Th9细胞及其细胞因子对于乙型肝炎肝纤维化程度的诊断效能

摘要/Abstract

摘要： 目的探讨Th9细胞及相关细胞因子IL-9联合多指标对不同程度乙型肝炎肝纤维化患者的诊断效能。方法选取东部战区总医院秦淮医疗区收治的HBV感染者207例,按病理检查结果分为无纤维化组31例、轻中度纤维化组77例及重度纤维化组99例。采用流式细胞术检测外周血Th9细胞水平,ELISA法检测IL-9水平,并计算FIB-4、APRI、AAR、RPR。通过Spearman相关性分析各指标与乙型肝炎肝纤维化程度的相关性;绘制受试者工作特征曲线评价其诊断效能。结果无纤维化组、轻中度纤维化组、重度纤维化组FIB-4分别为4.52(2.48,7.99)、4.71(3.33,6.63)、13.09(6.64,19.43),APRI分别为1.29(0.64,2.11)、1.39(0.75,1.87)、2.83(1.23,5.55),AAR分别为1.29(0.90,1.70)、1.35(0.94,1.83)、1.74(1.34,2.32),RPR分别为0.13(0.08,0.23)、0.14(0.11,0.21)、0.28(0.20,0.45),IL-9分别为24.97±3.615、34.553±5.708、43.684±6.534及Th9细胞水平分别为0.28±0.085、0.464±0.103、0.626±0.098,差异均有统计学意义(均P<0.05)。FIB-4、APRI、AAR、RPR、IL-9及Th9细胞水平与肝纤维化分期均呈正相关(r= 0.740、0.581、0.379、0.714、0.396、0.421,P<0.01)。FIB-4、APRI、AAR、RPR、IL-9及Th9对轻中度/重度乙型肝炎肝纤维化的诊断效能均较好,AUC分别为0.878/0.831、0.772/0.745、0.614/0.678、0.862/0.818、0.685/0.588、0.633/0.578。联合各变量可以提高对乙型肝炎肝纤维化的诊断效能,AUC分别为IL-9+Th9:0.774/0.668、IL-9+Th9+FIB-4:0.934/0.862、IL-9+Th9+RPR:0.929/0.818、IL-9+Th9+FIB-4+RPR:0.943/0.848。结论 FIB-4、APRI、AAR、RPR、IL-9及Th9细胞水平对乙型肝炎所致肝纤维化均有较好的诊断效能,联合诊断的效能更优,且均与肝纤维化分期呈明显正相关。

关键词: 乙型肝炎病毒, 辅助性T细胞9, 白细胞介素-9, 肝纤维化

Abstract: Objective To investigate the diagnostic efficacy of Th9 cells and related cytokine IL-9 in combination with multiple indicators for patients with different degrees of liver fibrosis caused by hepatitis B. Methods Two hundred and seven patients with hepatitis B viral infection were selected. They were divided into non-fibrosis group, mild to moderate fibrosis group and severe fibrosis group according to their pathological examination results. The level of Th9 cells in peripheral blood of each patient was detected by flow cytometry. The level of IL-9 was detected by enzyme linked immunosorbent assay (ELISA). The values of FIB-4 (fibrosis index based on the four factors), APRI (aspartate aminotransferase-to-platelet ratio index), AAR (aspartate aminotransferase/alanine aminotransferase ratio) and RPR (red cell distribution width-to-platelet ratio) were calculated. Spearman correlation analysis was used to explore the correlation between each index and the degree of liver fibrosis. Receiver operating characteristic curves (ROC) were drawn and the diagnostic efficiencies of each and the combination of variables were evaluated. Results There were significant differences in the levels of FIB-4 [4.52(2.48~7.99), 4.71(3.33~6.63), 13.09(6.64~19.43)], APRI [1.29(0.64~2.11), 1.39(0.75~1.87), 2.83(1.23~5.55), AAR [1.29(0.90~1.70), 1.35(0.94~1.83), 1.74(1.34~2.32)], RPR [0.13(0.08~0.23), 0.14(0.11~0.21), 0.28(0.20~0.45)]; IL-9 [24.97±3.615, 34.553±5.708, 43.684±6.534] and Th9 cells [0.28±0.085, 0.464±0.103, 0.626±0.098] among the three groups, respectively (P<0.05). The levels of FIB-4, APRI, AAR, RPR, IL-9 and Th9 cells were positively correlated with the stage of liver fibrosis (r=0.740/0.581/0.379/0.714/0.396/0.421, P<0.01); FIB-4, APRI, AAR, RPR, IL-9 and Th9 have better diagnostic efficacy for mild to moderate fibrostic patients and severe fibrostic patients caused by hepatitis B (AUC:0.878/0.831, 0.772/0.745, 0.614/0.678, 0.862/0.818, 0.685/0.588, 0.633/0.578, respectively). The Combination of various variables can improve the diagnostic efficacies for liver fibrosis caused by hepatitis B (AUC: IL-9+Th9, 0.774/0.668; IL-9+Th9+FIB-4, 0.934/0.862; IL-9+Th9+RPR, 0.929/0.818; IL-9+Th9+FIB-4+RPR, 0.943/0.848). Conclusion FIB-4, APRI, AAR, RPR, IL-9 and Th9 cells have better diagnostic efficacies for liver fibrosis caused by hepatitis B, and the diagnostic efficacies of their combinations are better. They were significantly and positively correlated with the stages of liver fibrosis.

Key words: HBV, Th9, IL-9, Hepatic fibrosis, FIB-4, APRI, AAR, RPR

王兰, 邱红, 朱月蓉, 顾畅, 张薇薇, 杨帆. Th9细胞及其细胞因子对于乙型肝炎肝纤维化程度的诊断效能[J]. 肝脏, 2023, 28(4): 440-444.

WANG Lan, QIU Hong, ZHU Yue-rong, GU Chang, ZHANG Wei-wei, YANG Fan. The diagnostic efficacy of Th9 cells and their cytokines for the degree of hepatitis B-related liver fibrosis[J]. Chinese Hepatolgy, 2023, 28(4): 440-444.

参考文献

[1] Wu J, Han MH, Li J, et al. Immunopathogenesis of HBV infection. Adv Exp Med Biol, 2020, 1179: 71-107.
[2] Chen J, Guan L, Tang L, et al. T helper 9 cells: a new player in immune-related diseases. DNA Cell Biol, 2019, 38 (10): 1040-1047.
[3] Wan J, Wu YQ, Ji XY, et al. IL-9 and IL-9-producing cells in tumor immunity. Cell Commun Signal, 2020, 18 (1): 50.
[4] Neurath MF, Kaplan MH. Th9 cells in immunity and immunopathological diseases. Semin Immunopathol, 2017, 39 (1): 1-4.
[5] Schmitt E, Klein M, Bopp T. Th9 cells, new players in adaptive immunity. Trends Immunol, 2014, 35:61-68.
[6] Lauder AJ, Jolin HE, Smith P, et al. Lymphomagenesis, hydronephrosis, and autoantibodies result from dysregulation of IL-9 and are differentially dependent on Th2 cytokines. J Immunol, 2004, 173:113-122.
[7] Yu X, Zheng Y, Deng Y, et al. Serum interleukin (IL)-9 and IL-10, but not T-helper 9 (Th9) cells, are associated with survival of patients with acute-on-chronic hepatitis B liver failure. Medicine (Baltimore), 2016, 95(16):e3405.
[8] Qin SY, Lu DH, Guo XY, et al. A deleterious role for Th9/IL-9 in hepatic fibrogenesis. Sci Rep, 2016, 6:18694.
[9] Ming D, Yu X, Guo R, et al. Elevated TGF-beta1/IL-31 pathway is associated with the disease severity of hepatitis B virus-related liver cirrhosis.Viral Immunol, 2015, 28(4):209-16.
[10] Shan YQ, Dong HL, Xiao YG, et al. A deleterious role for Th9/IL-9 in hepatic fibrogenesis. Sci Re, 2016, 6:18694.
[11] 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). 中华肝脏病杂志, 2019, 27(12):938-961.
[12] Oo YH, Adams DH. The role of chemokines in the recruitment of lymphocytes to the liver. J Autoimmun, 2010, 34: 45-54.
[13] Li X, Liu X, Tian L, et al. Cytokine-mediated immunopathogenesis of hepatitis B virus infections. Clin Rev Allergy Immunol, 2016, 50:41-54.
[14] Li J, Qiu SJ, She WM, et al. Significance of the balance between regulatory T (Treg) and T helper 17 (Th17) cells during hepatitis B virus related liver fibrosis. PLoS One, 2012, 7:e39307.

[1]	李芬, 韦淑珍, 李良, 莫雨灵, 傅小凡, 雷任国, 郑子玉. HBV携带孕妇妊娠期及产后肝炎发作风险及NAs干预观察[J]. 肝脏, 2023, 28(5): 527-529.
[2]	严景全, 刘娟, 卢雪兰, 蓝云翠, , 林占洲. 直接抗病毒药物对持续病毒学应答慢性丙型肝炎患者肝纤维化的影响[J]. 肝脏, 2023, 28(5): 530-533.
[3]	冯薇薇, 孔严, 康茹. 慢性丙型肝炎合并代谢相关脂肪性肝病患者的临床特征及预后评价[J]. 肝脏, 2023, 28(5): 534-536.
[4]	张朋垒, 张明婷, 郝礼森, 靳丽敏, 潘恩亮, 何宇, 苗笑佳, 王薇. 四氯化碳诱导的大鼠肝纤维化肝组织中SHP2表达与在体肝星状细胞活化及增殖的关系[J]. 肝脏, 2023, 28(5): 549-553.
[5]	李庆鑫, 尹卿, 关瑛琦, 邵春红. 幽门螺杆菌感染与自身免疫性肝病关系的分析[J]. 肝脏, 2023, 28(5): 590-592.
[6]	陈芬兰, 程计林, 林文, 陈丽萍. 血清HBV RNA的临床研究进展[J]. 肝脏, 2023, 28(5): 607-610.
[7]	邓霖霖, 石清兰, 韦华柱, 莫展进, 黄祖鸿. 乙型肝炎病毒相关肝细胞癌高危因素分析[J]. 肝脏, 2023, 28(5): 614-617.
[8]	李珊珊, 徐曼曼, 杨雪, 陈煜. 2012至2021年北京佑安医院HBV相关慢加急性肝衰竭患者住院费用分析[J]. 肝脏, 2023, 28(4): 405-409.
[9]	王志会, 周石. TLR4/MyD88/NF-κB信号通路调控肝星状细胞活化及其临床意义[J]. 肝脏, 2023, 28(4): 493-495.
[10]	陈文雅, 赵红, 谢雯. 免疫抑制疗法相关的HBV再激活及其预防[J]. 肝脏, 2023, 28(3): 275-278.
[11]	卢秋燕, 卢燕辉, 徐成润. 瞬时弹性成像检测肝硬度联合脾硬度对慢性乙型肝炎肝纤维化诊断的价值[J]. 肝脏, 2023, 28(3): 325-329.
[12]	王伟, 葛亮, 余宁, 熊晓芸. 非肥胖型非酒精性脂肪性肝病组织学特征及临床结局评价[J]. 肝脏, 2023, 28(3): 360-363.
[13]	陈静娜, 郝孟翰, 宋欣络, 王冰, 高攀, 钱宇妍, 陈岩松, 黄文俊, 赵萌, 张桠婕. 慢性乙型肝炎新的治疗方法[J]. 肝脏, 2023, 28(2): 135-145.
[14]	刘云霄, 符艳, 牛丽娜, 窦婧, 王晓忠. 核苷(酸)类似物治疗与乙型肝炎病毒相关肝癌术后生存的meta分析[J]. 肝脏, 2023, 28(2): 181-188.
[15]	厉绾, 韩艳霞, 谢寿珍, 马颖才, 杨永耿, 李萍英. 减重对CHB和(或)NAFLD患者肝纤维化及脂肪肝程度的影响[J]. 肝脏, 2023, 28(2): 203-206.