The level of expression of miR-196a in patients with chronic viral hepatitis C with the first genotype of HCV according to previous experience of antiviral therapy.

Authors

DOI:

https://doi.org/10.26641/2307-0404.2020.2.206387

Keywords:

chronic viral hepatitis C, miR-196a, hsa-miRNA-196a, antiviral therapy

Abstract

The authors present the study of the level of expression of miR-196a in 74 patients with chronic viral hepatitis C with the 1st genotype of HCV, based on previous experience in patients with antiviral therapy regimens containing interferon. The patients were divided into two groups, depending on the previous experience of antiviral therapy with circuits containing interferon – 21 patients who failed after antiviral therapy regimens containing interferon (group 1) and the comparison group (group 2) – 53 naive patients. To study the level of expression of miR-196a (miR-196a), a two-stage study according to the manufacturer's protocol was used. First, total RNA was isolated from the plasma by the method of phenol-chloroform extraction. Futher reverse transcription was performed using a kit for reverse transcription of miR TaqMan® (Applied Biosystems, USA), specific loop primers to achieve mature miRNA, snRNA U6 (as an endogenous control gene), and 10 ng of total RNA. Real-time quantitative PCR was performed using TaqMan® miRNA analysis. In order to optimize the prediction of response to antiviral therapy and the use of optimal treatment regimens for problem patients with treatment failure regimens containing interferon, analysis using ROC curves was used. The average level of expression of miR-196a in patients with chronic hepatitis C was evaluated. In the 1st group of patients it was 0.011 (IQR: 0.002; 0.310) and in the comparison group – 0.346 (IQR: 0.054; 1.239) at p=0.012 by U criterion. The conducted ROC analysis showed that the studied miR-196a could differentiate patients with chronic viral hepatitis C with HCV genotype 1, depending on previous experience of antiviral therapy, namely, patients with treatment failure regimens containing interferons and naive. AUC=0.688 (95% CI 0.570-0.791; p=0.017), J=0.40, Se=57.14%, Sp=83.02%. It gives additional opportunities for correction of therapeutic tactics. Therefore, the level of expression of miR-196a (<-1,75) may be an additional biomarker in the pathogenesis of HCV-infection, which can then be used in the monitoring and treatment of patients. Low expression of miR-196a may be the basis for prescribing more effective direct-acting antiviral therapy to patients and will allow personalizing therapeutic tactics in patients with chronic viral hepatitis C.

Author Biographies

L. R. Shostakovych-Koretskaya

SE «Dnipropetrovsk medical academy of Health Ministry of Ukraine» ¹
Department of Infectious Diseases

O. P. Shevchenko-Makarenko

SE «Dnipropetrovsk medical academy of Health Ministry of Ukraine» ¹
Department of Infectious Diseases

T. Yu. Lapikova-Bryhinska

Bogomoletz Institute of Physiology, National Academy of Sciences of Ukraine 

References

Anoxina IY. [Development of a scoring model using the methods of logistic regression and ROC analysis]. Informatika i kibernetika. 2016;3(5):13-21. Russian.

Shevchenko-Makarenko OP, Shostakovych-Ko­retska LR, Velychko SO, Shtepa OP, Rezvykh VH. [The incidence of chronic hepatitis C in the structure of other chronic viral hepatitis in the Dnipropetrovsk region and Ukraine]. Visnyk naukovykh doslidzhen – Bulletin of scientific researches. 2018;1:156-60. Ukrainian. doi: https://doi.org/10.11603/2415-8798.2018.1.8791

Shostakovych-Koretskaya LR, Shevchenko-Ma­karenko OP, Lapikova-Bryhinska TYu. [Basic level of miR-196a expression in patients with chronic viral hepatitis C, 1 genotype]. Gepatologia. 2019;2(44):35-44. Ukrainian. Available from: http://nbuv.gov.ua/node/554

Chiraz Atri, Fatma Z. Guerfali, Dhafer Laouini, MicroRNAs in diagnosis and therapeutics. AGO-Driven Non-Coding RNAs. Chapter 6. 2019:137-77. doi: https://doi.org/10.1016/b978-0-12-815669-8.00006-3

Conrad KD, Niepmann M. The role of mic­roRNAs in hepatitis C virus RNA replication. Arch Virol. May 2014;159(5):849-862. doi: https://doi.org/10.1007/s00705-013-1883-4

Scagnolari C, Zingariello P, Vecchiet J, Selvaggi C, Racciatti D, Taliani G et al. Differential expression of interferon-induced microRNAs in patients with chronic hepatitis C virus infection treated with pegylated inter­feron alpha. Virol J. 2010 Nov 12;7:311. PubMed PMID: 21070682; PubMed Central PMCID: PMC2996368. doi: https://doi.org/10.1186/1743-422X-7-311

Guidelines for the care and treatment of persons diagnosed with chronic hepatitis C virus infection. WHO July 2018:108. Available from: https://www.who.int/en/

Kozomara A, Birgaoanu M, Griffiths-Jones S. miRBase: from microRNA sequences to function, Nucleic Acids Research. 2019;47:D155-62, doi: https://doi.org/10.1093/nar/gky1141

Kwon YC, Ray RB, Ray R. Hepatitis C virus in­fection: establishment of chronicity and liver disease progression. EXCLI journal. 2014;13:977.

Ree MH, Meer AJ, Nuenen AC. Bruijne J. Ottosen S. Janssen HL et all. Miravirsen dosing in chronic hepatitis C patients results in decreased microRNA‐122 levels without affecting other microRNAs in plasma. Aliment Pharmacol Ther. 2016;43:102-13. doi: https://doi.org/10.1111/apt.13432

Musaddaq G, Shahzad N, Ashraf MA, Ar­shad MI. Circulating liver-specific microRNAs as noninvasive diagnostic biomarkers of hepatic diseases in human. Biomarkers. 2019 Mar;24(2):103-109. Epub 2018 Oct 23. PMID: 30252499. doi: https://doi.org/10.1080/1354750X.2018.1528631

El-Guendy NM, Helwa R, El-Halawany MS, Ab­del Rahman Ali S, Tantawy Aly M, Hasan Alieldin N, et al. The Liver MicroRNA Expression Profiles Associated With Chronic Hepatitis C Virus (HCV) Genotype-4 Infection: A Preliminary Study. Hepatitis monthly. 2016;16(4):e33881. doi: https://doi.org/10.5812/hepatmon.3388. PMCID: PMC4893413

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Shostakovych-Koretskaya LR, Shevchenko-Makarenko OP, Lapikova-Bryhinska TY. The level of expression of miR-196a in patients with chronic viral hepatitis C with the first genotype of HCV according to previous experience of antiviral therapy. Med. perspekt. [Internet]. 2020Jul.1 [cited 2024Dec.23];25(2):130-7. Available from: https://journals.uran.ua/index.php/2307-0404/article/view/206387

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CLINICAL MEDICINE