Hepatitis B: Symptoms, Causes & Treatment | aihealz

USA

Hepatitis B: Symptoms, Causes & Treatment | aihealz | aihealz

§ 02

How you might notice it

01Two-thirds of adult acute hepatitis B infections are asymptomatic; the remaining third experience the prodrome and icteric phases described below.

02Prodromal flu-like illness with fatigue, low-grade fever, nausea, anorexia, right-upper-quadrant abdominal pain, headache, and joint pains 1-4 weeks before jaundice.

03Urticaria, polyarthralgia, and serum-sickness-like syndrome in roughly 10% of acute cases, driven by immune complexes.

04Yellowing of skin and sclera, dark urine, and pale stools developing over 1-2 weeks with peak transaminases at 10-100× upper limit of normal.

05Right-upper-quadrant tenderness with a slightly enlarged tender liver during the icteric phase.

06In chronic hepatitis B, most patients are entirely asymptomatic for decades; symptoms (fatigue, mild right-upper-quadrant discomfort) appear when significant fibrosis or active hepatitis is present.

07Symptoms and signs of cirrhosis in advanced chronic disease: ascites, peripheral oedema, easy bruising, spider naevi, palmar erythema, splenomegaly, encephalopathy.

08Hematemesis or melena from variceal bleeding in decompensated cirrhosis.

09Confusion, asterixis, sleep-wake reversal, and personality change from hepatic encephalopathy.

10Insidious weight loss, abdominal distension, and new pain in the setting of hepatocellular carcinoma.

early warning signs

•Mild persistently elevated transaminases on routine blood tests in a person born in or with parental origin from an HBV-endemic region
•Family history of hepatocellular carcinoma or chronic hepatitis B
•Anti-HBc total positive with negative HBsAg and negative anti-HBs — past exposure that may reactivate under immunosuppression
•New-onset fatigue, polyarthralgia, or rash combined with subtle right-upper-quadrant discomfort in young adults
•Acute jaundice without obvious cause in a sexually active adult or person with intravenous drug use

● emergency signs

•Profound jaundice with prolonged prothrombin time, encephalopathy, hypoglycemia, or rising ammonia — acute liver failure requires transplant referral
•Hematemesis or melena in a known cirrhotic patient — variceal hemorrhage requires resuscitation, endoscopic band ligation, and vasoactive drugs
•Acute kidney injury, oliguria, and ascites in cirrhotic patient — possible hepatorenal syndrome
•Confusion, agitation, asterixis, or coma — hepatic encephalopathy
•Reactivation flare with very high HBV DNA, marked ALT rise, and jaundice in a previously inactive patient — needs urgent antiviral therapy and may require transplant assessment

§ 03

How it’s diagnosed

diagnosis

Diagnosis combines clinical assessment with a defined panel of serological markers, viral nucleic acid testing, and biochemical and imaging staging of liver disease. The initial test is HBsAg: positive HBsAg indicates current HBV infection (acute or chronic). HBsAg present for more than 6 months establishes chronic infection. The complementary panel — anti-HBs (immunity from prior infection or vaccination), anti-HBc total (past or current infection), IgM anti-HBc (acute infection), HBeAg (active replication and high infectivity), anti-HBe (often associated with lower viral replication) — defines the phase of infection. Quantitative HBV DNA by real-time PCR measures viral load and guides treatment decisions and monitoring. Liver function tests (ALT, AST, GGT, alkaline phosphatase, bilirubin, albumin, INR) and platelets define disease activity and synthetic function. Non-invasive markers of fibrosis (FIB-4, APRI), transient elastography (Fibroscan), or shear-wave elastography stage fibrosis without biopsy. Liver biopsy is reserved for ambiguous cases or research. All chronic HBV patients are also tested for HIV, hepatitis C, hepatitis D (HBV/HDV coinfection in 5-10% of chronic HBV), and hepatocellular carcinoma surveillance (abdominal ultrasound and alpha-fetoprotein every 6 months in patients with cirrhosis, family history of HCC, or other high-risk features). Pregnant women are screened universally for HBsAg at first antenatal visit; HBsAg-positive women with HBV DNA above 200,000 IU/mL receive tenofovir disoproxil fumarate from week 28 of pregnancy to reduce mother-to-child transmission. Genotype testing is helpful when interferon therapy is considered (genotype A responds best) but not routine for nucleos(t)ide treatment.

Key tests

Hepatitis B surface antigen (HBsAg)Indicates current HBV infection — acute or chronic

Anti-HBs and anti-HBc totalDistinguishes resolved infection (anti-HBs and anti-HBc positive), vaccination (anti-HBs positive alone), and current infection (anti-HBc positive, HBsAg positive)

HBeAg, anti-HBeIdentifies replicative phase and infectivity

Quantitative HBV DNA (real-time PCR)Measures viral load to guide treatment decisions, monitor response, and detect relapse

Liver function tests, full blood count, INR, albuminAssesses inflammation, synthetic function, and platelet count

Non-invasive fibrosis assessment (FIB-4, APRI, transient elastography)Stages liver fibrosis without biopsy

Abdominal ultrasound and alpha-fetoprotein (HCC surveillance)Surveillance for hepatocellular carcinoma in patients at risk (cirrhosis, family history of HCC, certain age and genotype thresholds)

Hepatitis D virus antibody and HDV RNADetects HDV coinfection that accelerates liver disease

Outlook

Outcome depends on age at infection, phase of disease, and timely treatment. Adult acute hepatitis B resolves spontaneously in over 95% of immunocompetent adults; chronic infection develops in 90% of perinatally infected infants and 25-50% of children infected aged 1-5. Without treatment, roughly 8-20% of chronic HBV patients develop cirrhosis over 20-30 years; once cirrhosis is established, the annual risk of hepatocellular carcinoma is 2-5%. Effective antiviral therapy with TAF, TDF, or entecavir suppresses HBV DNA in over 95% of patients, normalizes ALT, halts or reverses fibrosis (compensated cirrhosis can regress on long-term therapy), and reduces but does not eliminate HCC risk — surveillance every 6 months continues even on therapy. HBsAg loss (functional cure) is uncommon (under 1% per year on NA therapy, 3-7% with pegIFN) but profoundly reduces HCC and disease-related death. HBV/HDV coinfection progresses faster — 10-20 year cumulative cirrhosis risk approaches 50-70% — and benefits from bulevirtide and pegIFN combinations. Liver transplantation cures end-stage HBV with 5-year post-transplant survival of 75-85% under modern antiviral prophylaxis. The WHO 2030 elimination targets (90% reduction in new infections, 65% reduction in mortality) are achievable with universal birth-dose vaccination, screen-and-treat expansion, and access to affordable generic nucleos(t)ide analogues.

§ 05

Causes & risk factors

known causes

Mother-to-child (perinatal) transmission: Vertical transmission from HBsAg-positive mothers, typically at or near delivery rather than transplacentally. Risk approaches 90% if mother is HBeAg-positive without intervention; reduced to under 5% with combined hepatitis B immune globulin and active vaccination at birth, and to under 1% with maternal tenofovir disoproxil fumarate from week 28 of pregnancy when HBV DNA exceeds 200,000 IU/mL.
Horizontal childhood transmission: Close household contact, shared toothbrushes and razors, traditional scarification, and minor open wounds account for early-childhood acquisition that drives chronicity in 25-50% of cases. Particularly important in sub-Saharan Africa.
Sexual transmission: HBV is far more transmissible than HIV (100× higher per exposure) through unprotected vaginal, anal, or oral sex with infected partners. Dominant route of new infections in non-endemic adult populations.
Percutaneous and parenteral exposure: Injection drug use with shared needles, unsterile medical or dental procedures, traditional tattooing and piercing without sterile equipment, occupational needlestick injuries, and (historically) contaminated blood products.
Healthcare exposure: Pre-1990s blood transfusion, hemodialysis without segregation of HBsAg-positive patients, multidose vials, and unsterile injection practices. Risk has dropped dramatically in countries with universal donor screening and single-use syringes.
Iatrogenic reactivation during immunosuppression: Latent HBV (resolved or occult infection) can reactivate during chemotherapy, rituximab, glucocorticoids, anti-TNF therapy, hematopoietic stem-cell transplantation, or HIV antiretroviral changes. Reactivation can cause fatal hepatic failure if not prevented with prophylactic antivirals.

risk factors

Birth in or origin from an HBV-endemic regionnon-modifiable: China, sub-Saharan Africa, South-East Asia, Pacific Islands, and Eastern Europe have HBsAg prevalence above 5%. Children of mothers from these regions are at highest risk, especially without birth-dose vaccination.
HIV co-infectionmodifiable: HIV-positive individuals have 5-10× higher HBV chronicity rate, faster progression to cirrhosis, and higher mortality. Combined antiretroviral therapy with TDF/TAF treats both infections.
Injection drug usemodifiable: Shared needles, syringes, cookers, or filters dramatically increase HBV risk. Comprehensive harm reduction (needle exchange, opioid substitution therapy) reduces transmission.
Multiple sexual partners or unprotected sex with infected partnermodifiable: HBV is more efficiently transmitted sexually than HIV. Vaccination provides reliable protection; condoms reduce but do not eliminate risk.
Healthcare or laboratory occupationmodifiable: Surgeons, dentists, dialysis staff, laboratory technicians, and traditional birth attendants face elevated exposure to blood. Universal vaccination of healthcare workers is standard.
Household contact with HBsAg-positive personmodifiable: Sharing personal items (razors, toothbrushes, manicure tools) with an HBsAg-positive household member transmits HBV. Vaccinate household and sexual contacts.

Living with Hepatitis B

Timeline

Acute hepatitis B: jaundice and acute symptoms resolve over 2-12 weeks; HBsAg clearance occurs in over 95% of immunocompetent adults within 6 months. Chronic hepatitis B on antiviral therapy: HBV DNA suppression within 6-12 months; ALT normalization within 6-18 months; fibrosis improvement over 1-5 years; HBsAg loss is uncommon and slow (sometimes >10 years on NA). After liver transplant: graft function recovers over weeks; HBV prophylaxis lifelong.

Lifestyle

01Avoid alcohol entirely or limit to less than 14 units per week with no binge drinking.
02Maintain healthy body weight to reduce coexisting non-alcoholic fatty liver disease.
03Take antiviral therapy at the same time daily and do not stop without specialist advice — sudden discontinuation can cause severe hepatic flare.
04Disclose chronic HBV status to all sexual partners and household members and ensure they are vaccinated.
05Avoid raw or undercooked shellfish (risk of hepatitis A or vibrio coinfection).
06Vaccinate against hepatitis A and consider influenza and pneumococcal vaccination annually.
07Attend regular HCC surveillance appointments every 6 months if cirrhosis or high-risk features are present.

Daily management

01Take antiviral therapy at the same time daily with or without food, as advised.
02Attend appointments for HBV DNA, ALT, and liver function every 3-6 months during treatment.
03Schedule HCC surveillance ultrasound and AFP every 6 months if cirrhosis or family history of HCC.
04Maintain weight, blood pressure, and metabolic indices to reduce coexisting NAFLD.
05Update contact tracing and vaccination of household and sexual contacts.
06Carry medical-alert documentation if cirrhotic; carry a medication list.

Exercise

Regular moderate aerobic exercise (150 minutes per week) and resistance training reduce hepatic steatosis, support weight management, and improve quality of life. Vigorous exercise is safe in chronic HBV unless decompensated cirrhosis or active flare is present. Avoid contact sports during severe thrombocytopenia.

§ 08

Frequently asked

What is hepatitis B?

Hepatitis B is a viral infection of the liver caused by hepatitis B virus (HBV), a DNA virus transmitted through blood, sexual contact, and from mother to child. Most adults clear acute infection, but 90% of infected infants and 25-50% of young children develop chronic infection that can lead to cirrhosis and liver cancer.

How is hepatitis B spread?

HBV is transmitted through blood, semen, and other body fluids. The dominant routes are mother-to-child at birth, sexual contact, shared needles or razors, and unsterile medical or tattoo procedures. HBV is roughly 100 times more transmissible per exposure than HIV. It is not spread by casual contact, kissing, or breastfeeding without nipple trauma.

Is hepatitis B curable?

Acute hepatitis B is cleared spontaneously in over 95% of immunocompetent adults. Chronic hepatitis B can be effectively controlled but not yet fully cured. Oral antivirals (tenofovir, entecavir) suppress the virus in over 95% of patients and prevent cirrhosis and HCC, but functional cure (HBsAg loss) is uncommon.

What are the symptoms of hepatitis B?

Two-thirds of acute infections are asymptomatic. The remaining third have fatigue, fever, nausea, abdominal pain, dark urine, and jaundice over 1-3 months. Chronic infection is usually silent for decades until cirrhosis or HCC develops, which can produce fatigue, ascites, jaundice, encephalopathy, or weight loss.

Is the hepatitis B vaccine effective?

Yes. The recombinant HBsAg vaccine, available since 1982, induces protective antibody in over 95% of healthy infants and adults after three doses (or two doses with Heplisav-B in adults). WHO recommends universal birth-dose vaccination followed by completion of the infant schedule. Protection is durable, with no booster needed for healthy adults.

Can hepatitis B be transmitted by kissing?

No. HBV is not spread by casual contact, hugging, kissing, or sharing utensils. Transmission requires exposure to infected blood or body fluids — primarily through sexual contact, shared needles, unsterile medical procedures, or mother-to-child during childbirth.

What is HBsAg?

Hepatitis B surface antigen (HBsAg) is a protein on the outer surface of the hepatitis B virus. Its presence in blood indicates current HBV infection — acute (less than 6 months) or chronic (more than 6 months). Loss of HBsAg with development of anti-HBs antibody indicates recovery and immunity.

What treatments are used for chronic hepatitis B?

First-line treatments are oral nucleos(t)ide analogues — tenofovir alafenamide, tenofovir disoproxil fumarate, and entecavir — taken once daily for years to lifelong. They suppress HBV DNA in over 95% of patients and reduce risk of cirrhosis and liver cancer. Pegylated interferon alpha is an alternative finite-course option in selected patients.

How long does hepatitis B treatment last?

Most patients on oral antivirals continue therapy indefinitely. Stopping treatment can cause severe flares and rapid progression to liver failure. Pegylated interferon is given as a 48-week course. Treatment may be reassessed in patients who achieve HBsAg loss or who are at very low risk of progression.

Can pregnant women take hepatitis B treatment?

Yes. Tenofovir disoproxil fumarate is given to HBsAg-positive pregnant women with HBV DNA above 200,000 IU/mL from week 28 of pregnancy to reduce mother-to-child transmission. This, combined with hepatitis B immune globulin and birth-dose vaccine, reduces transmission to under 1%.

What is the difference between hepatitis B and hepatitis C?

Hepatitis B is caused by a DNA virus, transmitted predominantly perinatally or sexually, prevented by vaccine, and managed with lifelong antivirals. Hepatitis C is caused by an RNA virus, transmitted predominantly by blood (injection drug use, contaminated transfusion), with no vaccine, but curable in 95% with 8-12 weeks of direct-acting antivirals.

Can hepatitis B cause liver cancer?

Yes. Hepatitis B causes 50-55% of hepatocellular carcinoma worldwide. Annual HCC risk in cirrhotic HBV patients is 2-5%. Even non-cirrhotic HBV carriers have elevated risk, particularly with Asian or African origin, age over 40, family history of HCC, or high viral load. Surveillance with ultrasound and AFP every 6 months is standard for high-risk patients.

Is hepatitis B reactivation dangerous?

Yes. HBV reactivation during chemotherapy, rituximab, transplantation, biologic therapy, or HIV treatment changes can cause severe hepatitis and death. All candidates for immunosuppression should be screened for HBsAg, anti-HBc, and HBV DNA, and prophylactic antiviral therapy given where indicated.

Should family members of hepatitis B patients be tested?

Yes. Household and sexual contacts of HBsAg-positive patients should be tested for HBsAg, anti-HBs, and anti-HBc. Susceptible contacts should be vaccinated. Newborns of HBsAg-positive mothers must receive birth-dose vaccine and hepatitis B immune globulin within 12 hours of delivery.

Is there a one-time test for hepatitis B?

WHO and CDC recommend at least one-time hepatitis B screening for all adults aged 18 and older, regardless of risk factors. The screening panel includes HBsAg, anti-HBs, and anti-HBc total. People with positive HBsAg or anti-HBc need further evaluation by a hepatologist.

Can people with hepatitis B donate blood or organs?

People with active HBV infection (HBsAg positive) cannot donate blood. Organ donation is possible in selected circumstances with full disclosure and recipient consent. People with resolved HBV (anti-HBc positive, HBsAg negative) may be eligible to donate blood in some jurisdictions after thorough screening.

What is hepatitis D?

Hepatitis D virus (HDV) is a defective RNA virus that requires HBsAg for replication. HBV/HDV coinfection accelerates liver disease in 15-20 million chronic HBV patients globally. Bulevirtide became the first specific HDV therapy approved in Europe in 2020. All chronic HBV patients should be tested for HDV at least once.

Does hepatitis B affect life expectancy?

Chronic HBV with effective antiviral suppression and good adherence has near-normal life expectancy. Untreated chronic HBV with progression to cirrhosis or HCC carries significantly reduced life expectancy. Early diagnosis, sustained treatment, and HCC surveillance dramatically improve outcomes.

Can hepatitis B be passed through breast milk?

Breastfeeding by HBsAg-positive mothers is considered safe when the infant has received birth-dose vaccine and HBIG. The infant's protection comes from vaccination, not from avoiding breast milk. Mothers with cracked nipples should temporarily express and discard milk while healing.

What lifestyle changes help hepatitis B?

Avoid alcohol entirely, maintain healthy weight, eat a Mediterranean-style diet, take prescribed antivirals at the same time daily, attend regular follow-up, get vaccinated against hepatitis A, and ensure household and sexual contacts are vaccinated. Avoid raw shellfish and aflatoxin-contaminated foods.

Is hepatitis B going to be eliminated?

WHO has set 2030 elimination targets — 90% reduction in new chronic infections and 65% reduction in mortality. Reaching these targets requires universal birth-dose vaccination, scale-up of testing and treatment, prevention of mother-to-child transmission, and access to affordable generic antivirals. Progress is significant but uneven globally.

Hepatitis B.

What it is

How you might notice it

How it’s diagnosed

Treatment & cost

Causes & risk factors

Living with it

When to seek help

Related conditions

Easily confused with

Often appears alongside

Types and stages

Living with Hepatitis B

Complementary approaches

Patient support resources

Frequently asked

Sources & references

Top Gastroenterologists in Argentina.

Connect with top Gastroenterologists in Argentina.