Authored for clinicians with emphasis on evidence-based practice, updated guidelines (AASLD 2018, EASL 2017/2024 updates), and practical decision-making tools.
Epidemiology & Virology Primer (Clinician Refresher)
HBV is a Hepadnaviridae family, enveloped virus with a partially double-stranded, relaxed circular DNA genome. It replicates via an RNA intermediate using a viral reverse transcriptase — a feature conferring high mutagenic potential and underpinning antiviral resistance concerns. Key antigenic components include:
| Antigen/Ab | Clinical Significance |
|---|---|
| HBsAg | Marker of current infection (acute or chronic); appears 1–10 weeks post-exposure; clearance defines resolution |
| anti-HBs | Protective immunity (post-infection or vaccination); titer ≥10 mIU/mL confers long-term protection |
| IgM anti-HBc | Hallmark of recent acute infection (appears at symptom onset, declines over 6 months) |
| Total anti-HBc (IgG + IgM) | Lifelong marker of exposure (past or present infection); persists after resolution |
| HBeAg | Marker of high-level viral replication and infectivity; associated with “immune-tolerant” phase in chronic HBV |
| anti-HBe | Seroclearance often signifies reduced replication, but not always (e.g., pre-core/core promoter mutants) |
Note: HBV DNA levels can range from undetectable to >10⁹ IU/mL in acute infection. Genotype matters: Genotypes A & D more likely to progress to chronicity; B & C have higher rates of HBeAg seroconversion but may exhibit reactivation later.
Clinical Presentation & Diagnosis: When to Suspect Acute HBV
Epidemiologic Red Flags:
- Recent exposure (e.g., needlestick, unprotected sex, IV drug use, travel to endemic region [Southeast Asia, Sub-Saharan Africa, Amazon basin])
- Perinatal transmission risk (infants of HBsAg+ mothers despite immunoprophylaxis)
- Unexplained hepatitis in patients with negative HEV, HAV, HSV, CMV, EBV, autoimmune markers
Symptoms (Incidence: 30–50% in adults; <10% in children <5 y):
- Prodrome: Flu-like symptoms (fever, myalgia, malaise), nausea/vomiting
- Icteric phase: Jaundice, dark urine, pale stools, RUQ pain/tenderness (hepatomegaly ± splenomegaly)
- Fulminant presentation (<1% of acute cases): Rapid deterioration with encephalopathy, coagulopathy (INR >2.0), ascites, hepatic hydrothorax — mortality up to 80% without transplant
Key Clinical Pearl:
Acute HBV should be considered in any adult with unexplained ALT >5× ULN + bilirubin elevation, even if asymptomatic or minimally symptomatic.
Source: AASLD 2018 Guidance onHBV Prevention, Diagnosis, and Management.
Diagnostic Workup: Serology & Beyond
Essential Initial Testing (Order as Panel)
| Test | Interpretation in Acute HBV | Caveats |
|---|---|---|
| HBsAg | Positive (definitive current infection) | May be transiently negative during window period (IgM anti-HBc+ only); repeat if high suspicion |
| IgM anti-HBc | Positive (diagnostic of acute/recent infection) | False positives occur; confirm with HBV DNA and clinical context |
| Total anti-HBc | Positive | Not useful acutely alone (doesn’t distinguish acute vs chronic) |
| anti-HBs | Negative or low-titer rising (if vaccine-naïve); may become positive during recovery | |
| HBeAg & anti-HBe | Often HBeAg+ early; seroconversion predicts resolution | Not required for diagnosis but informs prognosis |
Confirmatory & Prognostic Testing
- HBV DNA quantification (qPCR, LOQ ~10–20 IU/mL)
- Acute HBV: Typically >10⁷ IU/mL during peak viremia; declines over weeks-months
- Prognostic value: Failure to decline by 8–12 weeks predicts chronicity
- Liver Function Tests (LFTs):
- ALT often >1000 U/L (can exceed 5000 U/L); AST usually <ALT; ALP mildly elevated
- Bilirubin: Direct bilirubin predominates; >3 mg/dL warrants urgent assessment for fulminant hepatitis
- Coagulation: INR is more sensitive than PT for synthetic dysfunction
- Ultrasound with Doppler (if decompensation suspected): Assess liver morphology, portal flow, exclude thrombosis
Coinfection Screening (Mandatory in All New Diagnoses)
- HCV RNA (ELISA alone insufficient due to window period)
- HIV antibody/antigen (4th gen assay)
- HDV IgM/IgG + total anti-HDVespecially if:
- HBsAg+ for >6 months
- Unusual severity or rapid progression
- Origin from HDV-endemic regions (Mediterranean, West Africa, Amazon basin)
Evidence: Coinfection increases risk of fulminant hepatitis and cirrhosis (AASLD 2018; J Hepatol 2024 HDV guidelines).
Management: When to Treat & How
Supportive Care (95–98% of Acute HBV Cases)
- Hydration, nutritional support, avoid hepatotoxins (alcohol, unnecessary meds)
- No antivirals in uncomplicated acute hepatitis — may delay immune clearance and select for resistance
Antiviral Therapy Indications (AASLD/EASL Criteria)
Antivirals are indicated only in:
- Fulminant hepatic failure (FHF):
- Defined by: INR ≥1.5 + encephalopathy ± ascites in setting of acute hepatitis
- Start immediately — do not wait for serology confirmation if clinical suspicion high
- Protracted severe acute hepatitis B (pS-AHB):
- Persistent bilirubin >3 mg/dL (or direct >1.5 mg/dL) AND INR >1.5 despite supportive care
- Or progressive synthetic dysfunction (e.g., hypoalbuminemia <3 g/dL, rising creatinine)
First-Line Antivirals (All Nucleos(t)ide Analogues – NUCs):
| Drug | Dosing | Advantages | Limitations |
|---|---|---|---|
| Entecavir | 1 mg daily | High barrier to resistance; well-tolerated | Renal monitoring if eGFR <50 mL/min |
| Tenofovir Alafenamide (TAF) | 25 mg daily | Lower bone/kidney toxicity vs TDF; similar efficacy | Avoid in BMI >35 (reduced exposure) |
| Tenofovir Disoproxil Fumarate (TDF) | 300 mg daily | Long-term safety data; preferred in pregnancy | Monitor renal function & bone density |
Critical Notes:
- Do NOT use interferon alpha — contraindicated due to risk of precipitating liver failure and severe flu-like side effects (Hepatology 2019;69:2137–2152).
- Duration of therapy:
- In FHF/pS-AHB: Continue until sustained HBsAg loss (confirmed ≥6 months apart)
- If undergo liver transplant: Lifelong NUC therapy (retransplantation often required without suppression)
Monitoring During Antiviral Therapy:
- Weekly: LFTs, INR, bilirubin
- Biweekly:HBV DNA until suppressed (<20 IU/mL)
- Monthly: Clinical assessment for decompensation
Defining Transition to Chronic Infection & Next Steps
Chronic HBV is diagnosed if:
✅ HBsAg persists >6 months after initial diagnosis
(Note: 90% of chronic cases arise from perinatal infection; only 5–10% of immunocompetent adults fail to clear)
Actionable Steps Upon Diagnosis of Chronicity:
- Repeat full serologic panel (HBsAg, anti-HBs, total anti-HBc, HBeAg, anti-HBe)
- Baseline HBV DNA, LFTs, liver ultrasound ± FibroScan®/ELF test
- Assess for HCC screening eligibility (age >40, family HCC history, cirrhosis, high viral load >2000 IU/mL)
- Refer to hepatology if:
- ALT persistently elevated + HBV DNA >2000 IU/mL
- Signs of advanced fibrosis (F3/F4 on elastography/biopsy)
- HBeAg-negative disease with fluctuating enzymes/DNA
Prevention & Public Health Imperatives
- Post-Exposure Prophylaxis (PEP):
- Perinatal: HBV vaccine + HBIG within 12h of birth → 95% efficacy
- Occupational (needlestick): Unvaccinated → initiate vaccine series + HBIG; vaccinated with unknown Ab status → check anti-HBs; if <10 mIU/mL, give booster ± HBIG
- Vaccination: All adults ≤60 y (USPSTF Grade B); older adults with risk factors (Grade C)
- Household/sexual contacts: Test & vaccinate if anti-HBs negative
Evidence Summary Table: Key Practice-changing Data
| Clinical Scenario | Guideline Recommendation | Supporting Evidence |
|---|---|---|
| Acute HBV without decompensation | Supportive care only | AASLD 2018 (Strong, moderate evidence) |
| Fulminant hepatitis B | Start entecavir/TDF immediately; urgent transplant eval | EASL 2017 (Level A); Liver Transpl 2020;26:1539–1549 |
| Antiviral choice in acute HBV | Entecavir or TAF preferred over TDF (if renal/bone risk) | Clin Infect Dis 2021;73:e591–e601 (real-world outcomes) |
| HDV screening | All HBsAg+ patients should be tested at diagnosis | J Hepatol 2024;80:522–538 (Global HDV consensus) |
Final Clinical Pearls:
- The “window period” is real: If HBsAg– but IgM anti-HBc+ with elevated ALT, repeat serology in 2 weeks.
- HBeAg status doesn’t guide acute management — focus on clinical severity and viral kinetics.
- Never assume resolution without confirmatory HBsAg negativity at 6 months.
- Chronicity is preventable: Early antiviral use in pS-AHB may reduce progression to cirrhosis (Hepatology Commun 2022;6:1485–1495).
For full chronic HBV management algorithms, refer to the AASLD 2018 Guidance or EASL Clinical Practice Guidelines: Hepatitis B update (2024). Always consult institutional antiviral resistance protocols when selecting therapy.
— Prepared by Infectious Disease & Hepatology Consult Service — Last updated: June 2024.
