injury by inhibiting NF-kBpatway during acute viral myocarditis[J].Eur Rev Med Pharmacol Sci, 2014, 18 (16):2349-2356.
[30] Xu HF, Ding YJ, Shen YW, et al.MicroRNA-1represses Cx43 expression in viral myocarditis[J].Moll Cell Biochem, 2012, 362 (1-2):141-148.
[31] Miquerol L, Dupays L, Theveniau-Ruissy M, et al.Gap junctional connexins in the developing mouse cardiac conduction system[J].Novartis Found Symp, 2003, 250:80-98.
[32] Chen Y, Chen J, Wang H, et al.HCV-induced miR-21 contributes to evasion of host immune system by targeting MyD88 and IRAK1[J].PLoS Pathog, 2013, 9 (4):e1003248.
[33] Ye X, Zhang HM, Qiu Y, et al.Coxsackievirus-induced miR-21 disrupts cardiomyocyte interactions via the downregulation of intercalated disk components[J].PLoS Pathog, 2014, 10 (4):e1004070.
[34] Liu YL, Wu W, Xue Y, et al.MicroRNA-21and-146b are involved in the pathogenesis of murine viral myocarditis by regulating TH-17differentiation[J].Arch Virol, 2013, 7:158 (9):1953-1963.
[35] Xu HF, Gao XT, Lin JY, et al.MicroRNA-20bsuppresses the expression of ZFP-148in viral myocarditis[J].Mol Cell Biochem, 2017, 429 (1-2):199-210.
[36] Wang D, Li T, Cui H, et al.Analysis of the Indicating Value of Cardiac Troponin I, Tumor Necrosis Factor-α, Interleukin-18, Mir-1and Mir-146bfor Viral Myocarditis among Children[J].Cell Physiol Biochem, 2016, 40 (6):1325-1333.
[37] Chen ZG, Liu H, Zhang JB, et al.Upregulated microRNA-214enhances cardiac injury by targeting ITCH during coxsackievirus infection[J].Mol Med Rep, 2015, 12 (1):1258-6124.
[38] Zhang Y, Sun L, Sun H, et al.Overexpression of microRNA-133breduces myocardial injuries in children with viral myocarditis by targeting Rab27B gene[J].Cell Mol Biol (Noisy-le-grand), 2017, 63 (10):80-86.
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