Predictive value of quantitative detection of hepatitis B virus surface antigen in the relapse of hepatitis B induced by entecavir

doi:10.3877/cma.j.issn.1674-1358.2018.04.014

Abstract

Abstract:

Objective

To investigate the diagnostic efficacy of quantitative detection of hepatitis B virus surface antigen (HBsAg) in patients with hepatitis B relapse after entecavir withdrawal.

Methods

Total of 80 patients with chronic hepatitis B (CHB) who received antiviral treatment with entecavir in Dongfang Hospital of Hainan Province from January 2013 to January 2016 were analyzed, retrospectively. The patients were divided into recurrence group (60 cases) and non-recurrence group (20 cases). The virological indexes including HBV DNA load and HBsAg determination were compared between the two groups. The influencing factors of relapse after entecavir treatment were analyzed by Cox regression model. The value of quantitative HBsAg detection after treatment in predicting the recurrence of patients with entecavir treatment was evaluated by ROC curve.

Results

A total of 60 cases (75.00%) had virological recurrence during the 24-month follow-up, with the median recurrence time of 9.5 (5-24) months. There was no significant difference in age, sex ratio, body mass index, history of CHB and AFP between recurrent group and non-recurrence group (t= 0.854,χ²= 1.077,t = 0.749,t= 1.354,t= 1.499;P= 0.396, 0.299, 0.456, 0.180, 0.138). The positive rate of HBeAg, cirrhosis, family history of hepatitis B, HBV DNA load before treatment, HBsAg quantification after treatment and HBsAg positive rate in recurrence group were significantly higher than those in the non-recurrence group (χ²= 4.364, 6.667, 4.689,t= 4.096, 2.040, 8.219, 5.760;P= 0.037, 0.010, 0.030, 0.043,< 0.001, 0.016), but the medication time was significantly lower than that of non-recurrence group (t= 2.006,P= 0.048), with significant differences. Multivariate Cox regression analysis showed that cirrhosis (HR= 1.587,P= 0.041), HBeAg positive (HR= 1.742,P= 0.044) and HBsAg quantitative (HR= 2.606,P= 0.008) were independent risk factors for the relapse after entecavir treatment. ROC curve showed that the area under the curve of HBsAg quantification (AUC= 0.902,P< 0.001) was higher than that of semi-quantitative detection (AUC= 0.650,P = 0.046), with significant differences. The best cut-off point of HBsAg quantification was 2.03 log₁₀IU/ml. The accuracy, sensitivity, specificity, positive predictive value and negative predictive value were 91.25%, 91.67%, 90%, 96.49% and 78.26%, respectively.

Conclusions

Liver cirrhosis, HBeAg positive and high HBsAg levels after treatment are independent risk factors for the relapse of hepatitis B after entecavir withdrawal. The quantitative detection of HBsAg for predicting the recurrence of patients with entecavir withdrawal had a high diagnostic efficacy.

Key words: Chronic hepatitis B, Entecavir, Hepatitis B surface antigen, Relapse

Changsheng Wang, XiaoHe Yue, Miao Lu. Predictive value of quantitative detection of hepatitis B virus surface antigen in the relapse of hepatitis B induced by entecavir[J]. Chinese Journal of Experimental and Clinical Infectious Diseases(Electronic Edition), 2018, 12(04): 386-391.

/ / Recommend

Add to citation manager EndNote|Ris|BibTeX

URL: https://zhsyhlcgrbzz.cma-cmc.com.cn/EN/10.3877/cma.j.issn.1674-1358.2018.04.014

https://zhsyhlcgrbzz.cma-cmc.com.cn/EN/Y2018/V12/I04/386

Figures/Tables 4

References 25

[1]	科技部十二五重大专项联合课题组专家. 乙型肝炎病毒相关肝硬化的临床诊断,评估和抗病毒治疗的综合管理[J]. 中华肝脏病杂志,2014,22(5):327-335.
[2]	McMahon BJ. Chronic hepatitis B virus infection[J]. Med Clin North Am,2014,98(1):39-54.
[3]	慢性乙型肝炎核苷(酸)类似物经治患者抗病毒治疗专家委员会. 慢性乙型肝炎核苷(酸)类似物经治患者抗病毒治疗专家共识: 2016年更新[J]. 中国肝脏病杂志(电子版),2016,8(3):15-20.
[4]	Martinot-Peignoux M,Lapalus M,Asselah T,Marcellin P. HBsAg quantification: useful for monitoring natural history and treatment outcome[J]. Liver Int,2014,34(S1):S97-S107.
[5]	Martinot-Peignoux M,Asselah T,Marcellin P. HBsAg quantification to optimize treatment monitoring in chronic hepatitis B patients[J]. Liver Int,2015,35(S1):82-90.
[6]	中华医学会感染病学分会. 慢性乙型肝炎防治指南(2010年版)[J]. 中华肝脏病杂志,2011,19(1):13-24.
[7]	慢性乙型肝炎核苷(酸)类药物经治患者抗病毒治疗专家委员会. 慢性乙型肝炎核苷(酸)类药物经治患者抗病毒治疗专家共识[J]. 中华医学信息导报,2014,29(1):122-126.
[8]	抗乙型肝炎病毒核苷酸类似物不良反应管理专家委员会. 抗乙型肝炎病毒核苷(酸)类似物不良反应管理专家共识[J/CD]. 中华实验和临床感染病杂志(电子版),2016,10(5):522-526.
[9]	张国民,孙校金,王富珍, 等. 中国18-59岁人群乙型病毒性肝炎流行病学特征分析及乙型肝炎疫苗免疫策略探讨[J]. 中国疫苗和免疫,2013,19(3):266-270.
[10]	Tsai MC,Chen CH,Hu TH, et al. Long-term outcomes of hepatitis B virus-related cirrhosis treated with nucleos(t)ide analogs[J]. J Formos Med Assoc,2017,116(7):512-521.
[11]	Jang JW,Choi JY,Kim YS, et al. Long-term effect of antiviral therapy on disease course after decompensation in patients with hepatitis B virus-related cirrhosis[J]. Hepatology,2015,61(6):1809-1820.
[12]	Ridruejo E,Marciano S,Galdame O, et al. Relapse rates in chronic hepatitis B naïve patients after discontinuation of antiviral therapy with entecavir[J]. J Viral Hepat,2014,21(8):590-596.
[13]	Fung J,Wong T,Chok K, et al. Long-term outcomes of entecavir monotherapy for chronic hepatitis B after liver transplantation: Results up to 8 years[J]. Hepatology,2017,66(4):1036-1044.
[14]	Ahn J,Lee HM,Lim JK, et al. Entecavir safety and effectiveness in a national cohort of treatment-naïve chronic hepatitis B patients in the US--the ENUMERATE study[J]. Aliment Pharmacol Ther,2016,43(1):134-144.
[15]	史萍,蒋龙凤,李军. 慢性乙型肝炎患者核苷(酸)类药物停药后复发的相关因素荟萃分析[J]. 中华临床感染病杂志,2015,8(1):58-69.
[16]	Lee HA,Seo YS,Park SW, et al. Hepatitis B surface antigen titer is a good indicator of durable viral response after entecavir off-treatment for chronic hepatitis B[J]. Clin Mol Hepatol,2016,22(3):382-389.
[17]	Shinkai N,Kusumoto S,Murakami S, et al. Novel monitoring of hepatitis B reactivation based on ultra-high sensitive hepatitis B surface antigen assay[J]. Liver Int,2017,37(8):1138-1147.
[18]	Wang CC,Tseng KC,Hsieh TY, et al. Assessing the durability of entecavir-treated hepatitis B using quantitative HBsAg[J]. Am J Gastroenterol,2016,111(9):1286-1294.
[19]	Ji M,Hu K. Recent advances in the study of hepatitis B virus covalently closed circular DNA[J]. Virol Sin,2017,32(6):454-464.
[20]	Gao Y,Li Y,Meng Q, et al. Serum hepatitis B virus DNA, RNA, and HBsAg: which correlated better with intrahepatic covalently closed circular DNA before and after nucleos(t)ide analogue treatment?[J]. J Clin Microbiol,2017,55(10):2972-2982.
[21]	Sonneveld MJ,Rijckborst V,Zeuzem S, et al. Presence of precore and core promoter mutants limits the probability of response to peginterferon in hepatitis B e antigen-positive chronic hepatitis B[J]. Hepatology,2012,56(1):67-75.
[22]	Kim SH. ELISA for Quantitative determination of hepatitis B virus surface antigen[J]. Immune Netw,2017,17(6):451-459.
[23]	游春芳,周利民,邓薇. 基因1b型慢性丙型肝炎患者血清铁蛋白水平与聚乙二醇干扰素抗病毒疗效的关系[J]. 临床肝胆病杂志,2017,33(9):1713-1716.
[24]	Sonneveld MJ,Rijckborst V,Boucher CA, et al. Prediction of sustained response to peginterferon alfa-2b for hepatitis B e antigen-positive chronic hepatitis B using on-treatment hepatitis B surface antigen decline[J]. Hepatology,2010,52(4):1251-1257.
[25]	Zhang L,Xie XY,Chen Y, et al. Hepatitis B surface antigen predicts recurrence after radiofrequency ablation in patients with low hepatitis B virus loads[J]. Medicine (Baltimore),2017,96(52):e9377.

临床资料		复发组（60例）	未复发组（20例）	统计量	P值
年龄（±s，岁）		43.6 ± 6.3	45.0 ± 6.7	t= 0.854	0.396
性别[例（%）]		?	?	χ²= 1.077	0.299
?	男性	35（58.3）	9（45.0）	?	?
?	女性	25（41.7）	11（55.0）	?	?
BMI（±s，kg/m²）		23.1 ± 2.7	23.6 ± 2.2	t= 0.749	0.456
治疗前HBeAg定性[例（%）]		?	?	χ²= 4.364	0.037
?	阳性	40（66.7）	10（50.0）	?	?
?	阴性	20（33.3）	10（50.0）	?	?
用药时间（±s，年）		1.8 ± 0.4	2.0 ± 0.4	t= 2.006	0.048
乙型肝炎病史（±s，年）		4.2 ± 2.4	3.3 ± 2.3	t= 1.354	0.180
肝硬化[例（%）]		25（41.7）	3（15.0）	χ²= 4.689	0.030
乙型肝炎家族史[例（%）]		20（33.3）	2（10.0）	χ²= 4.096	0.043
治疗前HBV DNA载量（±s，log₁₀IU/ml）		7.1 ± 1.6	6.2 ± 1.5	t= 2.040	0.045
治疗后HBsAg定量（±s，log₁₀IU/ml）		2.9 ± 0.6	1.9 ± 0.4	t= 8.219	< 0.001
?	治疗后HBsAg定性[例（%）]	?	?	χ²= 5.760	0.016
?	阳性	27（45.0）	3（15.0）	?	?
?	阴性	33（55.0）	17（85.0）	?	?
甲胎蛋白（±s，μg/L）		46.7 ± 7.2	44.1 ± 5.6	t= 1.499	0.138

临床资料		复发组（60例）	未复发组（20例）	统计量	P值
年龄（±s，岁）		43.6 ± 6.3	45.0 ± 6.7	t= 0.854	0.396
性别[例（%）]		?	?	χ²= 1.077	0.299
?	男性	35（58.3）	9（45.0）	?	?
?	女性	25（41.7）	11（55.0）	?	?
BMI（±s，kg/m²）		23.1 ± 2.7	23.6 ± 2.2	t= 0.749	0.456
治疗前HBeAg定性[例（%）]		?	?	χ²= 4.364	0.037
?	阳性	40（66.7）	10（50.0）	?	?
?	阴性	20（33.3）	10（50.0）	?	?
用药时间（±s，年）		1.8 ± 0.4	2.0 ± 0.4	t= 2.006	0.048
乙型肝炎病史（±s，年）		4.2 ± 2.4	3.3 ± 2.3	t= 1.354	0.180
肝硬化[例（%）]		25（41.7）	3（15.0）	χ²= 4.689	0.030
乙型肝炎家族史[例（%）]		20（33.3）	2（10.0）	χ²= 4.096	0.043
治疗前HBV DNA载量（±s，log₁₀IU/ml）		7.1 ± 1.6	6.2 ± 1.5	t= 2.040	0.045
治疗后HBsAg定量（±s，log₁₀IU/ml）		2.9 ± 0.6	1.9 ± 0.4	t= 8.219	< 0.001
?	治疗后HBsAg定性[例（%）]	?	?	χ²= 5.760	0.016
?	阳性	27（45.0）	3（15.0）	?	?
?	阴性	33（55.0）	17（85.0）	?	?
甲胎蛋白（±s，μg/L）		46.7 ± 7.2	44.1 ± 5.6	t= 1.499	0.138

变量	B值	标准误差	Wald值	P值	HR值	95%CI
肝硬化	0.581	0.557	3.653	0.041	1.587	1.112～3.766
HBeAg阳性	0.632	0.622	3.502	0.044	1.742	1.096～4.662
治疗后HBsAg	1.018	0.326	6.298	0.008	2.606	1.278～5.911

变量	B值	标准误差	Wald值	P值	HR值	95%CI
肝硬化	0.581	0.557	3.653	0.041	1.587	1.112～3.766
HBeAg阳性	0.632	0.622	3.502	0.044	1.742	1.096～4.662
治疗后HBsAg	1.018	0.326	6.298	0.008	2.606	1.278～5.911

Please choose a citation manager

Content to export