Abstract
Hepatitis D virus (HDV) infection increases the risk of hepatocellular carcinoma (HCC) in the natural course of chronic hepatitis B (CHB) patients. Its role in patients treated with nucleotide/nucleoside analogues (NAs) is unclear. We aimed to study the role of hepatitis D in the development of HCC in CHB patients treated with NAs. Altogether, 1349 CHB patients treated with NAs were tested for anti-HDV antibody and RNA. The incidence and risk factors of HCC development were analyzed. Rates of anti-HDV and HDV RNA positivity were 2.3% and 1.0%, respectively. The annual incidence of HCC was 1.4 per 100 person-years after a follow-up period of over 5409.5 person-years. The strongest factor association with HCC development was liver cirrhosis (hazard ratio [HR]/95% confidence interval [CI] 9.98/5.11–19.46, P < 0.001), followed by HDV RNA positivity (HR/ CI 5.73/1.35–24.29, P = 0.02), age > 50 years old (HR/CI 3.64/2.03–6.54, P < 0.001), male gender (HR/CI 2.69/1.29–5.60, P: 0.01), and body mass index (BMI, HR/CI 1.11/1.03–1.18, P = 0.004). The 5-year cumulative incidence of HCC was 7.3% for patients with HDV RNA negativity compared to that of 22.2% for patients with HDV RNA positivity (P = 0.01). In the subgroup of cirrhotic patients, the factors associated with HCC development were HDV RNA positivity (HR/CI 4.45/1.04–19.09, P = 0.04) and BMI (HR/CI 1.11/1.03–1.19, P = 0.01). HDV viremia played a crucial role in HCC development in CHB patients who underwent NA therapy.
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Introduction
Hepatitis B virus (HBV) infection is one of the major etiological factors of hepatocellular carcinoma (HCC), which imposes a heavy burden on global health. HBV was highly prevalent in adults prior to the launch of the national HBV vaccination programs. It is the leading cause of HCC in Taiwan1,2. The etiology of HBV-related HCC is multifactorial and includes virological factors such as HBV DNA levels, HBV genotypes, mutants, and host factors such as age, gender, cirrhosis, and metabolic disorders3. Among the risk factors, liver cirrhosis has been the most crucial determinant of HCC. The incidence of HCC increases significantly after the development of liver cirrhosis. The incidence of HCC has been reported to be 0.2 per 100 person-years in inactive carriers, 0.6 per 100 person-years in non-cirrhotic patients, and 3.7 per 100 person-years in patients with compensated cirrhosis4. However, antiviral therapy including nucleotide/nucleoside analogues (NAs) is reported to result in an improvement in hepatic inflammation and fibrosis, which in turn reduces the risk of HCC development and mortality5,6.
Hepatitis D virus (HDV) is a single-stranded RNA virus and its propagation depends on HBV7. The worldwide prevalence of HDV ranges from < 1% to > 50%8. Among chronic hepatitis B (CHB) patients, the hepatitis D antibody (anti-HDV) positivity rate is reported to be 2–5% in the general population9,10 and up to 68.9% in persons who inject drugs in Taiwan11. Chronic hepatitis D (CHD) infection may result in a deterioration of liver function and may also lead to a threefold increase in the risk of HCC in the typical course of the disease12,13. Notably, the impact of HDV on HCC occurrence in CHB patients treated with NAs remains unclear. Hence, we aimed to address this issue by enrolling a well-characterized CHB cohort treated with NAs. HDV serology and virology in this cohort were also studied and considered for the evaluation of its impact on HCC development.
Methods
Patients
CHB patients allocated to NAs were consecutively enrolled in a medical center in Taiwan from June 2000 to July 2018 in the retrospective study. Patients were followed up from the beginning of NA treatment. The treatment indications for NAs were based on the national health insurance reimbursement regulations of the Ministry of Health and Welfare in Taiwan2,14, Briefly, the criteria included (1) HBeAg-negative patients with HBV DNA greater than 2000 IU/mL with persistent alanine aminotransferase abnormality greater than two times the upper limit of normal (ULN) on two occasions 3 months apart, and (2) HBeAg-positive patients with HBV DNA greater than 20,000 IU/mL with ALT abnormality greater than two times the ULN for two occasions 3 months apart, or with ALT > 5 times the ULN, (3) cirrhotic patients with HBV DNA greater than 2000 IU/mL, and (4) liver decompensation, denoted as prothrombin time prolongs > 3 s or a total bilirubin > 2 mg/dL2. Patients were excluded if they had any of the following conditions: alcoholism (≥ 20 g daily), coinfection with human immunodeficiency virus or hepatitis C virus (HCV), ongoing interferon-based therapy, pre-existing HCC before the use of NAs, and the use of NAs for chemotherapy prophylaxis. The study was conducted in accordance with the principles of the Declaration of Helsinki of 1975, as revised in 2008. The ethics committee of Kaohsiung Medical University Hospital approved the study. All patients provided informed consent before enrollment.
Laboratory analyses
Biochemical analyses were performed using a multichannel autoanalyzer (Hitachi Inc., Tokyo, Japan). Hepatitis B surface antigen (HBsAg) was detected using standard quantitative chemiluminescent microparticle immunoassay (ARCHITECT HBsAg, Abbott Diagnostics, Chicago, IL, USA). Serum HBV DNA was examined using a standardized, automated quantitative polymerase chain reaction assay (COBAS TaqMan HBV test, Roche Diagnostics, Branchburg, NJ; detection limit 12 IU/mL)15. Anti-HDV antibody was verified at the initiation of treatment with anti-HBV agents. Screening for anti-HDV immunoglobulin G was performed using the anti-HDV enzyme-linked immunosorbent assay kit (General Biologicals Corporation, Hsinchu, Taiwan)7,10. HDV RNA was tested in patients with anti-HDV positivity using the LightMix Kit HDV (Roche Life Science, Berlin, Germany) on the Roche LightCycler (Roche Life Science, Berlin, Germany; detection limit: 10 copies/mL)16. The fibrosis-4 index was calculated by using the following formula: age (years) × aspartate aminotransferase [U/L]/platelets [109/L] × alanine transaminase [U/L])1/2. Liver cirrhosis was diagnosed using transient elastography (FibroScan; Echosens, Paris, France; >12 kPa)17, histology, or the presence of laboratory, radiological, endoscopic, or clinical evidence of portal hypertension and/or cirrhosis. HCC was confirmed by clinical or histological diagnosis according to the guidelines of the American Association for the Study of Liver Diseases18 and the Asian Pacific Association for the Study of the Liver19. Patients visited the clinics every 1 to 3 months depending on the physician’s discretion. Laboratory tests, including aspartate aminotransferase (AST), alanine aminotransferase (ALT), alpha-fetoprotein (AFP), and hepatitis B virus serology/virology were assessed every 3 to 6 months if the patient’s condition was stable. HCC surveillance by abdominal sonography was performed every 3 to 6 months based on the severity of the liver disease.
Statistical analyses
Frequencies were analyzed between the groups using the chi-square (χ2) test with Yates correction or Fisher’s exact test. Data are presented as mean ± standard deviation. Data were compared using analysis of variance, Student’s t-test, or the nonparametric Mann-Whitney U test. A stepwise logistic regression analysis was applied to analyze the characteristics associated with anti-HDV and HDV RNA positivity by analyzing the covariates with P values < 0.1 in the univariate analysis. Kaplan–Meier analysis and a log-rank test was performed for the comparison of the cumulative incidence of HCC with respect to various determinants. Cox regression analysis was applied to analyze the factors independently associated with HCC development by analyzing the covariates with P-values < 0.2 in the univariate analysis or the factors considered to have potential and clinical relevance. Statistical analyses were performed using IBM SPSS Statistics, version 20 (IBM Corp., Armonk, NY, USA). All statistical analyses were based on two-sided hypothesis tests with statistical significance set at P < 0.05.
Results
Patient characteristics
Altogether, 2500 CHB patients who received NAs were initially recruited. After excluding patients with pre-existing HCC (n = 343), patients using NAs for chemotherapy prophylaxis (n = 771), patients with anti-HCV positivity (n = 27), and patients receiving interferon-based therapy (n = 10), 1349 patients were enrolled for analysis (Fig. 1). The mean age was 48.0 years and 72.4% of the patients were male. The mean HBV DNA level was 5.9 log10 IU/mL. Patients with liver cirrhosis accounted for 29.1% (n = 392) of the study population. The rates of anti-HDV and HDV RNA positivity were 2.3% and 1.0%, respectively. The most commonly used NAs were entecavir (45.2%) and tenofovir disoproxil fumarate (12.2%) (Table 1).
Characteristics of patients with HDV infection
Compared to anti-HDV negative patients, those with anti-HDV positivity were older (55.4 years vs. 47.9 years, P = 0.003) and had lower HBV DNA levels (4.4 log10 IU/mL vs. 6.0 log10 IU/mL, P = 0.001). Logistic regression analysis revealed that factors associated with anti-HDV positivity included age (odds ratio [OR], 95% confidence interval [CI] 1.04/1.01–1.07; P: 0.007) and HBV DNA level (OR/CI 0.71/0.59–0.86; P < 0.001) (Supplementary Table 1). There was no difference in terms of the mean HBV DNA level (1.4 log10 IU/mL vs. 1.2 log10 IU/mL, P = 0.35) and the proportion of undetectable HBV DNA (79.5% vs. 90.5%, P = 0.28) after 1 year of NA therapy between anti-HDV negative and positive patients.
Compared to HDV RNA negative patients, those with HDV RNA positivity had lower baseline HBV DNA levels (4.0 log10 IU/mL vs. 5.9 log10 IU/mL, P = 0.003). Logistic regression analysis revealed that the only factor independently associated with HDV RNA positivity was a baseline HBV DNA level (OR/CI 0.63/0.48–0.83; P < 0.001) (Supplementary Table 2).
Cumulative incidence and risk factors of HCC development
Seventy-six (5.6%) patients developed HCC over a follow-up period of 5409.5 person-years (range: 1.0–15.0 years; annual incidence: 1.4%). The cumulative incidence of HCC was 2.3%, 5.4%, and 7.5% at the 1-year, 3-year, and 5-year follow-ups, respectively. Compared to patients without HCC development, patients with HCC had higher proportions of: age over 50 years (69.7% vs. 40.9%, P < 0.001), male gender (85.5% vs. 71.6%, P = 0.008), liver cirrhosis (81.6% vs. 25.9%, P < 0.001), higher body mass index (BMI) (26.1 kg/m2 vs. 24.5 kg/m2, P = 0.001), lower platelet count (117.1×103 u/L vs. 169.3×103 u/L, P < 0.001), and a substantially higher proportion of HDV RNA positivity (2.6% vs. 0.9%, P = 0.16, Table 2). Cox-regression analysis revealed that the strongest factor associated with HCC development was liver cirrhosis (hazard ratio [HR]: 95% confidence interval [CI] 9.98/5.11–19.46, P < 0.001), followed by HDV RNA positivity (HR: 5.73, CI 1.35–24.29, P = 0.02), age over 50 years (HR: 3.64, CI 2.03–6.54, P < 0.001), male gender (HR: 2.69, CI 1.29–5.60, P=0.01), and BMI (HR: 1.11, CI 1.03–1.18, P = 0.004, Table 2). The 1-year, 3-year, and 5-year cumulative incidence rates of HCC were 2.1%, 5.3%, and 7.3%, respectively, in anti-HDV (−) or anti-HDV (+)/HDV RNA (−) patients when compared with the incidence rates of 22.2%, 22.2%, and 22.2%, respectively, in HDV RNA (+) patients (log-rank P = 0.01, Fig. 2a). Among the 31 anti-HDV-positive patients, there was no identifiable factor associated with HCC development (Supplementary Table 3).
Risk factors of HCC development in patients with or without liver cirrhosis
Since underlying liver cirrhosis was the most important predictive factor of HCC, we analyzed the occurrence of HCC stratified by liver cirrhosis. Sixty-two out of 392 cirrhotic patients (15.8%) developed HCC over a follow-up period of 1355.7 person-years (annual incidence: 4.6%). The cumulative incidence rates of HCC were 6.0%, 16.4%, and 23.5% at the 1-year, 3-year, and 5-year follow-ups, respectively. Compared to patients without HCC development, patients with HCC had substantially higher BMI (26.1 kg/m2 vs. 25.2 kg/m2, P = 0.13) and a substantially higher proportion of HDV RNA positivity (3.2% vs. 0.9%, P = 0.18), although the differences did not reach the conventional level of statistical significance (Table 3). Cox regression analysis revealed that the factors associated with HCC development were BMI (HR/CI 1.11/1.03–1.19, P = 0.01) and HDV RNA positivity (HR/CI 4.45/1.04–19.09, P = 0.04, Table 3). In cirrhotic patients, the 1-year, 3-year, and 5-year cumulative incidence rates of HCC were 5.4%, 15.9%, and 23.1%, respectively, in anti-HDV (−) or anti-HDV (+)/HDV RNA (−) patients when compared with the incidence rates of 50.0%, 50.0%, and 50.0%, respectively, in anti-HDV (+)/HDV RNA (+) patients (log-rank P = 0.04, Fig. 2b).
Fourteen out of 957 non-cirrhotic patients (1.5%) developed HCC over a follow-up period of 4051.3 person-years (annual incidence: 0.35%). The cumulative incidence rates of HCC in non-cirrhotic patients were 0.8%, 1.2%, and 1.2%, respectively, at the 1-year, 3-year, and 5-year follow-ups, respectively. Compared to patients without HCC development, those with HCC represented a higher proportion of patients over 50 years (85.7% vs. 34.5%, P < 0.001), diabetes (35.7% vs. 11.9%, P = 0.02) and lower platelet counts (145.5×103 vs. 185.7×103 u/L, P = 0.05). Cox regression analysis revealed that the factors associated with HCC development were an age over 50 years (HR/CI 13.26/1.60–109.75, P < 0.001) and platelet count (HR/CI 0.99/0.98–1.00, P = 0.04) (Supplementary Table 4).
Discussion
In the present study, we observed that the annual incidence of HCC was 1.4% in CHB patients treated with NAs. As expected, liver cirrhosis was the most important risk factor associated with HCC occurrence. We demonstrated that coinfection with HDV also played an essential role in HCC development, although the prevalence was low in Taiwanese patients. Compared to patients without concurrent HDV infection, those with HDV viremia had a nearly sixfold risk of HCC development.
HBV infection induces hepatic inflammation, which leads to liver cirrhosis and HCC. The HBV DNA level has a dose-dependent association with HCC development in the typical course of the disease20. The other risk factors of HBV-related HCC include liver cirrhosis, age, gender, and metabolic factors21,22. Several models have assessed the risk of HCC in CHB patients without antiviral therapy23,24. Moreover, emerging evidence has shown that HBV DNA suppression with NAs25,26 or interferon27,28 significantly reduced the HCC risk when compared with untreated controls. Currently, NAs are the mainstream agents for CHB therapy. They have reduced the HCC risk by 34–78% according to various studies29. However, HCC continues to develop under viral suppression. Some HCC prediction models have also been created in patients undergoing treatment with NAs30,31 and the pre-treatment viral loads were not found to be as crucial as those in NA-naïve patients. Underlying liver cirrhosis was reported to be the most critical determinant of HCC32, which is consistent with the results of the present study. The reported annual incidence of HCC was 0.3–1.2% in non-cirrhotic CHB patients and 1.8–6.0% in cirrhotic CHB patients undergoing NA therapy33. We observed a similar incidence of HCC in our patient cohort, with an annual incidence of 0.4% in non-cirrhotic patients and 4.6% in cirrhotic patients. Continuous surveillance of HCC remains mandatory in CHB patients receiving antiviral therapy, and it is crucial in cirrhotic patients.
The prevalence of HDV in the general population is low. It has been decreasing in Taiwan in recent decades9,10. The seroprevalence of anti-HDV and HDV RNA was 2.3% and 1%, respectively, in the present study, which is similar to that observed in a recent report in Taiwan9. HDV would increase the risk of HCC in the typical course of the disease13,22. However, debates continue regarding this issue9,34. There is no potent treatment against HDV infection. To date, interferon has been the standard of care35 and NAs are not effective in treating CHD36. However, NAs remain the mainstay for managing CHB. The impact of HDV on HCC has rarely been elucidated in NA-treated cohorts. Brancaccio et al. conducted a case-control study that disclosed that despite long-term NAs use, an increased risk of HCC remained in HDV-infected patients compared to those with HBV mono-infection37. In the current long-term observational study with a larger Asian cohort, we consistently demonstrated that HDV viremia increases the risk of HCC. This finding was also in line with the results from another recent study38. The aforementioned study by Kamal et al. suggested that HDV viremia might increase the incidence of liver-related events such as HCC, hepatic decompensation, and death. Notably, the majority of the patients were treated with interferon, while only a few patients received NAs38. In the present NA-based cohort study, we observed that one-fifth of the patients with HDV viremia had developed HCC at the 5-year follow-up. Moreover, 50% of the HDV-RNA positive cirrhotic patients eventually developed HCC. Currently, there is no potent antiviral agent to treat HDV infection. Given the high risk of HCC development, we suggest that each HDV-infected subject should be monitored regularly and closely until effective or curative anti-HDV agents can be prescribed in the clinical setting.
The present study has some limitations. Due to the low prevalence of HDV infection in the region where the study was conducted, the retrospective cohort was limited by relatively few index patients with HDV infection, particularly in non-cirrhotic subjects. This may have restricted the cumulative clinical impact of HDV on HCC. As with the majority of other studies, the current study aimed to identify baseline factors including HDV status rather than the sequential parameters predictive of HCC. We failed to provide information regarding cirrhotic development or resolution at the time of event occurrence or patient censoring. In addition, the follow-up duration was more condensed in HDV-infected patients. Although the follow-up duration was condensed in the HDV group, the HCC incidence was significantly higher than that in HBV mono-infected patients during the relatively brief observation period. The difference in HCC incidence between the groups was postulated to be more pronounced if the follow-up duration was prolonged in the HDV group.
In conclusion, the results of the present study suggest that HDV viremia plays an essential role in HCC development in CHB patients treated with NAs. HDV testing should be proposed for each HBV subject even when HBV replication is under control by NAs. We hope that these results will promote further validated studies, particularly in regions where HDV infection is widespread.
References
Yang, J. F. et al. Viral hepatitis infections in southern Taiwan: A multicenter community-based study. Kaohsiung J. Med. Sci. 26, 461–469 (2010).
Chien, R. N. et al. Taiwan consensus statement on the management of chronic hepatitis B. J. Formos Med. Assoc. 118, 7–38 (2019).
El-Serag, H. B. Epidemiology of viral hepatitis and hepatocellular carcinoma. Gastroenterology 142(1264–1273), e1261 (2012).
Fattovich, G., Bortolotti, F. & Donato, F. Natural history of chronic hepatitis B: Special emphasis on disease progression and prognostic factors. J. Hepatol. 48, 335–352 (2008).
Grossi, G., Vigano, M., Loglio, A. & Lampertico, P. Hepatitis B virus long-term impact of antiviral therapy nucleot(s)ide analogues (NUCs). Liver Int. 37(Suppl 1), 45–51 (2017).
Chen, V. L. et al. Anti-viral therapy is associated with improved survival but is underutilised in patients with hepatitis B virus-related hepatocellular carcinoma: Real-world east and west experience. Aliment Pharmacol. Ther. 48, 44–54 (2018).
Mentha, N., Clement, S., Negro, F. & Alfaiate, D. A review on hepatitis D: From virology to new therapies. J. Adv. Res. 17, 3–15 (2019).
Vlachogiannakos, J. & Papatheodoridis, G. V. New epidemiology of hepatitis delta. Liver Int. 40(Suppl 1), 48–53 (2020).
Lin, H. H. et al. Changing hepatitis D virus epidemiology in a hepatitis B virus endemic area with a national vaccination program. Hepatology 61, 1870–1879 (2015).
Jang, T. Y. et al. Serial serologic changes of hepatitis D virus in chronic hepatitis B patients receiving nucleos(t)ides analogues therapy. J. Gastroenterol. Hepatol. 35(11), 1886–1892 (2020).
Hsieh, M. H. et al. Hepatitis D virus infections among injecting drug users with and without human immunodeficiency virus infection in Taiwan. Kaohsiung J. Med. Sci. 32, 526–530 (2016).
Tamura, I. et al. Risk of liver cirrhosis and hepatocellular carcinoma in subjects with hepatitis B and delta virus infection: A study from Kure, Japan. J. Gastroenterol. Hepatol. 8, 433–436 (1993).
Alfaiate, D., Clement, S., Gomes, D., Goossens, N. & Negro, F. Chronic hepatitis D and hepatocellular carcinoma: A systematic review and meta-analysis of observational studies. J. Hepatol. 73(3), 533–539 (2020).
https://www.nhi.gov.tw/BBS_Detail.aspx?n=73CEDFC921268679&sms=D6D5367550F18590&s=66360DBE1F9DFA41. Accessed on 2019.09.07.
Lin, Y. Y. et al. Performance characteristics of two real-time PCR assays for quantification of hepatitis B virus DNA. Scand. J. Infect. Dis. 41, 614–618 (2009).
Ghamari, S. et al. Prevalence of hepatitis delta virus (HDV) infection in chronic hepatitis B patients with unusual clinical pictures. Hepat. Mon. 13, e6731 (2013).
Castera, L. et al. Prospective comparison of transient elastography, Fibrotest, APRI, and liver biopsy for the assessment of fibrosis in chronic hepatitis C. Gastroenterology 128, 343–350 (2005).
Heimbach, J. K. et al. AASLD guidelines for the treatment of hepatocellular carcinoma. Hepatology 67, 358–380 (2018).
Omata, M. et al. Asia-Pacific clinical practice guidelines on the management of hepatocellular carcinoma: A 2017 update. Hepatol. Int. 11, 317–370 (2017).
Chen, C. J. & Yang, H. I. Natural history of chronic hepatitis B REVEALed. J. Gastroenterol. Hepatol. 26, 628–638 (2011).
Kasmari, A. J. et al. Independent of cirrhosis, hepatocellular carcinoma risk is increased with diabetes and metabolic syndrome. Am. J. Med. 130, 746.e741-746.e747 (2017).
Romeo, R. et al. A 28-year study of the course of hepatitis Delta infection: A risk factor for cirrhosis and hepatocellular carcinoma. Gastroenterology 136, 1629–1638 (2009).
Yang, H. I. et al. Risk estimation for hepatocellular carcinoma in chronic hepatitis B (REACH-B): Development and validation of a predictive score. Lancet Oncol. 12, 568–574 (2011).
Yang, H. I. et al. Real-world effectiveness from the Asia Pacific Rim liver consortium for HBV risk score for the prediction of hepatocellular carcinoma in chronic hepatitis B patients treated with oral antiviral therapy. J. Infect. Dis. 221, 389–399 (2020).
Lin, C. L. & Kao, J. H. Perspectives and control of hepatitis B virus infection in Taiwan. J. Formos Med. Assoc. 114, 901–909 (2015).
Wu, C. Y. et al. Association of nucleos(t)ide analogue therapy with reduced risk of hepatocellular carcinoma in patients with chronic hepatitis B: A nationwide cohort study. Gastroenterology 147(143–151), e145 (2014).
Lin, S. M. et al. Interferon therapy in HBeAg positive chronic hepatitis reduces progression to cirrhosis and hepatocellular carcinoma. J. Hepatol. 46, 45–52 (2007).
Yeh, M. L., Huang, J. F., Dai, C. Y., Yu, M. L. & Chuang, W. L. Pharmacokinetics and pharmacodynamics of pegylated interferon for the treatment of hepatitis B. Expert Opin. Drug Metab. Toxicol. 15, 779–785 (2019).
Lin, C. L. & Kao, J. H. Review article: The prevention of hepatitis B-related hepatocellular carcinoma. Aliment Pharmacol. Ther. 48, 5–14 (2018).
Hsu, Y. C. et al. Development of a scoring system to predict hepatocellular carcinoma in Asians on antivirals for chronic hepatitis B. J. Hepatol. 69, 278–285 (2018).
Kim, J. H. et al. Modified PAGE-B score predicts the risk of hepatocellular carcinoma in Asians with chronic hepatitis B on antiviral therapy. J. Hepatol. 69, 1066–1073 (2018).
Liu, L. Clinical features of hepatocellular carcinoma with hepatitis B virus among patients on Nucleos(t) ide analog therapy. Infect. Agent Cancer 15, 8 (2020).
Hiramatsu, N., Yamada, R. & Takehara, T. The suppressive effect of nucleos(t)ide analogue treatment on the incidence of hepatocellular carcinoma in chronic hepatitis B patients. J. Gastroenterol. Hepatol. 31, 546–552 (2016).
Huo, T. I. et al. Comparison of clinico-pathological features in hepatitis B virus-associated hepatocellular carcinoma with or without hepatitis D virus superinfection. J. Hepatol. 25, 439–444 (1996).
Krause, A., Haberkorn, U. & Mier, W. Strategies for the treatment of HBV/HDV. Eur. J. Pharmacol. 833, 379–391 (2018).
Petersen, J., Thompson, A. J. & Levrero, M. Aiming for cure in HBV and HDV infection. J. Hepatol. 65, 835–848 (2016).
Brancaccio, G., Fasano, M., Grossi, A., Santantonio, T. A. & Gaeta, G. B. Clinical outcomes in patients with hepatitis D, cirrhosis and persistent hepatitis B virus replication, and receiving long-term tenofovir or entecavir. Aliment Pharmacol. Ther. 49, 1071–1076 (2019).
Kamal, H. et al. Long-term study of hepatitis D infection at secondary care centers: The impact of viremia on liver-related outcomes. Hepatology 72(4), 1177–1190 (2020).
Acknowledgements
This work was supported in part by a grant from 1. Center for Liquid Biopsy (KMU-TC108B06) 2. Center for Cancer Research (KMU-TC108A04-3) 3. Cohort Research Center (KMU-TC108B07) 4. Kaohsiung Medical University (KMU-DK109002, MOST 108-2314-B-037-066-MY3) 5. Kaohsiung Medical University Hospital (KMUH108-8R05).
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T.Y.J. wrote the main manuscript text and C.F.H. prepared figures. All authors reviewed the manuscript.
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Ming-Lung Yu: Research support (grant) from Abbott, BMS, Gilead, and Merck. Consultant of Abbvie, Abbott, BMS, Gilead, Merck and Roche. Speaker of Abbvie, Abbott, BMS, Gilead, Merck, and IPSEN. Chung-Feng Huang: Speaker of Gilead, Abbie, Merck and BMS. Other authors share no competing interests.
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Jang, TY., Wei, YJ., Liu, TW. et al. Role of hepatitis D virus infection in development of hepatocellular carcinoma among chronic hepatitis B patients treated with nucleotide/nucleoside analogues. Sci Rep 11, 8184 (2021). https://doi.org/10.1038/s41598-021-87679-w
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DOI: https://doi.org/10.1038/s41598-021-87679-w
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