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Vol. 16. Issue 3.
Pages 412-420 (May - June 2017)
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  • Abstract
  • Keywords
  • Introduction
  • Material and methods
  • Results
    • Abstract
    • Keywords
    • Introduction
    • Material and methods
    • Patients
    • Follow-up and treatment for tumor recurrences
    • Evaluation of prognostic clinical and pathological variables
    • Statistical analysis
    • Results
    • Factors associated with overall survival in univariate and multivariate analyses
    • Factors associated with early and late recurrence after curative resection
    • Discussion
    • Abbreviations
    • Grants
    • Acknowledgements
    • Bibliography
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Vol. 16. Issue 3.
Pages 412-420 (May - June 2017)
DOI: 10.5604/01.3001.0009.8596
Open Access
Risk Factors for Prognosis of Hepatocellular Carcinoma After Curative Resection In Patients with Low Hepatitis B Viral Load
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Li-Shuai Qu, Jin-Xia Liu, Jing Zhu, Cui-Hua Lu
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lucuihua@yeah.net

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Department of Gastroenterology, Affiliated Hospital of Nantong University, Jiangsu Province, China
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Tables (4)
Table 1. Patient characteristics.
Table 2. Factors identified on univariate and multivariate Cox regression analyses that influenced overall survival in HCC patients undergoing curative resection.
Table 3. Factors identified on univariate and multivariate Cox regression analyses that influenced early recurrence (≤ 2 years) in HCC patients undergoing curative resection.
Table 4. Factors identified on univariate and multivariate Cox regression analyses that influenced late recurrence (> 2 years) in HCC patients undergoing curative resection.
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Abstract
Background

A retrospective cohort study was conducted to investigate the effect of hepatitis B surface antigen (HBsAg) level on prognosis in low viral load (< 2000 IU/mL) patients with hepatitis B-related hepatocellular carcinoma (HCC) after curative resection.

 Material and Methods

A total of 192 patients with low viral load who had received curative resection of pathologically confirmed HCC were analyzed to determine the factors affecting prognosis. The risk factors for survival, early and late recurrence (2 years as a cut-off) were studied.

 Results

The median follow-up time was 38.5 months. The overall survival rates at 1-, 3-, and 5-year after curative resection were 94.2%, 64.0%, and 45.2%, respectively. The cumulative recurrence rates at 1-, 3-, and 5-year after curative resection were 22.4%, 46.5%, and 67.0%, respectively. Patients with high serum HBsAg levels (> 250 IU/mL) had significantly lower survival rates than those with low HBsAg levels (HR: 1.517, 95% CI: 1.005-2.292, P = 0.047). Stratified analysis showed that patients with high HBsAg levels had a significantly higher late recurrence incidence than those with low HBsAg levels (HR: 2.155, 95% CI: 1.094-4.248, P = 0.026), but did not have a significantly higher risk of early recurrence postoperatively (HR: 1.320, 95% CI: 0.837-2.082, P = 0.233). Multivariate analysis revealed that HBsAg > 250 IU/mL was an independent risk factor associated with late recurrence (HR: 2.109, 95% CI: 1.068-4.165, P = 0.032).

 Conclusions

HBsAg > 250 IU/mL at the time of tumor resection was an independent risk factor for late recurrence in low viral load HCC patients.

Keywords:
HBsAg level
Hepatocellular carcinoma
Curative resection
Prognosis
Full Text
Introduction

Hepatocellular carcinoma (HCC) is a highly prevalent and lethal cancer type being the third leading cause of cancer-related deaths worldwide. Etiologically, HCC usually develops in chronic hepatitis B virus (HBV) carriers, especially in East Asia and sub-Saharan Africa, where HBV is endemic. For these HCC patients, curative tumor resection remains the most effective treatment and the prognosis of HCC was greatly improved. However, high opportunity of intrahepatic recurrence remains a major obstruction for further improving the prognosis of HCC patients after curative resection. It has been hypothesized that early and late intrahepatic recurrence of HCC was attributable to two different mechanisms: intrahepatic metastasis and de novo multicentric carcinogenicity, respectively. Imamura, et al. proposed a convenient framework to clinically differentiate each type of recurrence as ‘early’ or ‘late’ based on a cut-off of 2 years postoperatively. Potentially, risk factors including tumor size, nodule number, positive surgical margin, microvascular invasion, tumor node metastasis (TNM) stage, and Edmondson's grade were significantly related to early HCC recurrence. With successful risk surveillance of HCC development and curative resection, the development of early recurrence can be avoided in a higher number of patients, thereby helping them survive longer. Meanwhile, the risk factors contributing to late recurrence after surgery have not been investigated on a comprehensive basis. Although the precise mechanism underlying recurrent carcinogene-sis associated with HBV in the remaining liver in patients who have undergone curative therapy remains unclear, it is possible that viral replication and integration of sub-ge-nomic HBV DNA fragments into the host liver cells play a key role in contributing to the carcinogenic process. According to current opinions, there is sufficient and powerful evidence connecting elevated serum HBV DNA levels with an increased risk of HCC recurrence and death after curative resection. In particular, patients with serum HBV DNA levels > 2,000 IU/mL at study entry have an increased risk of HCC recurrence. In contrast, those with HBV DNA levels < 2,000 IU/mL are usually designated inactive or low-risk HBV carriers. However, even these low viral load patients still carry a high incidence of HCC recurrence. Therefore, it is necessary to identify factors other than viral load that are predictive of HCC in these low-risk patients. Recently, the quantification of hepatitis B surface antigen (HBsAg) level has been introduced as a surrogate marker for the management of chronic hepatitis B infection. A Taiwanese cohort study demonstrated that high HBsAg levels predicted the risk of HCC in hepatitis B e antigen (HBeAg) negative patients with low HBV DNA levels. Tseng, et al. also demonstrated that high HB-sAg levels could predict disease progression in HBeAg negative patients. However, there are only a few studies assessing the role of HBsAg levels as a risk factor of recurrence in HCC. Thus, the effect of HBsAg levels on HCC recurrence after curative resection in low viral load patients remains uncertain.

We therefore aimed to conduct a retrospective cohort study to assess the impact of serum HBsAg levels on the prognosis of HCC among patients with low viral load (< 2,000 IU/mL). In addition, based on the hypothesis that early and late intrahepatic recurrence of HCC was attributable to different mechanisms, we also investigated the risk factors for early (≤ 2 years) and late (> 2 years) intra-hepatic recurrence, separately.

Material and MethodsPatients

Between January 2009 and December 2011, 192 patients with HBV-related HCC who underwent curative resection as the primary therapy at the Affiliated Hospital of Nantong University were enrolled in this retrospective cohort study based on the following inclusion criteria:

  • Positive serum HBsAg for at least 12 months with a serum HBV DNA level < 2,000 IU/mL.

  • Complete resection of all tumor nodules and a surgical free margin of more than 5 mm by pathological examination.

  • No cancerous thrombus in the portal vein (main trunk or two major branches), hepatic veins, or bile duct.

  • No more than three tumor nodules.

  • No extrahepatic metastasis.

  • No adjuvant antiviral therapy with nucleoside analogue was given before or after the operation.

  • Death in the hospital not due to postoperative hepatic failure; and

  • Presence of early recurrence at least 3 months postop-eratively (excluding pre-existing metastases before HCC resection).

The histological grade proposed by Edmondson and Steiner, maximal tumor size, nodule number, capsular formation around the tumor, microvascular invasion, liver cirrhosis, and extent of resection were also determined. The protocol was approved by the Ethics Committee of the Affiliated Hospital of Nantong University in accordance with the tenets of the Declaration of Helsinki.

Follow-up and treatment for tumor recurrences

After surgical resection of HCC, all 192 patients were assessed every 3-6 months with dynamic contrast-enhanced computer tomography (CT) and/or magnetic resonance imaging (MRI), as well as with measurement of a serum tumor marker such as AFP. Hepatic angiography was performed when recurrence was suspected. Postoper-atively, 19 patients received interferon-alpha (IFN-α) treatment, which was started at a pilot dose of 3 million units (MU) two times a week by intramuscular injection for 2 weeks, then 5 MU three times a week for 18 months. The IFN-α treatment was terminated when recurrence was confirmed. Diagnosis of intrahepatic recurrence was based on histopathologic examination of tumor tissue in 23 patients undergoing repeat hepatic resection and on the characteristic appearance of CT, MRI, and hepatic angiog-raphy in 85 patients. When recurrence was confirmed, the patients received the optimal treatment modality for each case based on the number and location of the recurrent tumors and liver function tests. Treatment of recurrent HCC included repeat hepatic resection, radiofrequency ablation (RFA), percutaneous ethanol injection (PEI), chemotherapy or radiotherapy, and transcatheter arterial chemoembolization (TACE) and hepatic arterial infusion chemotherapy.

Evaluation of prognostic clinical and pathological variables

Clinical and pathological factors in this study were selected for their potential relationship to prognosis on the basis of previous studies, and included age (continuous variable), gender (male or female), alanine aminotransferase level (continuous variable), total bilirubin level (continuous variable), albumin level (continuous variable), prothrombin time (continuous variable), HBeAg status (positive or negative), serum HBsAg level (< 250 or > 250 IU/mL), co-existing hepatitis C virus (HCV) infection (yes or no), liver cirrhosis (yes or no), Child-Pugh grade (A or B), Okuda stage (I or II), serum AFP level (< 400 or > 400 ng/mL), tumor size (< 3 or > 3 cm in diameter), number of tumor nodules (single or multiple), tumor capsular formation (yes or no), microvascular invasion (yes or no), differentiation of tumor cells (Edmond-son's classification I/II or III/IV), postoperative IFN-cc therapy (yes or no), and extent of resection (minor, < 3 segments or major, > 3 segments) based on Couinaud's nomenclature. Serum HBV DNA levels were determined using the fluorescein quantitative polymerase chain reaction (FQ-PCR) detection system (TaqMan; Roche Diagnostics, Branchburg, NJ, USA). HBsAg level was quantified by the automated chemiluminescent micropar-ticle immunoassay (Architect HBsAg, Abbott, IL, USA). The detection range of the Architect HBsAg assay was 0.05 to 250 IU/mL.

Statistical analysis

Data were presented as means ± SD, proportions, or median (range). Clinical and pathological data at the time of resection were analyzed to identify factors that influenced prognosis via the Cox proportional hazards model. The overall survival rate was calculated from the date of resection to the date of death or last follow-up. The cumulative recurrence rates were calculated from the date of resection to the date when tumor recurrence was diagnosed, or if recurrence was not diagnosed at the time of study, cases were censored on the date of death or last follow-up. To investigate factors contributing to early and late recurrence separately, we set 2 years as the cut-off between early and late recurrence, as suggested by Imamura's study. Survival curves were calculated by the Kaplan-Meier method and differences were compared by the log-rank test. Multivari-ate analysis was performed by the Cox proportional hazards regression model. Statistical significance was defined by a P value < 0.05. Statistical analyses were performed using the Statistical Program for Social Sciences (SPSS v.11.5 for Windows; SPSS, Inc., Chicago, IL, USA).

Results

During a median observation period of 38.5 months (with a range of 3 to 72 months), recurrence was found in 108 patients (56.3%). Of these, 23 patients received a second resection, 7 patients received RFA, 56 patients received TACE, 14 patients received chemotherapy or radiotherapy or PEI, and the remainder received a conservative treatment. During follow-up, 91 patients died, 14 of whom did not have recurrent HCC but died due to other causes, mainly chronic deterioration of liver function and massive upper digestive tract bleeding caused by es-ophageal varices. The overall survival rates at 1-, 3-, and 5-year after curative resection were 94.2%, 64.0%, and 45.2%, respectively. The cumulative recurrence rates at 1-, 3-, and 5-year after curative resection were 22.4%, 46.5%, and 67.0%, respectively. The baseline demographic, clinical, and pathological features of the study population are depicted in table 1.

Table 1.

Patient characteristics.

Characteristics  N (%)  Values 
Patients (n)  192 (100)   
Median age, years (range)    50 (26-78) 
Male: female ratio  163:29 (84.9:15.1)   
Co-existing HCV infection  5 (2.6)   
Presence of cirrhosis  144 (75.0)   
HBeAg seropositivity  64 (33.3)   
HBsAg > 250 IU/mL  83 (43.2)   
AFP > 400 ng/mL  38 (19.8)   
Median baseline biochemistry and hematology (range)     
Total bilirubin, μmol/L    15.8 (5.3-38.8) 
Albumin, g/L    42 (30-52) 
Aminotransferase, IU/L    43.5 (10-324) 
Prothrombin time, s    11.4 (9.5-15.3) 
Tumor size (≤ 3 cm:> 3 cm)  84:108 (43.8:56.3)   
Tumor number (Single:multiple)  156:36 (81.3:18.8)   
Microvascular invasion  45 (23.4)   
Capsular formation  107 (55.7)   
Differentiation of tumor (I/II:III/IV)  134:58 (69.8:30.2)   
Child-Turcotte-Pugh grade     
182 (94.8)   
10 (5.2)   
Okuda stage I  179 (93.2)   
I I  13 (6.8)   
Type of surgical procedure (major:minor)  74:118 (38.5:61.5)   
Postoperative IFN-α treatment  19 (9.9)   
Median follow-up time (months)    38.5 (3-72) 
Median time of recurrence (months)    24.5 (3-66) 
Median time of survival (months)    50.5 (5-69.8) 
Factors associated with overall survival in univariate and multivariate analyses

In the univariate analysis, serum HBsAg level > 250 IU/mL (hazards ratio (HR): 1.517, 95% confidence interval (CI): 1.005 - 2.292, P = 0.047), tumor size > 3 cm in diameter (HR: 1.673, 95% CI: 1.086 - 2.577, P = 0.020), and presence of microvascular invasion (HR: 1.751, 95% CI: 1.115 -2.750, P = 0.015) were significantly associated with poor overall survival postoperatively. Other clinical factors including sex, age, co-existing HCV infection, serum albumin level, total bilirubin level, aminotransferase level, prothrombin time, HBeAg status, presence of cirrhosis, tumor number, Child-Pugh grade, Okuda stage, extent of resection, and postoperative IFN-α treatment were not associated with survival (Table 2). The 1-, 3-, and 5-year overall survival rates for high HBsAg level patients (> 250 IU/mL) were 91.4%, 57.1%, and 35.4%, respectively, in contrast to 96.3%, 69.1%, and 52.0%, respectively, for low HBsAg level patients (≤ 250 IU/mL). Patients with high serum HBsAg levels had significantly lower survival rates than those with low HBsAg levels (log rank P = 0.045; Figure 1). However, in the multivariate analysis, the presence of microvascular invasion (HR: 1.740, 95% CI: 1.108 -2.734, P = 0.016) was the only independent risk factor for overall survival (Table 2).

Table 2.

Factors identified on univariate and multivariate Cox regression analyses that influenced overall survival in HCC patients undergoing curative resection.

Factors  P value  Hazard ratio  95% CI 
Univariate analysis       
Sex (male vs. female)  0.614  1.158  0.654-2.052 
Age, years  0.242  1.012  0.992-1.032 
Co-existing HCV infection  0.235  0.303  0.042-2.174 
Presence of cirrhosis  0.220  1.381  0.824-2.315 
HBeAg seropositivity  0.766  1.068  0.692-1.649 
HBsAg > 250 IU/mL  0.047  1.517  1.005-2.292 
AFP > 400 ng/mL  0.408  1.229  0.754-2.004 
Total bilirubin  0.134  1.022  0.993-1.053 
Albumin  0.225  0.970  0.923-1.019 
Aminotransferase  0.201  1.003  0.998-1.007 
Prothrombin time, s  0.217  1.111  0.940-1.312 
Tumor size (> 3 cm vs. ≤ 3 cm)  0.020  1.673  1.086-2.577 
Tumor number (multiple vs. single)  0.723  1.098  0.653-1.846 
Microvascular invasion  0.015  1.751  1.115-2.750 
Capsular formation  0.496  0.867  0.574-1.308 
Differentiation (III/IV vs. I/II)  0.844  0.956  0.609-1.500 
Child -Pugh grade (B vs. A)  0.067  2.065  0.950-4.489 
Okuda stage (II vs. I)  0.139  1.795  0.827-3.896 
Extent of resection (major vs. minor)  0.505  1.154  0.757-1.760 
Postoperative IFN-α treatment  0.078  0.444  0.180-1.094 
Multivariate analysis       
Microvascular invasion  0.016  1.740  1.108-2.734 
Comparison of overall survival rates after curative resection between different serum HBsAg levels at the time of tumor resection (log-rank test, P = 0.045).
Figure 1.

Comparison of overall survival rates after curative resection between different serum HBsAg levels at the time of tumor resection (log-rank test, P = 0.045).

(0.08MB).
Factors associated with early and late recurrence after curative resection

During follow-up, 108 patients had HCC recurrence. The median time from tumor resection to the detection of recurrence was 24.5 months (with a range of 3 to 66 months). Factors related to early recurrence (≤ 2 years) and late recurrence (> 2 years) were investigated separately, as suggested by Imamura's study4 (Tables 3 and 4).

Table 3.

Factors identified on univariate and multivariate Cox regression analyses that influenced early recurrence (≤ 2 years) in HCC patients undergoing curative resection.

Factors  P value  Hazard ratio  95% CI 
Univariate analysis       
Sex (male vs. female)  0.949  0.980  0.528-1.819 
Age, years  0.343  0.989  0.968-1.011 
Co-existing HCV infection  0.307  1.826  0.575-5.799 
Presence of cirrhosis  0.282  1.365  0.774-2.405 
HBeAg seropositivity  0.965  0.989  0.611-1.602 
HBsAg > 250 IU/mL  0.233  1.320  0.837-2.082 
AFP > 400 ng/mL  0.006  2.014  1.223-3.316 
Total bilirubin  0.849  0.997  0.965-1.030 
Albumin  0.838  1.006  0.953-1.061 
Aminotransferase  0.223  1.003  0.998-1.007 
Prothrombin time, s  0.231  0.886  0.727-1.080 
Tumor size (> 3 cm vs. ≤ 3 cm)  0.001  2.285  1.377-3.791 
Tumor number (multiple vs. single)  0.642  0.868  0.477-1.579 
Microvascular invasion  < 0.001  2.546  1.595-4.064 
Capsular formation  0.040  0.620  0.392-0.979 
Differentiation (III/IV vs. I/II)  0.530  1.179  0.706-1.969 
Child -Pugh grade (B vs. A)  0.490  1.377  0.555-3.418 
Okuda stage (II vs. I)  0.709  0.825  0.301-2.261 
Extent of resection (major vs. minor)  0.800  1.062  0.666-1.694 
Postoperative IFN-α treatment  0.080  0.407  0.148-1.115 
Multivariate analysis       
AFP > 400 ng/mL  0.047  1.679  1.007-2.801 
Tumor size > 3 cm  0.020  1.871  1.103-3.175 
Microvascular invasion  0.011  1.917  1.163-3.159 
Table 4.

Factors identified on univariate and multivariate Cox regression analyses that influenced late recurrence (> 2 years) in HCC patients undergoing curative resection.

Factors  P value  Hazard ratio  95% CI 
Univariate analysis       
Sex (male vs. female)  0.116  3.148  0.752-13.180 
Age, years  0.444  1.013  0.980-1.048 
Co-existing HCV infection  0.241  2.356  0.563-9.865 
Presence of cirrhosis  0.033  2.821  1.089-7.310 
HBeAg seropositivity  0.290  1.449  0.729-2.879 
HBsAg > 250 IU/mL  0.026  2.155  1.094-4.248 
AFP > 400 ng/mL  0.232  1.721  0.707-4.191 
Total bilirubin  0.406  1.023  0.970-1.078 
Albumin  0.551  0.975  0.898-1.059 
Aminotransferase  0.757  0.999  0.990-1.008 
Prothrombin time, s  0.542  0.912  0.679-1.226 
Tumor size (> 3 cm vs. ≤ 3 cm)  0.108  1.749  0.885-3.456 
Tumor number (multiple vs. single)  0.014  2.504  1.206-5.200 
Microvascular invasion  0.101  2.012  0.872-4.640 
Capsular formation  0.997  0.999  0.505-1.976 
Differentiation (III/IV vs. I/II)  0.929  1.034  0.494-2.166 
Child -Pugh grade (B vs. A)  0.712  1.457  0.198-10.694 
Okuda stage (II vs. I)  0.432  1.780  0.423-7.493 
Extent of resection (major vs. minor)  0.560  0.803  0.383-1.680 
Postoperative IFN-α treatment  0.477  0.684  0.240-1.948 
Multivariate analysis       
HBsAg > 250 copies/mL  0.032  2.109  1.068-4.165 
Multiple tumor number  0.017  2.446  1.172-5.104 

Among 192 patients, 74 had recurrence within 2 years. Stratified Cox regression analysis identified four variables as factors related to early recurrence: AFP > 400 ng/mL (HR: 2.014, 95% CI: 1.223 - 3.316, P = 0.006), tumor size > 3 cm in diameter (HR: 2.285, 95% CI: 1.377-3.791, P = 0.001), presence of microvascular invasion (HR: 2.546, 95% CI: 1.595 - 4.064, P < 0.001), and presence of capsular formation (HR: 0.620, 95% CI: 0.392-0.979, P = 0.040). The presence of high HBsAg levels was not associated with a significantly higher cumulative risk of tumor recurrence during first 2 years after curative resection (log rank P = 0.227). In the multivariate analysis, AFP > 400 ng/mL (HR: 1.679, 95% CI: 1.007 - 2.801, P = 0.047), tumor size > 3 cm in diameter (HR: 1.871, 95% CI: 1.103-3.175, P = 0.020), and presence of microvascular invasion (HR: 1.917, 95% CI: 1.163-3.159, P = 0.011) were independently associated with early tumor recurrence.

Factors related to late recurrence were investigated in 96 patients who were recurrence-free during the first 2 years. Recurrence was detected in 34 patients during follow-up. Univariate analysis identified three risk factors contributing to late recurrence: the presence of cirrhosis (HR: 2.821, 95% CI: 1.089 - 7.310, P = 0.033), multiple tumor number (HR: 2.504, 95% CI: 1.206 - 5.200, P = 0.014), and serum HBsAg > 250 IU/mL (HR: 2.155, 95% CI: 1.094 - 4.248, P = 0.026). Patients with high HBsAg levels at resection had a significantly higher cumulative late recurrence rate than those with low HBsAg levels (log rank P = 0.022; Figure 2). In the multivariate analysis, the presence of multiple tumor nodules (HR: 2.446, 95% CI: 1.172-5.104, P = 0.017) and serum HBsAg > 250 IU/mL (HR: 2.109, 95% CI: 1.068 - 4.165, P = 0.032) were independent risk factors associated with late recurrence.

Cumulative late recurrence (> 2 years) related to the initial HBsAg levels at the time of tumor resection (log-rank test, P = 0.022).
Figure 2.

Cumulative late recurrence (> 2 years) related to the initial HBsAg levels at the time of tumor resection (log-rank test, P = 0.022).

(0.07MB).
Discussion

In this retrospective cohort study, we focused primarily on the correlation between serum HBsAg levels and prognosis of HBV-related HCC patients with low viral load (< 2,000 IU/L) after curative resection. Multivariate analysis demonstrated that early recurrence was independently associated with the presence of microvascular invasion, AFP > 400 ng/mL, and tumor size > 3 cm in diameter. On the other hand, the risk factors for late recurrence were high HBsAg levels (> 250 IU/mL) and the presence of multiple tumor number. However, the presence of microvascular invasion was the only independent risk factor related to overall survival in low viral load subjects after curative resection.

Previous studies have confirmed that high AFP level, tumor size, multiple nodule number, vascular invasion, a positive surgical margin, and Edmondson's grade are prognostic factors predicting tumor recurrence after curative resection. Early recurrence, which appears with 2 years postoperatively, is associated with tumor-related factors; late recurrence appears > 2 years postoperatively, and is considered to be associated with hepatic inflammation and viral replication. The latter is clonally independent from the primary tumor. However, there has been a paucity of studies concerning the HBV status of patients undergoing HCC resection in the past, probably due in part to the lack of interest in hepatitis virology among liver surgeons who manage these patients. Till date, several studies assessing the effect of HBV status on the prognosis of HCC patients receiving curative resection have been reported. Some potential viral risk factors associated with prognosis have been identified, such as seropositivity of HBeAg, high viral load, genotype, and specific viral sequence mutations. Among these factors, an elevated serum HBV DNA level is widely considered to be the most important risk factor for the poor prognosis of HCC patients after tumor resection, as well as for cases most suitable for intervention. In some case series studies on the recurrence of HBV-related HCC after curative resection, patients with a high viral load at study entry had a significantly higher risk of tumor recurrence than those with a low viral load. In our previous study, during a mean follow-up period of 33.7 months after curative resection, we found that serum HBV DNA levels of 104 copies/mL or more at pre-operation was an independent risk factor for HCC recurrence. However, even in these low viral load patients who received tumor resection, the risk of tumor recurrence 2 years postoperatively remained. Recently, the introduction of HBsAg quantification has attracted much attention for its value in stratifying the risk of disease progression and predicting the prognosis of patients with chronic HBV infection. A Taiwanese cohort study demonstrated that high HBsAg levels predicted the risk of HCC in HBeAg-negative patients with low HBV DNA levels.16 However, the role of HBsAg in the recurrence of HBV-related HCC in low HBV DNA level subjects was seldom reported yet. In this study, we evaluated the role of serum HBsAg levels on the prognosis of low viral load HCC patients (< 2,000 IU/mL). Our results revealed that in a subgroup of 96 patients who were recurrence-free for first 2 years, the presence of multiple tumor nodules and HBsAg > 250 IU/mL were independent risk factors for late recurrence. However, high HBsAg levels were not associated with early tumor recurrence or overall survival in the multivariate analysis. In a recent study, Huang, et al. also confirmed that a preoperative serum HBsAg ≥ 1,000 IU/mL was an independent risk factor for HCC recurrence in patients with low HBV DNA levels. In our latest meta-analysis, despite recommended cutoffs and significant heterogeneity among the different included studies, the results still supported the opinion that the presence of high HBsAg level was associated with a high risk of late recurrence after curative resection of HCC, although the rate of early recurrence was not higher in high HBsAg patients compared to the patients with low HBsAg level.

The precise mechanism for recurrent carcinogenesis associated with high HBsAg levels in patients with chronic HBV infection remains unclear. As we known, HBsAg is the hallmark of HBV infection and was first reported by Blumberg, et al. in 1968. Measurement of HBsAg is usually used to identify HBV infection. The level of serum HB-sAg reflects the transcriptional activity of covalently closed circular DNA (cccDNA). It is generally believed that serum HBsAg concentration is significantly correlated with intrahepatic amounts of total HBV DNA and cccDNA. HBsAg is mainly derived from the integrated form of HBV DNA rather than the episomal form, and patients with a low viral load who have high HBsAg levels may have more hepatocytes with HBV integration than those who have low HBsAg levels. It has been speculated that the higher risk of HCC in high HBsAg level patients might be attributed to the increased genomic instability as a result of integrated viral sequences, which plays an important role in hepatocarcinogenesis. Additionally, in theory, late recurrence (> 2 years) has been speculated to be associated with the background liver disease condition, such as hepatic inflammation and liver damage. High HB-sAg levels in patients may indicate higher cccDNA levels and confer further increased viral replication, leading to even higher HCC risk. When these lines of evidence are taken together, these studies may provide a new insight into the role of serum HBsAg levels in the recurrence of HBV-related HCC after curative resection. Based on our data, preoperative measurement of HBsAg levels in addition to HBV DNA levels could be used as a potential clinical marker useful for the prediction of prognosis in HBV-related HCC.

Other independent risk factors associated with HCC prognosis after curative resection that were identified in this study included preoperative AFP ≥ 400 ng/mL, multiple tumor number, and the presence of microvascular invasion. These findings were consistent with those described previously. Patients with high AFP level tended to have greater tumor size, bilobar involvement, massive or diffuse types, and tumor vascular invasion. The presence of microvascular invasion was consistently reported as strongly predictive of intrahepatic metastasis. Meanwhile, tumor multiplicity was thought to be a variable reflecting increased carcinogenicity of the background liver tissue. Our stratified analysis demonstrated that the presence of multiple tumor nodules was an independent risk factor for late recurrence. This finding strongly supported the hypothesis that late recurrence was mainly attributable to de novo multicentric carcinogenicity.

There is strong evidence linking elevation in serum HBV DNA levels and HCC recurrence after tumor resection in chronic hepatitis B. In the present study, we further showed that high HBsAg levels (> 250 IU/mL) were associated with a significantly higher later recurrence rate after curative resection in low viral load patients. There are also several limitations in this study. First, HB-sAg quantification was based on a single blood sample obtained at surgery; therefore, we could not assess the risk of fluctuation in serum HBsAg levels during follow-up on the prognosis of HCC. Second, as a retrospective cohort study, it is difficult to reach a firm conclusion and a large-scale, well-designed prospective study with long-term follow-up should be conducted to solve this issue in the future.

In summary, we found that the independent risk factors for early recurrence after curative resection of HBV-relat-ed HCC were the presence of microvascular invasion, AFP > 400 ng/mL, and tumor size > 3 cm in diameter. Meanwhile, late recurrence was associated with high preoperative HBsAg levels and multiple tumor number at resection in low viral load HCC subjects. If the role of HBsAg levels in predicting HBV-related HCC prognosis after curative resection is further confirmed, this new potential biomarker could be incorporated into the risk calculator for HCC recurrence, particularly in patients with low viral load.

Abbreviations

  • CI: Confidence interval.

  • HBsAg: Hepatitis B surface antigen.

  • HBV: Hepatitis B virus.

  • HCC: Hepatocellular carcinoma.

  • HR: Hazards ratio.

Grants

The study was financially supported by National Nature Science Foundation of China (No. 81302056), China Ministry of Health (W201202), Natural Science Foundation of Jiangsu Province (BK2012225), and Foundation of Jiangsu Province (WS056).

Acknowledgements

The authors thank all the patients and clinical investigators who are involved in the studies included in this study.

Conflicts of Interest

None.
References
[1.]
Llovet J.M., Burroughs A., Bruix J..
Hepatocellular carcinoma.
Lancet, 362 (2003), pp. 1907-1917
http://dx.doi.org/10.1016/S0140-6736(03)14964-1 | Medline
[2.]
Kao J.H., Chen D.S..
Global control of hepatitis B virus infection.
Lancet Infect Dis, 2 (2002), pp. 395-403
Medline
[3.]
Lavanchy D..
Hepatitis B virus epidemiology, disease burden, treatment, and current and emerging prevention and control measures.
J Viral Hepat, 11 (2004), pp. 97-107
Medline
[4.]
Imamura H., Matsuyama Y., Tanaka E., Ohkubo T., Hasegawa K., Miyagawa S., Sugawara Y., et al.
Risk factors contributing to early and late phase intrahepatic recurrence of hepatocellular carcinoma after hepatectomy.
J Hepatol, 38 (2003), pp. 200-207
Medline
[5.]
Poon R.T., Fan S.T., Ng I.O., Lo C.M., Liu C.L., Wong J..
Different risk factors and prognosis for early and late intrahepatic recurrence after resection of hepatocellular carcinoma.
Cancer, 89 (2000), pp. 500-507
Medline
[6.]
Tung-Ping Poon R., Fan S.T., Wong J..
Risk factors, prevention, and management of postoperative recurrence after resection of hepatocellular carcinoma.
Ann Surg, 232 (2000), pp. 10-24
http://dx.doi.org/10.1097/00000658-200007000-00003 | Medline
[7.]
Cha C., Fong Y., Jarnagin W.R., Blumgart L.H., DeMatteo R.P..
Predictors and patterns of recurrence after resection of hepatocellular carcinoma.
J Am Coll Surg, 197 (2003), pp. 753-758
http://dx.doi.org/10.1016/j.jamcollsurg.2003.07.003 | Medline
[8.]
Utsunomiya T., Shimada M., Taguchi K.I., Hasegawa H., Ya-mashita Y., Hamatsu T., Aishima S.I., et al.
Clinicopathologic features and postoperative prognosis of multicentric small hepatocellular carcinoma.
J Am Coll Surg, 190 (2000), pp. 331-335
Medline
[9.]
Huang Y., Tong S., Tai A.W., Hussain M., Lok A.S..
Hepatitis B virus core promoter mutations contribute to hepatocarcinogen-esis by deregulating SKP2 and its target, p21.
Gastroenterology, 141 (2011), pp. 1412-1421
http://dx.doi.org/10.1053/j.gastro.2011.06.048 | Medline
[10.]
Mun H.S., Lee S.A., Kim H., Hwang E.S., Kook Y.H., Kim B.J..
Novel F141L pre-S2 mutation in hepatitis B virus increases the risk of hepatocellular carcinoma in patients with chronic genotype C infections.
J Virol, 85 (2011), pp. 123-132
http://dx.doi.org/10.1128/JVI.01524-10 | Medline
[11.]
Pan J., Clayton M., Feitelson M.A..
Hepatitis B virus X antigen promotes transforming growth factor-beta1 (TGF-beta1) activity by up-regulation of TGF-beta1 and down-regulation of alpha2-macroglobulin.
J Gen Virol, 85 (2004), pp. 275-282
http://dx.doi.org/10.1099/vir.0.19650-0 | Medline
[12.]
Kubo S., Hirohashi K., Tanaka H., Tsukamoto T., Shuto T., Yamamoto T., Ikebe T., et al.
Effect of viral status on recurrence after liver resection for patients with hepatitis B virus-related hepatocellular carcinoma.
Cancer, 88 (2000), pp. 1016-1024
Medline
[13.]
Hung I.F., Poon R.T., Lai C.L., Fung J., Fan S.T., Yuen M.F..
Recurrence of hepatitis B-related hepatocellular carcinoma is associated with high viral load at the time of resection.
Am J Gastroenterol, 103 (2008), pp. 1663-1673
http://dx.doi.org/10.1111/j.1572-0241.2008.01872.x | Medline
[14.]
Wu J.C., Huang Y.H., Chau G.Y., Su C.W., Lai C.R., Lee P.C., Huo T.I., et al.
Risk factors for early and late recurrence in hepatitis B-related hepatocellular carcinoma.
J Hepatol, 51 (2009), pp. 890-897
http://dx.doi.org/10.1016/j.jhep.2009.07.009 | Medline
[15.]
Qu L.S., Jin F., Huang X.W., Shen X.Z..
High hepatitis B viral load predicts recurrence of small hepatocellular carcinoma after curative resection.
J Gastrointest Surg, 14 (2010), pp. 1111-1120
http://dx.doi.org/10.1007/s11605-010-1211-1 | Medline
[16.]
Tseng T.C., Liu C.J., Yang H.C., Su T.H., Wang C.C., Chen C.L., Kuo S.F., et al.
High levels of hepatitis B surface antigen increase risk of hepatocellular carcinoma in patients with low HBV load.
Gastroenterology, 142 (2012), pp. 1140-1149
http://dx.doi.org/10.1053/j.gastro.2012.02.007 | Medline
[17.]
Tseng T.C., Liu C.J., Yang H.C., Su T.H., Wang C.C., Chen C.L., Hsu C.A., et al.
Serum hepatitis B surface antigen levels help predict disease progression in patients with low hepatitis B virus loads.
Hepatology, 57 (2013), pp. 441-450
http://dx.doi.org/10.1002/hep.26041 | Medline
[18.]
Sohn W., Paik Y.H., Kim J.M., Kwon C.H., Joh J.W., Cho J.Y., Gwak G.Y., et al.
HBV DNA and HBsAg levels as risk predictors of early and late recurrence after curative resection of HBV-re-lated hepatocellular carcinoma.
Ann Surg Oncol, 21 (2014), pp. 2429-2435
http://dx.doi.org/10.1245/s10434-014-3621-x | Medline
[19.]
Huang G., Lau W.Y., Zhou W.P., Shen F., Pan Z.Y., Yuan S.X., Wu M.C..
Prediction of Hepatocellular Carcinoma Recurrence in Patients With Low Hepatitis B Virus DNA Levels and High Pr-eoperative Hepatitis B Surface Antigen Levels.
JAMA Surg, 149 (2014), pp. 519-527
http://dx.doi.org/10.1001/jamasurg.2013.4648 | Medline
[20.]
Chen Y.J., Yeh S.H., Chen J.T., Wu C.C., Hsu M.T., Tsai S.F., Chen P.J., et al.
Chromosomal changes and clonality relationship between primary and recurrent hepatocellular carcinoma.
Gas-troenterology, 119 (2000), pp. 431-440
[21.]
Sun H.C., Zhang W., Qin L.X., Zhang B.H., Ye Q.H., Wang L., Ren N., et al.
Positive serum hepatitis B e antigen is associated with higher risk of early recurrence and poorer survival in patients after curative resection of hepatitis B-related hepa-tocellular carcinoma.
. J Hepatol, 47 (2007), pp. 684-690
http://dx.doi.org/10.1016/j.jhep.2007.06.019 | Medline
[22.]
Yang T., Lu J.H., Zhai J., Lin C., Yang G.S., Zhao R.H., Shen F., et al.
High viral load is associated with poor overall and recurrence-free survival of hepatitis B virus-related hepatocellu-lar carcinoma after curative resection: a prospective cohort study.
Eur J Surg Oncol, 38 (2012), pp. 683-691
http://dx.doi.org/10.1016/j.ejso.2012.04.010 | Medline
[23.]
Liang T.J., Mok K.T., Liu S.I., Huang S.F., Chou N.H., Tsai C.C., Chen I.S., et al.
Hepatitis B genotype C correlated with poor surgical outcomes for hepatocellular carcinoma.
J Am Coll Surg, 211 (2010), pp. 580-586
http://dx.doi.org/10.1016/j.jamcollsurg.2010.06.020 | Medline
[24.]
Yeh C.T., So M., Ng J., Yang H.W., Chang M.L., Lai M.W., Chen T.C., et al.
Hepatitis B virus-DNA level and basal core promoter A1762T/G1764A mutation in liver tissue independently predict postoperative survival in hepatocellular carcinoma.
Hepatology, 52 (2010), pp. 1922-1933
http://dx.doi.org/10.1002/hep.23898 | Medline
[25.]
Su C.W., Chiou Y.W., Tsai Y.H., Teng R.D., Chau G.Y., Lei H.J., Hung H.H., et al.
The Influence of Hepatitis B Viral Load and Pre-S Deletion Mutations on Post-Operative Recurrence of Hepatocellular Carcinoma and the Tertiary Preventive Effects by Anti-Viral Therapy.
PLoS One, 8 (2013), pp. e66457
http://dx.doi.org/10.1371/journal.pone.0066457 | Medline
[26.]
Qu L.S., Liu J.X., Zhang H.F., Zhu J., Lu C.H..
Effect of serum hepatitis B surface antigen levels on predicting the clinical outcomes of chronic hepatitis B infection: A meta-analysis.
Hepatol Res,
[27.]
Blumberg B.S., Sutnick A.I., London W.T..
Hepatitis and leukemia: their relation to Australia antigen.
Bull N Y Acad Med, 44 (1968), pp. 1566-1586
Medline
[28.]
Chan H.L., Wong V.W., Tse A.M., Tse C.H., Chim A.M., Chan H.Y., Wong G.L., et al.
Serum hepatitis B surface antigen quantita-tion can reflect hepatitis B virus in the liver and predict treatment response.
Clin Gastroenterol Hepatol, 5 (2007), pp. 1462-1468
http://dx.doi.org/10.1016/j.cgh.2007.09.005 | Medline
[29.]
Nguyen T., Thompson A.J., Bowden S., Croagh C., Bell S., Desmond P.V., Levy M., et al.
Hepatitis B surface antigen levels during the natural history of chronic hepatitis B: a perspective on Asia.
J Hepatol, 52 (2010), pp. 508-513
http://dx.doi.org/10.1016/j.jhep.2010.01.007 | Medline
[30.]
Brunetto M.R..
A new role for an old marker, HBsAg.
J Hepa-tol, 52 (2010), pp. 475-477
[31.]
Kumada T., Nakano S., Takeda I., Sugiyama K., Osada T., Kiriya-ma S., Sone Y., et al.
Patterns of recurrence after initial treatment in patients with small hepatocellular carcinoma.
. Hepatology, 25 (1997), pp. 87-92
http://dx.doi.org/10.1053/jhep.1997.v25.pm0008985270 | Medline
[32.]
Jaroszewicz J., Calle Serrano B., Wursthorn K., Deterding K., Schlue J., Raupach R., Flisiak R., et al.
Hepatitis B surface antigen (HBsAg) levels in the natural history of hepatitis B virus (HBV)-infection: a European perspective.
J Hepatol, 52 (2010), pp. 514-522
http://dx.doi.org/10.1016/j.jhep.2010.01.014 | Medline
[33.]
Werle-Lapostolle B., Bowden S., Locarnini S., Wursthorn K., Petersen J., Lau G., Trepo C., et al.
Persistence of cccDNA during the natural history of chronic hepatitis B and decline during adefovir dipivoxil therapy.
Gastroenterology, 126 (2004), pp. 1750-1758
Medline
[34.]
Ikai I., Arii S., Kojiro M., Ichida T., Makuuchi M., Matsuyama Y., Nakanuma Y., et al.
Reevaluation of prognostic factors for survival after liver resection in patients with hepatocellular carcinoma in a Japanese nationwide survey.
Cancer, 101 (2004), pp. 796-802
http://dx.doi.org/10.1002/cncr.20426 | Medline
[35.]
Sumie S., Kuromatsu R., Okuda K., Ando E., Takata A., Fukushi-ma N., Watanabe Y., et al.
Microvascular invasion in patients with hepatocellular carcinoma and its predictable clinico-pathological factors.
Ann Surg Oncol, 15 (2008), pp. 1375-1382
http://dx.doi.org/10.1245/s10434-008-9846-9 | Medline
[36.]
Tangkijvanich P., Anukulkarnkusol N., Suwangool P., Lertma-harit S., Hanvivatvong O., Kullavanijaya P., Poovorawan Y..
Clinical characteristics and prognosis of hepatocellular carcinoma: analysis based on serum alpha-fetoprotein levels.
. J Clin Gastroenterol, 31 (2000), pp. 302-308
Medline
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