Summary

This document provides an overview of hepatitis, covering acute and chronic forms, causes, symptoms, and investigations. It details various types of hepatitis, including viral, bacterial, and metabolic causes. The document also describes the clinical picture, management, and diagnostic procedures for hepatitis.

Full Transcript

Hepatitis 1. Acute hepatitis a. Infections i. Viral hepatitis: A, B, C, D, E. ii. Other viruses causing hepatitis: EBV, CMV, HSV, Yellow fever. iii. Bacterial hepatitis: Neisseria meningitidis and gonorrhea, salmonella, brucella, campylobacter. b. Drugs...

Hepatitis 1. Acute hepatitis a. Infections i. Viral hepatitis: A, B, C, D, E. ii. Other viruses causing hepatitis: EBV, CMV, HSV, Yellow fever. iii. Bacterial hepatitis: Neisseria meningitidis and gonorrhea, salmonella, brucella, campylobacter. b. Drugs and toxins: Alcohol, halothane, isoniazid, paracetamol. c. Metabolic: Wilson's disease. 2. Chronic hepatitis: Inflammation of the liver lasting for at least six months. a. Viral Hepatitis: B, C, D. b. Autoimmune hepatitis. c. Drugs and toxins: Alcohol, isoniazid (INH), methyldopa. d. Metabolic: Wilson's disease, 𝛼-1 antitrypsin deficiency. ACUTE VIRAL H E PAT I T I S Acute Viral Hepatitis HAV HBV HCV HDV HEV Genome RNA DNA RNA RNA RNA Transmission Oral Blood Blood Blood Oral IP 2-6w 1-6 m 1-6 m 1-6 m 2-6 w Sporadic or Sporadic Sporadic Sporadic Sporadic or Incidence epidemic epidemic Age Young Any Any Any Young Mild Severe Mild Severe Mild (except Acute attack in pregnant) No No chronicity + no Chronicity + Chronicity + chronicity + After hepatitis Chronicity relation to HCC HCC HCC no relation to HCC Prophylaxis Prevented by Vaccine Vaccine ---------- ---------- (active) HBV vaccine Prophylaxis Immuno- Immunoglobulins ---------- ---------- (Passive) globulin Hepatitis A Virus (HAV) → RNA virus.  Fecal-oral transmission → children and young adults affected → sporadic or epidemic incidence.  IP 2-6 weeks → acute attack is usually mild → NO chronicity / HCC.  Prophylaxis with vaccination or immunoglobulin. Hepatitis E Virus (HEV) → RNA virus.  Fecal-oral transmission → children and young adults affected → sporadic or epidemic incidence.  IP 2-6 weeks → acute attack is usually mild except in pregnant females → NOT associated with chronicity or HCC.  No prophylaxis Hepatitis B Virus (HBV) → DNA virus.  Blood, sexual, or vertical (from mother to child) transmission → affects any age → sporadic incidence.  IP 1-6 months → acute attack is usually severe → associated with both chronicity and HCC.  Prophylaxis with vaccination or immunoglobulins. Hepatitis C Virus (HCV) → RNA virus.  Transmitted by blood and community acquired (unknown etiology) → affects any age (more common in adults) → sporadic incidence.  IP 1-6 months → acute attack is usually mild or may go unnoticed → associated with both chronicity and HCC.  No prophylaxis. Hepatitis D Virus (HDV) Weak incomplete RNA virus "Delta agent" dependent on HBsAg → affects only those infected with HBV, either as: 1. Co-infection: HBV and HDV infection occurs simultaneously → C/P of acute hepatitis which may be fulminant. 2. Super-infection: HDV infection occurs in a chronic HBV carrier → activation of hepatitis in a previously stable patient. Blood, sexual, and vertical transmission → affects any age → sporadic incidence. IP 1-6 months → acute attack is usually severe → associated with chronicity. Prophylaxis is vaccination against HBV. Clinical Picture 1. Anicteric hepatitis (usually missed in diagnosis)  Mild cases with influenza-like symptoms and no jaundice. 2. Icteric hepatitis a. Pre - icteric stage (3 days-2 weeks) Symptoms 1. Acute onset fever / marked anorexia / nausea / vomiting 2. Dull aching pain in the right hypochondrium / epigastrium Signs 1. Fever with non-specific skin rash 2. Enlarged, tender, soft liver b. Icteric stage (1 - 4 weeks) Symptoms 1. Fever subsides / anorexia, nausea, vomiting improve. 2. Dark urine at first (bilirubinuria) → then pale stools (no bilirubin entering the gut) → then jaundice Signs 1. Liver is enlarged, tender, soft. 2. Spleen and LN are slightly enlarged. c. Convalescence stage  Symptoms and signs gradually improve, then disappear.  Complete recovery of the liver (clinical / biochemical / histological) may take up to 6 months. Sequelae 1. Complete recovery a. Most cases: HAV and HEV b. Many cases: HBV and HDV c. Few cases: HCV 2. Complications a. Hepatic complications i. Relapse: Original attack recurs and jaundice reappears → serum bilirubin + enzymes  once again ii. Cholestatic hepatitis (especially with HAV): Prolonged cholestasis →  ALP, pruritus, jaundice (may persist for 8-28 weeks) → complete recovery. iii. Fulminant hepatitis: Massive hepatic necrosis → features of acute liver failure (rare). iv. Post-hepatitis syndrome: Transaminitis (all investigations are normal EXCEPT mild  of transaminases). Presents with fatigue, anorexia, pain in right hypochondrium. v. Chronic sequelae (only in HBV, HCV, HDV) Chronic hepatitis Cirrhosis Hepatocellular Carcinoma. Carrier state b. Extrahepatic complications (antigen-antibody complexes) i. Arthritis. ii. Aplastic anemia. iii. Guillain-Barré syndrome (nerve weakness → paralysis). iv. Extrahepatic complications occurring only with HBV / HCV: Glomerulonephritis. Polyarteritis nodosa (inflammation of BV → nodules). Cryoglobulinemia (cryoglobulins = abnormal proteins → precipitated by cold in body tissues → arthralgia, myalgia, fatigue, kidney affection). Investigations 1. Liver function tests a.  Serum bilirubin, transaminases, ALP, gamma globulins. b. Normal albumin. 2. Abdominal ultrasound: Hepatomegaly / splenomegaly (20%). 3. Urine analysis a. Dark, frothy urine due to the presence of bilirubin and bile salts. b. Slight proteinuria and hematuria (due to glomerulonephritis). 4. Stool analysis: Pale stool with steatorrhea. 5. Blood picture: Leucopenia with relative lymphocytosis. 6. Hepatitis markers in blood a. Hepatitis A: Anti-HAV antibodies i. IgM ± IgG = recent / acute infection. ii. IgG (without IgM) = immunity to HAV. b. Hepatitis B (HBV has 3 antigens: surface, core, e): i. HBsAg (Hepatitis B surface antigen): Appears 6 weeks after infection → disappears after 3 months (persistence >6m = carrier state OR chronic state) ii. Anti-HBs antibodies: Appear after 3m and persist = recovery OR immunity from infection and in vaccinated individuals. iii. Anti-HBc antibodies Appear with symptoms of acute hepatitis and persist for life. The only markers of hepatitis B detectable in the "window period" (between clearance of HBsAg and appearance of anti- HBs). IgM positive = recent infection

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