中文English
ISSN 1001-5256 (Print)
ISSN 2097-3497 (Online)
CN 22-1108/R
Volume 36 Issue 5
May  2020
Turn off MathJax
Article Contents
Article Navigation >  Journal of Clinical Hepatology  > 2020  >  36(5): 1019-1023

Effect of T-lymphocyte phenotype on immune status in chronic hepatitis B virus infection and its application value

DOI: 10.3969/j.issn.1001-5256.2020.05.014

  • The First Clinical Medical College,Lanzhou University

Research funding:

 

  • Received Date: 2019-12-16
  • Published Date: 2020-05-20
    Abstract

  • Objective To investigate the association between T-lymphocyte phenotype and immune status in chronic hepatitis B(CHB)and its application value.Methods A total of 77 CHB patients who attended The First Hospital of Lanzhou University from January 2015 to May 2019 were enrolled, and according to the status of HBeAg and the serum levels of alanine aminotransferase(ALT), HBsAg, and HBV DNA, they were divided into immune tolerance group and non-immune tolerance group. The laboratory results of T-lymphocyte phenotype, HBV serological test, HBV DNA load, routine blood test, and liver function were obtained, and aspartate aminotransferase-to-platelet ratio index(APRI) and fibrosis-4(FIB-4) were calculated. Thettest was used for comparison of normally distributed continuous data between two groups; and the Mann-WhitneyUtest was used for comparison of non-normally distributed continuous data between two groups; the chi-square test was used for comparison of categorical data between groups. Spearman correlation analysis was used to test the correlation effect between the two variables. The diagnostic efficacy of Treg, CD8+PD-1+T lymphocyte percentage and CD8+CD45 RO+T lymphocyte percentage were evaluated by AUC.Results Compared with the non-immune tolerance group, the immune tolerance group had significantly higher percentages of Treg and CD8+PD-1+T cells(U= 12. 0 and 59. 0,P< 0. 001,P= 0 013) and significantly lower percentages of CD3+CD8+T cells and CD8+CD45 RO+T cells(U= 50. 0 and 38. 5, bothP< 0. 05). Compared with the high HBV DNA load group, the low HBV DNA load group had significantly lower percentages of Treg and CD8+PD-1+T cells(U= 178 5 and 255.0,P= 0. 003 and 0. 018) and significantly higher percentages of CD3+T cells and CD8+CD45 RO+T cells(U= 104. 0 and1495,P= 0. 033 and 0. 025). APRI was negatively correlated with the percentage of Treg(r=-0. 379,P= 0. 013), and FIB-4 was negatively correlated with the percentages of CD3+CD4+, CD3+CD8+, CD4+CD45 RO+, and CD8+CD45 RO+T cells(r=-0. 259,-0. 275,-0. 233, and-0. 229,P= 0. 023, 0. 016, 0. 041, and 0. 045). Treg, CD8+PD-1+T cells, and CD8+CD45 RO+T cellshad an area under the ROC curve of 0. 793(95% confidence interval [CI]: 0. 651-0. 936), 0. 802(95% CI: 0. 678-0. 927), and0. 816(95% CI: 0. 706-0. 927), respectively, in evaluating immune status.Conclusion There are various T-lymphocyte phenotypesin patients with chronic HBV infection, and different T lymphocytes have different abilities to eliminate HBV. Detection of T-lymphocytephenotype helps to understand the immune status and adjust the immune function in CHB patients and can provide a reference for the func-tional cure of CHB patients.

     

    • FullText(HTML)
  • loading
    • References(16)
  • [1] GEHRING AJ, PROTZER U. Targeting innate and adaptive immune responses to cure chronic HBV infection[J]. Gastroenterology, 2019, 156(2):325-337.
    [2] PROTZER U, MAINI MK, KNOLLE PA. Living in the liver:Hepatic infections[J]. Nat Rev Immunol, 2012, 12(3):201-213.
    [3] MUELLER SN, AHMED R. High antigen levels are the cause of T cell exhaustion during chronic viral infection[J]. Proc Natl Acad Sci U S A, 2009, 106(21):8623-8628.
    [4] UTZSCHNEIDER DT, ALFEI F, ROELLI P, et al. High antigen levels induce an exhausted phenotype in a chronic infection without impairing T cell expansion and survival[J]. J Exp Med, 2016, 213(9):1819-1834.
    [5] KENNEDY P, SANDALOVA E, JO J, et al. Preserved T-cell function in children and young adults with immune-tolerant chronic hepatitis B[J]. Gastroenterology, 2012, 143(3):637-645.
    [6] Chinese Society of Infectious Diseases, Chinese Medical Association; Chinese Society of Hepatology, Chinese Medical Association. Guidelines for the prevention and treatment of chronic hepatitis B(version 2019)[J]. J Clin Hepatol, 2019,35(12):2648-2669.(in Chinese)中华医学会感染病学分会,中华医学会肝病学分会.慢性乙型肝炎防治指南(2019年版)[J].临床肝胆病杂志,2019, 35(12):2648-2669.
    [7] LANG J, NEUMANN-HAEFELIN C, THIMME R. Immunological cure of HBV infection[J]. Hepatol Int, 2019, 13(2):113-124.
    [8] RAO PE, PETRONE AL, PONATH PD. Differentiation and expansion of T cells with regulatory function from human peripheral lymphocytes by stimulation in the presence of TGF-{beta}[J]. J Immunol, 2005, 174(3):1446-1455.
    [9] WANG X, DONG Q, LI Q, et al. Dysregulated response of follicular helper T cells to hepatitis B surface antigen promotes HBV persistence in mice and associates with outcomes of patients[J]. Gastroenterology, 2018, 154(8):2222-2236.
    [10] ASABE S, WIELAND SF, CHATTOPADHYAY PK, et al. The size of the viral inoculum contributes to the outcome of hepatitis B virus infection[J]. J Virol, 2009, 83(19):9652-9662.
    [11] THIMME R, WIELAND S, STEIGER C, et al. CD8(+)T cells mediate viral clearance and disease pathogenesis during acute hepatitis B virus infection[J]. J Virol, 2003, 77(1):68-76.
    [12] XIE DY, CHEN FJ, LIN BL, et al. The expressions of PD-1and PD-L1 and the correlation with the degree of liver damage in HBV chronic infection[J/CD]. Chin J Exp Clin Infect Dis(Electronic Version), 2010, 4(3):31-34.(in Chinese)谢冬英,陈凤娟,林炳亮,等.PD-1和PD-L1表达与慢性HBV感染者肝脏病变程度的相关性[J/CD].中华实验和临床感染病杂志(电子版),2010, 4(3):31-34.
    [13] ZHAO HZ, QI QG, LIU RJ, et al. The relationship among programmed death receptor 1 expression of peripheral blood T lymphocytes, hepatitis B virus DNA load and alanine aminotransferase level in chronic hepatitis B patients under different immune status[J/CD]. Chin J Exp Clin Infect Dis(Electronic Edition), 2018,12(6):585-589.(in Chinese)赵海珍,其其格,刘瑞军,等.慢性乙型肝炎患者不同免疫状态下外周血T淋巴细胞程序性死亡受体1表达与乙型肝炎病毒DNA载量及丙氨酸氨基转移酶水平的相关性[J/CD].中华实验和临床感染病杂志(电子版),2018,12(6):585-589.
    [14] HOOGEVEEN RC, ROBIDOUX MP, SCHWARZ T, et al. Phenotype and function of HBV-specific T cells is determined by the targeted epitope in addition to the stage of infection[J].Gut, 2019, 68(5):893-904.
    [15] KAH J, KOH S, VOLZ T, et al. Lymphocytes transiently expressing virus-specific T cell receptors reduce hepatitis B virus infection[J]. J Clin Invest, 2017, 127(8):3177-3188.
    [16] PALEY MA, KROY DC, ODORIZZI PM, et al. Progenitor and terminal subsets of CD8+T cells cooperate to contain chronic viral infection[J]. Science, 2012, 338(6111):1220-1225.
    • Relative Articles
    • Supplements(0)
    • Cited By
  • 加载中

Catalog

    通讯作者: 陈斌, bchen63@163.com
    • 1. 

      沈阳化工大学材料科学与工程学院 沈阳 110142

    1. 本站搜索
    2. 百度学术搜索
    3. 万方数据库搜索
    4. CNKI搜索
    Get Citation
    PDF
    XML

    Article Metrics

    Article views (783) PDF downloads(143) Cited by()
    Proportional views
    Related
        

    The first journal specializing in hepatobiliary and pancreatic diseases in China

    Supervisor:Ministry of Education of the People's Republic of China

    Sponsor:Jilin University

    Academic Support: Chinese Society of Hepatology,Chinese Medical Association

    Address: 461 Xinjiang Road, Changchun

    Submit:0431-88782044

    Peer review:0431-88783542

    Email:lcgdb@vip.163.com

    About Journal

    Submission Guideline

    Journal Online

    Hepatobiliary College

    Guidelines

    YesterdayIP[]YesterdayPV[]TodayIP[]TodayPV[]Online[]

    Website Design © 2020 Editorial Board of Journal of Clinical Hepatology 吉ICP备10000617号-1 Supported by: Beijing Renhe Information Technology Co. Ltd  

    /

    DownLoad:  Full-Size Img  PowerPoint
    Return
    Return