PAGE-B Score Calculator- Free HCC Risk Prediction Tool for Chronic Hepatitis B

PAGE-B Score Calculator – Free HCC Risk Tool for Hepatitis B | Super-Calculator.com

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Important Medical Disclaimer

This calculator is provided for informational and educational purposes only. It is not intended to replace professional medical advice, diagnosis, or treatment. Always consult with a qualified healthcare professional before making any medical decisions. The results from this calculator should be used as a reference guide only and not as the sole basis for clinical decisions.

PAGE-B Score Calculator

Estimate 5-year hepatocellular carcinoma (HCC) risk in treated chronic hepatitis B using the validated PAGE-B scoring system – enter platelet count, patient age, and sex to receive an instant HCC risk category, reference range display, and clinical surveillance guidance based on Papatheodoridis et al. 2016.

Patient Age (years) 55

Sex

Platelet Count (x10^9/L) 185

PAGE-B Total Score

out of 24 maximum points

Where Your PAGE-B Score Falls on the HCC Risk Scale

Low Risk (0 to 9) Intermediate (10 to 17) High Risk (18 to 24)

5-Year HCC Risk Category

INTERMEDIATE RISK

Estimated 5-year HCC probability: approximately 3 to 5%

Component Reference Range Panel

Age Component 6 / 10 pts Moderate

0 pts (age 16-29)10 pts (age 70+)

Platelet Count Component 4 / 8 pts Reduced

0 pts (200+ x10^9/L)8 pts (below 100)

Sex Component 6 / 6 pts Male

0 pts (Female)6 pts (Male)

Surveillance Protocol: Mandatory 6-monthly abdominal ultrasound surveillance. Consider supplementary AFP measurement and liver stiffness assessment (FibroScan) to further refine individual HCC risk stratification.

PAGE-B risk classification based on Papatheodoridis et al. Gastroenterology 2016. Current patient score highlighted in the table.

PAGE-B Score	Risk Category	5-Year HCC Risk	Surveillance Recommendation
0 to 9	Low Risk	~1%	Standard 6-monthly ultrasound
10 to 17	Intermediate Risk	~3 to 5%	6-monthly ultrasound, consider AFP and LSM
18 to 24	High Risk	~10%+	Intensive surveillance, specialist referral

Detailed scoring criteria for each PAGE-B component. Current patient values highlighted. Maximum total score is 24 points.

Component	Criterion	Points	Clinical Basis
Age	16 to 29 years	0	Lowest cumulative HBV exposure
Age	30 to 39 years	2	Early accumulation of viral injury
Age	40 to 49 years	4	Moderate fibrosis accumulation
Age	50 to 59 years	6	Advanced fibrosis risk period
Age	60 to 69 years	8	High cumulative injury burden
Age	70 years or older	10	Highest age-related HCC risk
Sex	Female	0	Hormonal protection, lower androgen effect
Sex	Male	6	2-4x higher HCC incidence than female
Platelet Count	200 x10^9/L or above	0	Normal – preserved liver architecture
Platelet Count	100 to 199 x10^9/L	4	Mild portal hypertension, moderate fibrosis
Platelet Count	Below 100 x10^9/L	8	Severe portal hypertension, cirrhosis likely

How different patient profiles score on the PAGE-B scale. Your current score is shown for comparison.

Patient Profile	PAGE-B Score	Risk Category
Female, age 25, platelets 250	0	Low
Male, age 35, platelets 220	8	Low
Male, age 45, platelets 160	14	Intermediate
Your patient (score 16)	16	Intermediate
Male, age 55, platelets 150	16	Intermediate
Male, age 65, platelets 90	22	High
Male, age 70+, platelets below 100	24	High

Important Medical Disclaimer

About This PAGE-B Score Calculator

This PAGE-B score calculator is designed for hepatologists, gastroenterologists, specialist nurses, and primary care clinicians managing adults with chronic hepatitis B on antiviral therapy. It calculates the validated PAGE-B score – a three-variable clinical tool that estimates the 5-year risk of hepatocellular carcinoma (HCC) in patients receiving nucleos(t)ide analogue treatment. By entering the patient’s age, biological sex, and most recent platelet count, clinicians receive an instant total score from 0 to 24, a visual zone bar showing where the score falls on the low, intermediate, or high HCC risk scale, and a per-component reference range panel displaying the individual contribution of each variable.

The calculator applies the scoring algorithm derived by Papatheodoridis and colleagues (Gastroenterology, 2016): age contributes 0 to 10 points in 2-point increments per decade from age 30, male sex contributes 6 points reflecting the 2 to 4 times higher HCC incidence in men, and platelet count contributes 0, 4, or 8 points based on thresholds of 200, 100 to 199, or below 100 x10^9/L – each threshold representing increasing degrees of portal hypertension and liver fibrosis. The three tabs below the calculator provide a PAGE-B severity reference table, a detailed scoring criteria breakdown, and a score comparison table showing how the current patient’s result compares against representative clinical profiles.

The PAGE-B score fills a practical clinical need: once antiviral therapy normalises viral load and ALT levels, viral parameters lose discriminative power and simpler models based on routinely available data become more reliable for ongoing HCC risk stratification. This tool enables clinicians to calculate and document the PAGE-B score at each clinic visit, identify patients in the high-risk category (score 18 to 24) who may benefit from enhanced surveillance or specialist review, and communicate risk clearly to patients as part of shared decision-making. Annual recalculation is recommended for all patients on long-term antiviral therapy. Clinical judgement must always complement the score.

PAGE-B Score Calculator – Complete Guide to Predicting HCC Risk in Chronic Hepatitis B

The PAGE-B score is a validated, non-invasive clinical scoring tool designed to estimate the 5-year risk of hepatocellular carcinoma (HCC) in patients with chronic hepatitis B (CHB) who are receiving antiviral therapy. Unlike older models that required liver biopsy or complex imaging, PAGE-B uses three readily available parameters – age, sex, and platelet count – making it practical for use in both specialist clinics and resource-limited settings worldwide.

HCC remains one of the most common and lethal cancers globally, with chronic hepatitis B infection accounting for the majority of cases. Early identification of high-risk patients allows clinicians to intensify surveillance, optimise treatment strategies, and potentially intervene before malignant transformation occurs. The PAGE-B score fills a critical gap by providing reliable risk stratification during antiviral treatment, when other markers such as viral load and ALT levels may normalise and no longer distinguish patients by cancer risk.

PAGE-B Score Formula

PAGE-B = (Age points) + (Sex points) + (Platelet points)

Development and Validation of the PAGE-B Score

The PAGE-B score was developed by Papatheodoridis and colleagues, published in a landmark study in the journal Gastroenterology (2016). The derivation cohort included European patients with chronic hepatitis B on nucleos(t)ide analogue (NA) therapy, predominantly entecavir or tenofovir. The score achieved high discriminative accuracy in the development cohort and was subsequently validated in independent European and Asian populations.

The name PAGE-B is an acronym derived from its three input variables: Platelets, Age, Gender, and the disease context (Hepatitis B). The simplicity of the model was intentional – the investigators sought a tool that could be applied without additional blood tests, imaging, or biopsy, using only parameters routinely collected at clinic visits.

The original validation showed a c-statistic (AUROC) of approximately 0.82 in European cohorts, indicating good discriminative ability. Subsequent validation in Asian cohorts has yielded comparable or slightly variable performance, with most studies confirming its utility across diverse populations. Some studies in East Asian cohorts have suggested modest recalibration may improve accuracy, but the unadjusted score remains widely used clinically.

Understanding the Three Components

The three variables in the PAGE-B score were selected through multivariable regression analysis, each reflecting a distinct biological mechanism underlying HCC risk.

Age is the strongest predictor of HCC in chronic hepatitis B, independent of treatment status. Older patients have accumulated greater cumulative viral replication, longer duration of hepatic inflammation and fibrosis, and greater cellular replicative senescence. Age-related immune dysfunction may also impair viral suppression at the cellular level. In the PAGE-B model, each decade of age above 30 adds 2 points to the score, reflecting a consistent and near-linear increase in cancer risk with advancing age.

Sex contributes 6 points for male patients, reflecting the well-established male predominance in HCC development. Men with chronic hepatitis B carry approximately 2 to 4 times the HCC risk of women at equivalent levels of fibrosis and viral activity. This difference is attributable to higher androgen receptor expression in hepatocytes, sex differences in immune responses to HBV, lower rates of viral clearance in men, and differences in comorbid alcohol use and metabolic risk factors.

Platelet count serves as a validated surrogate marker for portal hypertension and advanced liver fibrosis. As fibrosis progresses to cirrhosis, portal hypertension leads to splenomegaly and platelet sequestration, while reduced thrombopoietin production by the failing liver further suppresses platelet production. A platelet count below 100 x10^9/L is a reliable indicator of clinically significant portal hypertension, and patients at this level carry substantially elevated HCC risk.

Key Point: PAGE-B in the Context of Antiviral Therapy

The PAGE-B score was specifically developed for patients already receiving antiviral therapy (nucleos(t)ide analogues). It should not be applied to untreated patients, where different risk models – such as the CU-HCC score or REACH-B score – are more appropriate. In treated patients, viral suppression normalises many biochemical markers, making simple algorithms based on age, sex, and platelets more robust than complex models incorporating viral parameters.

Risk Stratification Categories and Clinical Implications

The PAGE-B score divides patients into three risk categories based on their 5-year probability of developing HCC:

PAGE-B Risk Categories

Low Risk: 0 to 9 | Intermediate Risk: 10 to 17 | High Risk: 18 or above

Low Risk (0 to 9 points): 5-year HCC risk approximately 1% – standard surveillance protocols
Intermediate Risk (10 to 17 points): 5-year HCC risk approximately 3 to 5% – regular 6-monthly surveillance mandatory
High Risk (18 to 24 points): 5-year HCC risk approximately 10% or above – intensive surveillance, specialist review

For low-risk patients (score 0 to 9), some guidelines have explored whether surveillance intervals could be extended or simplified. However, the majority of major society guidelines – including the European Association for the Study of the Liver (EASL), the American Association for the Study of Liver Diseases (AASLD), and the Asian Pacific Association for the Study of the Liver (APASL) – continue to recommend 6-monthly ultrasound surveillance for all patients with chronic hepatitis B regardless of risk category.

Intermediate-risk patients (score 10 to 17) represent the majority of those in clinical practice and require consistent adherence to standard surveillance protocols. Clinicians may consider additional investigations such as AFP-L3, des-gamma-carboxyprothrombin (DCP/PIVKA-II), or liver stiffness measurement (LSM) via transient elastography to further refine individual risk.

High-risk patients (score 18 or above) warrant the most intensive clinical attention. This includes consideration of enhanced surveillance protocols, earlier discussion of treatment response adequacy, referral to specialist hepatology or liver oncology teams, and assessment for concurrent risk factors such as cirrhosis, diabetes, metabolic syndrome, and alcohol use.

Comparison with Other HCC Risk Scores in Treated Chronic Hepatitis B

Several validated scoring systems exist for predicting HCC risk in chronic hepatitis B. The mPAGE-B score (modified PAGE-B) adds serum albumin to the three original PAGE-B variables and demonstrated superior discrimination in validation studies, particularly in Asian populations. The CAMD score uses cirrhosis status, age, male sex, and diabetes – incorporating a clinical diagnosis of cirrhosis rather than a surrogate marker like platelet count. More complex models such as the REAL-B and HCC-RESCUE scores incorporate liver stiffness or additional biochemical parameters but are less practical for routine use.

In head-to-head comparative studies, PAGE-B and mPAGE-B consistently outperform REACH-B when applied to NA-treated populations, confirming the importance of using treatment-specific risk models.

Performance of PAGE-B Across Different Ethnic Populations

The PAGE-B score has been validated in diverse geographic and ethnic populations. In European populations (the derivation context), PAGE-B achieves AUROC values of 0.80 to 0.84 with well-calibrated risk estimates. In East Asian populations (predominantly Korean, Chinese, and Taiwanese cohorts), PAGE-B demonstrates AUROC values of 0.73 to 0.80. Some studies suggest modest underestimation of HCC risk in Asian patients, potentially because HCC can arise at earlier fibrosis stages due to perinatal infection acquisition and longer disease duration.

In South Asian and sub-Saharan African populations, limited validation data exist. Given the high burden of HBV-related HCC in these regions, further prospective validation is warranted. Across all populations studied, the direction of risk associations (higher age, male sex, and lower platelets increasing HCC risk) is consistent, suggesting the biological relationships are universal even if the precise numerical accuracy varies.

PAGE-B and Liver Fibrosis Assessment

Although the PAGE-B score does not directly incorporate liver fibrosis stage, its platelet component functions as a surrogate for advanced fibrosis and cirrhosis. Liver stiffness measurement (LSM) by transient elastography (FibroScan) is now widely available and provides a continuous fibrosis estimate. Several studies have examined whether combining LSM with PAGE-B improves risk prediction. PAGE-B retains its practical advantage in settings where elastography is unavailable or unreliable (e.g., in patients with high BMI, ascites, or significant hepatic inflammation).

The EASL guidelines acknowledge that in patients with compensated advanced chronic liver disease (cACLD, defined as LSM 10 to 15 kPa), additional risk stratification using scores like PAGE-B can guide surveillance intensity. In patients with definite cirrhosis (LSM above 15 kPa), HCC surveillance is recommended regardless of PAGE-B category.

Surveillance Protocols and When to Apply PAGE-B

HCC surveillance in chronic hepatitis B is recommended by all major hepatology guidelines. The standard protocol is abdominal ultrasound every 6 months, with or without serum alpha-fetoprotein (AFP). The PAGE-B score adds value in patients without confirmed cirrhosis, where the decision to initiate or intensify surveillance may otherwise be uncertain. In non-cirrhotic patients on antiviral therapy, a high PAGE-B score justifies maintaining strict 6-monthly surveillance despite the absence of cirrhosis.

The score is most appropriately applied at baseline when antiviral therapy is initiated, and can be recalculated at subsequent visits. Since platelet count may change with treatment response or disease progression, serial calculation captures dynamic changes in risk over time. Some experts recommend annual recalculation in all patients on long-term NA therapy.

Key Point: PAGE-B Does Not Replace Clinical Judgement

The PAGE-B score provides population-level risk estimates based on three variables. Individual patients may carry HCC risk factors not captured by the score, including coexisting NAFLD, significant alcohol use, family history of HCC, diabetes, and coinfection with HCV or HDV. Clinical assessment must integrate PAGE-B results with a comprehensive review of these additional factors.

Limitations of the PAGE-B Score

Despite its widespread clinical application, the PAGE-B score has important limitations. The score was derived in European patients receiving specific antiviral agents; its applicability to patients with suboptimal viral suppression is less well established. PAGE-B assigns binary weight to sex, not accounting for post-menopausal women who lose hormonal protection. The platelet thresholds create artificial categories from a continuous variable, and laboratory variation may affect classification near threshold values. The 5-year risk estimates are population averages, not precise individual predictions. The score also does not incorporate treatment response data or emerging biomarkers such as HBsAg quantification and HBcrAg levels.

HCC and Chronic Hepatitis B – Global Disease Burden

Hepatocellular carcinoma is the sixth most common cancer and the third leading cause of cancer-related mortality worldwide, with over 900,000 new cases diagnosed annually. Approximately 50 to 60% of HCC cases globally are attributable to chronic hepatitis B virus infection, with the highest burden concentrated in sub-Saharan Africa and East Asia.

Despite effective antiviral therapies that achieve viral suppression in more than 95% of treated patients, antiviral therapy does not eliminate HCC risk. Long-term studies of patients on entecavir and tenofovir confirm that while NA therapy substantially reduces HCC incidence, patients with advanced fibrosis or cirrhosis at treatment initiation remain at significantly elevated risk for decades after achieving undetectable HBV DNA.

Nucleos(t)ide Analogues and Their Impact on PAGE-B Score Components

Long-term antiviral therapy affects two of the three PAGE-B components. Age increases monotonically with treatment duration. Platelet count, however, may change during treatment. In patients with advanced fibrosis or compensated cirrhosis, effective viral suppression can lead to fibrosis regression and clinically meaningful increases in platelet count as portal hypertension ameliorates. A patient who was high-risk at treatment initiation due to low platelets may, after several years of therapy-induced fibrosis regression, experience platelet recovery that lowers their PAGE-B category. This dynamic reflects genuine risk reduction.

Integration with Clinical Decision-Making and Multidisciplinary Care

In practice, the PAGE-B score is most useful as part of a structured hepatitis B clinic review. At the time of antiviral therapy initiation, the score provides an immediate risk category that can guide the initial surveillance approach and inform patient counselling. Within multidisciplinary teams, PAGE-B offers a standardised, reproducible metric for risk communication between hepatologists, specialist nurses, gastroenterologists, and primary care physicians.

Frequently Asked Questions

What is the PAGE-B score used for?

The PAGE-B score estimates the 5-year risk of hepatocellular carcinoma (HCC) in adults with chronic hepatitis B who are receiving antiviral therapy with nucleos(t)ide analogues. It uses three variables – age, sex, and platelet count – to generate a total score between 0 and 24, which corresponds to low, intermediate, or high risk categories. The score helps clinicians stratify surveillance intensity and counsel patients about their cancer risk during treatment.

What are the three components of the PAGE-B score?

The PAGE-B score incorporates age (scored 0 to 10 points in 2-point increments per decade from age 30), sex (6 points for male, 0 for female), and platelet count (0 points for 200 x10^9/L or above, 4 points for 100 to 199, and 8 points for below 100). The maximum possible score is 24 – a man aged 70 or above with platelets below 100 x10^9/L. Age and platelet count can each be entered directly into the calculator to receive automated scoring.

What score corresponds to high HCC risk on the PAGE-B scale?

A PAGE-B score of 18 or above corresponds to high HCC risk, with an estimated 5-year HCC probability of approximately 10% or more. Intermediate risk spans scores from 10 to 17, with a 5-year risk of roughly 3 to 5%. Low risk (score 0 to 9) is associated with approximately 1% 5-year HCC risk. These thresholds were validated in the original derivation study and confirmed in subsequent independent cohorts across Europe and Asia.

Can the PAGE-B score be used in untreated hepatitis B patients?

No. The PAGE-B score was specifically developed and validated in patients actively receiving antiviral therapy with nucleos(t)ide analogues. For untreated patients, different risk models are more appropriate – such as the REACH-B score, CU-HCC score, or GAG-HCC score. These models often incorporate viral parameters (HBV DNA, HBeAg status) that are relevant in the untreated setting but become less informative after viral suppression is achieved.

Does a low PAGE-B score mean HCC surveillance can be stopped?

No. Major guidelines from EASL, AASLD, and APASL continue to recommend 6-monthly HCC surveillance for all patients with chronic hepatitis B, including those with low PAGE-B scores. A low score indicates relatively lower risk compared to intermediate and high-risk groups, but absolute risk is not zero. HCC can still occur in low-risk patients, and discontinuing surveillance based on PAGE-B score alone is not supported by current evidence or guidelines.

What antiviral therapy was used in the PAGE-B derivation cohort?

The PAGE-B score was derived in European chronic hepatitis B patients treated primarily with entecavir or tenofovir disoproxil fumarate – the two most potent first-line nucleos(t)ide analogues with high barriers to resistance. Both drugs achieve sustained viral suppression in the vast majority of adherent patients. The score’s performance in patients on older, less potent antivirals or tenofovir alafenamide is less rigorously validated, though clinical experience suggests comparable utility.

What is the mPAGE-B score and how does it differ from PAGE-B?

The mPAGE-B (modified PAGE-B) score adds serum albumin to the three standard PAGE-B variables. Albumin reflects hepatic synthetic function and nutritional status, and its addition improves discriminative accuracy particularly in East Asian populations. In head-to-head comparisons, mPAGE-B generally shows higher AUROC values than PAGE-B in Asian cohorts. Where albumin is routinely available, mPAGE-B may be the preferred tool; PAGE-B remains useful when albumin is unavailable.

How often should the PAGE-B score be recalculated?

There is no firm consensus guideline on recalculation frequency. Given that age increases continuously and platelet count may change with treatment response, fibrosis regression, or disease progression, annual recalculation at routine hepatitis B clinic visits is a reasonable approach. Clinicians should also reconsider the score if there is a significant change in platelet count, a new diagnosis of cirrhosis, or other clinical events that alter the patient’s risk profile.

Why does male sex add 6 points to the PAGE-B score?

Men with chronic hepatitis B develop HCC at 2 to 4 times the rate of women at equivalent fibrosis stages and viral activity. This difference is attributed to androgen receptor-mediated promotion of hepatocyte proliferation and HBV replication, sex-based differences in innate and adaptive immune responses to HBV, and higher rates of comorbid risk factors such as alcohol use and metabolic syndrome in men. Pre-menopausal hormonal protection in women also contributes to the lower female risk.

What does a platelet count below 100 mean for HCC risk?

A platelet count below 100 x10^9/L is a well-validated non-invasive indicator of clinically significant portal hypertension, typically reflecting advanced fibrosis or established cirrhosis. In chronic hepatitis B, this degree of thrombocytopenia indicates the presence of structural liver disease that dramatically elevates HCC risk. The 8-point contribution to the PAGE-B score for this threshold reflects the strongest platelet-based predictor category; patients at this level should be considered high-risk even if their age and sex components are modest.

Has PAGE-B been validated in Asian patients?

Yes, multiple validation studies have been conducted in Asian populations – particularly Korean, Taiwanese, Chinese, and Hong Kong cohorts. PAGE-B generally performs with AUROC values of 0.73 to 0.80 in Asian validation cohorts, somewhat lower than in European populations. Some investigators have suggested the mPAGE-B score performs better in Asian populations. Nonetheless, PAGE-B retains clinically meaningful discriminative ability in Asian patients and is referenced in regional guidelines.

Can PAGE-B be used in patients with coexisting liver conditions?

The PAGE-B score was derived in patients with hepatitis B as the primary liver disease. In patients with coexisting conditions – such as significant NAFLD/MASLD, heavy alcohol use, HDV coinfection, or autoimmune hepatitis – the score may underestimate HCC risk because these additional factors independently promote hepatic carcinogenesis. A low PAGE-B score in a patient with advanced NAFLD or significant alcohol use should not be reassuring without additional evaluation.

What is the maximum PAGE-B score possible?

The maximum PAGE-B score is 24 points, achieved by a male patient aged 70 or above with a platelet count below 100 x10^9/L (10 points for age + 6 points for male sex + 8 points for low platelets). This combination corresponds to the highest possible HCC risk category within the PAGE-B framework. The minimum possible score is 0, achieved by a female patient aged 16 to 29 with a platelet count of 200 x10^9/L or above.

Does achieving HBV viral suppression change the PAGE-B score?

Viral suppression itself does not directly change the PAGE-B score, as viral load is not a variable in the formula. However, effective viral suppression may indirectly affect platelet count over time through fibrosis regression and reduction in portal hypertension. Some patients with advanced fibrosis show meaningful platelet recovery after years of sustained viral suppression, which would reduce their PAGE-B score and reflect genuine risk reduction. Age continuously increases, partially offsetting any risk reduction from platelet improvement.

What is the 5-year HCC risk for each PAGE-B category?

Based on the original derivation and validation data, the approximate 5-year HCC cumulative incidence rates are: low risk (score 0 to 9) around 1%, intermediate risk (score 10 to 17) around 3 to 5%, and high risk (score 18 to 24) around 10% or above. These are population-level estimates from treated European cohorts and may vary in different populations, treatment durations, and baseline fibrosis distributions.

Should HCC surveillance differ based on PAGE-B category?

Standard 6-monthly abdominal ultrasound is recommended for all patients with chronic hepatitis B regardless of PAGE-B category. However, PAGE-B score may inform additional interventions: high-risk patients (score 18 or above) may benefit from supplementary AFP measurement, referral to specialist hepatology services, enhanced assessment for concurrent risk factors, and closer monitoring of surveillance adherence. Some expert groups are exploring whether low-risk patients could have extended surveillance intervals, but this is not currently standard practice.

What is the AUROC of the PAGE-B score?

In the original European derivation and validation cohorts, PAGE-B achieved AUROC values of approximately 0.82 for 5-year HCC prediction. In Asian validation studies, AUROC values have ranged from 0.73 to 0.80. An AUROC above 0.75 to 0.80 is generally considered adequate discriminative performance for a clinical risk score. The mPAGE-B score typically achieves AUROC values 0.02 to 0.05 higher than standard PAGE-B in comparative studies.

Is the PAGE-B score validated for predicting HCC risk beyond 5 years?

The PAGE-B score was specifically validated for 5-year HCC risk prediction. Data on its accuracy for longer time horizons (10 years or beyond) are more limited. Some studies have explored PAGE-B performance at 3 and 7 years, with generally consistent but slightly attenuated discriminative accuracy at time points beyond 5 years. Annual recalculation is recommended to account for changing risk over time.

What additional tests should be considered alongside PAGE-B assessment?

PAGE-B score provides a risk estimate from three variables but does not replace comprehensive clinical evaluation. Complementary assessments include liver stiffness measurement (LSM) by transient elastography for fibrosis staging, serum AFP, HBsAg quantification as a marker of HBV reservoir size, assessment for metabolic risk factors (BMI, diabetes, dyslipidaemia), alcohol history, family history of HCC, and evaluation for co-infections. In intermediate-risk patients, combining PAGE-B with LSM or mPAGE-B may provide a more refined individual risk estimate.

Who developed the PAGE-B score and when was it published?

The PAGE-B score was developed by George Papatheodoridis and colleagues in a multicentre European study, published in Gastroenterology in 2016. The derivation cohort included European patients from Greece and several other European centres, predominantly treated with entecavir or tenofovir. Since publication, the score has been validated in numerous independent cohorts across Europe, Asia, and North America, establishing it as one of the most widely used HCC risk stratification tools for treated chronic hepatitis B.

What does PAGE-B stand for?

PAGE-B is an acronym based on the components of the score: Platelets, Age, Gender (sex), and hepatitis B (the disease context). The name reflects the three clinical variables incorporated in the formula – platelet count, patient age, and patient sex – applied specifically to the chronic hepatitis B population. The acronym is sometimes written as PAGE B or PAGEB without the hyphen, but PAGE-B is the most commonly used form in the published literature.

How does diabetes affect HCC risk in chronic hepatitis B, and is it in the PAGE-B score?

Diabetes mellitus is an independent risk factor for HCC in chronic hepatitis B, increasing risk by approximately 1.5 to 2-fold in most studies. However, diabetes is not incorporated in the PAGE-B score. The original investigators prioritised simplicity and universal data availability, and diabetes was not independently retained in the final multivariable model used for PAGE-B derivation. The CAMD score explicitly includes diabetes and may be preferred in diabetic patients where additional risk stratification is clinically important.

What is the difference between PAGE-B and REACH-B scores?

PAGE-B and REACH-B target different patient populations. REACH-B was developed for untreated (treatment-naive) chronic hepatitis B patients and incorporates HBeAg status, serum HBV DNA, ALT level, age, and sex. These viral parameters are informative in untreated patients but lose predictive value after viral suppression. PAGE-B was developed specifically for patients already on nucleos(t)ide analogue therapy. REACH-B should not be applied to treated patients, and PAGE-B should not be applied to untreated patients.

Can the PAGE-B calculator be used for patients with HDV coinfection?

The PAGE-B score was not specifically validated in patients with hepatitis D virus (HDV) coinfection. HDV superinfection or coinfection accelerates fibrosis progression and independently elevates HCC risk beyond what is predicted by HBV-based models alone. In patients with known HDV coinfection, the PAGE-B score may underestimate HCC risk. Clinical management of HDV-HBV coinfected patients should involve specialist hepatology input.

Is the PAGE-B score used in clinical practice guidelines?

Yes. The PAGE-B score is referenced in major hepatology guidelines, including the EASL Clinical Practice Guidelines on the Management of Hepatitis B Virus Infection. It is cited as a validated, non-invasive tool for HCC risk stratification in treated chronic hepatitis B patients. Regional guidelines in Asia – including those from the Korean Association for the Study of the Liver, the Taiwan Liver Research Foundation, and APASL – also reference PAGE-B and mPAGE-B in their HCC surveillance recommendations.

What platelet count represents the highest risk category in PAGE-B?

A platelet count below 100 x10^9/L represents the highest platelet-based risk category in PAGE-B, contributing 8 points to the total score. This threshold is clinically significant as it typically indicates severe portal hypertension, often associated with established cirrhosis. A platelet count between 100 and 199 x10^9/L contributes 4 points (intermediate risk). Patients with platelets at or above 200 x10^9/L receive 0 points for this component, reflecting relatively preserved hepatic structure.

What are the key clinical scenarios where PAGE-B is most useful?

PAGE-B is most clinically valuable in four main scenarios: (1) at initiation of antiviral therapy, to establish baseline HCC risk and justify surveillance initiation; (2) in non-cirrhotic patients where the decision to implement 6-monthly surveillance may otherwise be uncertain; (3) in resource-limited settings where more complex assessments are unavailable; and (4) in clinical communication and patient counselling, where the score translates into clear risk categories that promote surveillance adherence.

Conclusion

The PAGE-B score represents a clinically practical, validated, and widely applicable tool for HCC risk stratification in adults with chronic hepatitis B receiving antiviral therapy. Its three-variable structure – age, sex, and platelet count – enables rapid calculation at every clinic visit using routinely available data, without the need for additional blood tests, imaging, or liver biopsy.

The score’s risk categories (low: 0 to 9, intermediate: 10 to 17, high: 18 to 24) provide clinically meaningful guidance for surveillance intensity, patient counselling, and resource allocation. While it does not replace comprehensive clinical evaluation, PAGE-B has established itself as an essential component of the hepatitis B specialist’s toolkit. All patients with chronic hepatitis B on antiviral therapy should have their PAGE-B score calculated, documented, and reviewed annually as part of routine clinical care.