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Friday, 6 June 2025

JAUNDICE - SYMPTOMS,TREATMENT AND MANAGEMENT

 


*Definition and Overview -

Jaundice is a clinical sign characterized by a yellowish discoloration of the skin, sclerae (whites of the eyes), and mucous membranes. It results from elevated levels of bilirubin—a yellow pigment produced during the breakdown of red blood cells—in the bloodstream and tissues. Bilirubin normally passes through the liver, where it is conjugated (made water-soluble) and excreted into bile. When any step in this process is disrupted, unconjugated or conjugated bilirubin accumulates, leading to visible yellowing.

1. Physiology and Pathophysiology

  1. Bilirubin Production
    • Senescent red blood cells are broken down in the spleen and reticuloendothelial system.
    • Hemoglobin is metabolized into unconjugated (indirect) bilirubin, which is lipid-soluble and travels bound to albumin in plasma.
  2. Hepatic Uptake and Conjugation
    • In the liver, hepatocytes take up unconjugated bilirubin.
    • Through the action of UDP-glucuronyl transferase, unconjugated bilirubin is converted into conjugated (direct) bilirubin, which is water-soluble.
  3. Excretion
    • Conjugated bilirubin is secreted into bile canaliculi, flows into the biliary tree, and ultimately reaches the intestine.
    • Intestinal bacteria convert it into urobilinogen; some is reabsorbed and excreted in urine, while most is eliminated in feces as stercobilin.
  4. Points of Disruption
    • Pre-hepatic (Hemolytic): Excessive breakdown of red blood cells produces more unconjugated bilirubin than the liver can handle.
    • Hepatic: Intrinsic liver disease (e.g., viral hepatitis, alcoholic liver injury, genetic enzyme defects) impairs uptake, conjugation, or both.
    • Post-hepatic (Obstructive/Cholestatic): Blockage of bile ducts prevents excretion of conjugated bilirubin into the gut (e.g., gallstones, pancreatic head tumors, strictures).

2. Classification of Jaundice

A. Pre-hepatic (Unconjugated, Indirect)

  • Mechanism: Hemolysis or ineffective erythropoiesis overwhelms the liver’s conjugating capacity.
  • Typical findings: Elevated indirect (unconjugated) bilirubin on labs; normal alkaline phosphatase (ALP); normal gamma‐glutamyl transferase (GGT); no dark urine (unconjugated bilirubin is not water-soluble, so it isn’t excreted in urine).
  • Common causes:
    • Hemolytic anemias (e.g., sickle cell disease, autoimmune hemolysis)
    • Hereditary conditions (e.g., Gilbert syndrome, Crigler–Najjar syndrome)
    • Transfusion reactions, malaria, snake bites (in endemic areas)

B. Hepatic (Mixed or Predominantly Indirect or Direct)

  • Mechanism: Dysfunction at hepatocyte level, affecting uptake, conjugation, or excretion.
  • Lab pattern: Elevated both direct (conjugated) and indirect bilirubin (though proportions vary). ALP and GGT may be mildly elevated or normal. Transaminases (AST/ALT) often elevated if there is hepatocellular damage.
  • Common causes:
    • Viral hepatitis (A, B, C, E, etc.)
    • Alcoholic liver disease
    • Nonalcoholic fatty liver disease (NAFLD/NASH)
    • Drug-induced liver injury (e.g., acetaminophen overdose, certain antibiotics)
    • Genetic syndromes (e.g., Dubin-Johnson, Rotor syndrome)

C. Post-hepatic (Obstructive or Cholestatic, Predominantly Conjugated)

  • Mechanism: Physical obstruction of bile flow from the liver to the duodenum.
  • Lab pattern: Predominant elevation of direct (conjugated) bilirubin. Markedly increased ALP and GGT. Dark urine (conjugated bilirubin is water-soluble and spills over into urine), pale or clay‐colored stools (reduced stercobilinogen).
  • Common causes:
    • Gallstones in common bile duct (choledocholithiasis)
    • Cholangiocarcinoma, pancreatic head carcinoma
    • Primary sclerosing cholangitis (PSC), primary biliary cholangitis (PBC)
    • Biliary strictures or post-surgical biliary injury

3. Clinical Presentation

  1. General Signs and Symptoms
    • Yellow discoloration: First noticed in sclerae, then skin/mucous membranes as bilirubin levels rise above approximately 2.5–3 mg/dL.
    • Dark urine: If conjugated bilirubin exceeds renal threshold (typically >2 mg/dL), urine may turn dark amber or tea-colored.
    • Pale stools: In obstructive forms, lack of stercobilin in bile leads to clay-colored or pale stools.
    • Pruritus (itching): Often intense in cholestatic forms due to bile salt deposition in the skin.
  2. Systemic or Underlying Disease Features
    • Pre-hepatic: Signs of hemolysis—fatigue, pallor, tachycardia, splenomegaly, elevated lactate dehydrogenase (LDH), low haptoglobin, reticulocytosis.
    • Hepatic: Malaise, anorexia, nausea/vomiting, right upper quadrant (RUQ) discomfort or pain, hepatomegaly or a tender liver. Features of chronic liver disease (e.g., ascites, spider angiomas, palmar erythema) in long-standing cases.
    • Post-hepatic: Severe colicky or constant RUQ/epigastric pain (e.g., due to gallstone obstruction), weight loss and anorexia if malignant, palpable non-tender gallbladder in carcinoma (“Courvoisier’s sign”).
  3. Associated Findings
    • Fever and chills: May suggest ascending cholangitis if infection of biliary tree is present (Charcot triad: fever/chills, RUQ pain, jaundice).
    • Coagulopathy: Advanced liver disease or obstruction can impair vitamin K metabolism, leading to prolonged prothrombin time (PT)/INR.
    • Fatigue and weight loss: Especially in chronic viral hepatitis or malignancies.

4. Diagnostic Evaluation

  1. Laboratory Tests
    • Serum Bilirubin Fractionation: Distinguish unconjugated versus conjugated dominance.
    • Liver Function Tests (LFTs):
      • AST/ALT: Markedly raised in acute hepatocellular injury (e.g., viral hepatitis).
      • ALP and GGT: Markedly raised in cholestatic/obstructive patterns.
      • Albumin and PT/INR: Assesses synthetic function; hypoalbuminemia and prolonged INR indicate severe or chronic liver disease.
    • Hemolysis Workup (if pre-hepatic suspected): Reticulocyte count, haptoglobin, LDH, peripheral smear, Coombs test (if autoimmune cause suspected).
    • Viral Serologies: Hepatitis A IgM, Hepatitis B surface antigen/IgM core antibody, Hepatitis C antibody/RNA, and others (E, D) depending on epidemiology and risk factors.
    • Autoimmune Markers (if cholestatic or hepatic autoimmune suspected): ANA, anti–smooth muscle antibody (ASMA), anti–mitochondrial antibody (AMA), IgG4 levels.
    • Metabolic and Genetic Tests: Ceruloplasmin (Wilson disease), alpha-1 antitrypsin levels and phenotype, ferritin/transferrin saturation (hemochromatosis), tests for Gilbert/Crigler–Najjar as indicated.
  2. Imaging Studies
    • Abdominal Ultrasound (first-line):
      • Detects biliary dilation (“double-duct” sign), gallstones, masses in liver or pancreas.
      • Assesses hepatic size, texture (fatty infiltration, cirrhosis), and spleen size.
    • Magnetic Resonance Cholangiopancreatography (MRCP): Non-invasive imaging of biliary tree to localize strictures, stones, or tumors.
    • Computed Tomography (CT) Scan: Useful when malignancy (e.g., pancreatic carcinoma) is suspected or to evaluate complications in hepatitis (e.g., liver abscesses).
    • Endoscopic Retrograde Cholangiopancreatography (ERCP): Both diagnostic and therapeutic—can identify obstructing stones or strictures and allow sphincterotomy, stone removal, or stent placement.
    • Liver Biopsy: Reserved for unclear hepatic processes when serology and imaging are inconclusive (e.g., autoimmune hepatitis, infiltrative disorders).
  3. Other Specialized Tests
    • Endoscopic Ultrasound (EUS): For detailed evaluation of pancreas head lesions or small biliary stones missed by transabdominal ultrasound.
    • Percutaneous Transhepatic Cholangiography (PTC): In cases where ERCP is not feasible (e.g., altered gastrointestinal anatomy).
    • Genetic Testing: Confirm inborn errors like Crigler–Najjar, Dubin-Johnson, or Rotor syndrome if suspected from family history and lab patterns.

5. Common Etiologies and Risk Factors

  1. Pre-hepatic (Hemolytic)
    • Hereditary: Sickle cell disease, thalassemias, hereditary spherocytosis, G6PD deficiency.
    • Autoimmune: Autoimmune hemolytic anemia (warm or cold agglutinin types).
    • Infections/Toxins: Malaria (in endemic regions), certain snake venoms, toxins causing red cell destruction.
    • Transfusion Reactions: Acute or delayed hemolytic transfusion reactions.
  2. Hepatic
    • Viral Hepatitis:
      • Hepatitis A/E: Often acute, self-limited, sometimes fulminant in elderly or those with liver disease.
      • Hepatitis B/C/D: Can be acute or chronic; chronic infection predisposes to cirrhosis and hepatocellular carcinoma.
    • Alcoholic Liver Disease:
      • Spectrum from steatosis to alcoholic hepatitis to cirrhosis; often accompanied by AST:ALT ratio >2:1.
    • Non-Alcoholic Fatty Liver Disease (NAFLD)/Non-Alcoholic Steatohepatitis (NASH)
      • Strongly linked to metabolic syndrome (obesity, diabetes, dyslipidemia).
    • Drug-Induced Liver Injury: Acetaminophen overdose, certain antibiotics (e.g., isoniazid), statins, anti-tubercular drugs.
    • Genetic/Metabolic:
      • Wilson’s disease (copper overload)
      • Hemochromatosis (iron overload)
      • Alpha-1 antitrypsin deficiency
      • Gilbert syndrome (benign, mild unconjugated hyperbilirubinemia, often asymptomatic)
      • Crigler–Najjar syndrome (severe unconjugated hyperbilirubinemia in infancy)
  3. Post-hepatic (Obstructive/Cholestatic)
    • Gallstones: Most common cause of extrahepatic obstruction; risk factors summarized by “4 Fs”: female, fat, forty, fertile.
    • Malignancies:
      • Cholangiocarcinoma (bile duct cancer)
      • Pancreatic head carcinoma (Courvoisier’s sign: palpable, nontender gallbladder + jaundice)
      • Ampullary carcinoma
    • Primary Sclerosing Cholangitis (PSC): Chronic progressive fibro-obliterative disease of intrahepatic and extrahepatic bile ducts; associated with ulcerative colitis.
    • Primary Biliary Cholangitis (PBC): Chronic autoimmune cholestatic disease affecting small intrahepatic bile ducts; strongly associated with AMA positivity.
    • Biliary Strictures or Injury: Postoperative (e.g., post-cholecystectomy), traumatic.

6. Management and Treatment

A. General Measures

  • Identify and Treat Underlying Cause: The primary goal is to correct the specific etiology—stop hemolysis, treat viral hepatitis, relieve obstruction, or discontinue hepatotoxic medications.
  • Supportive Care: Maintain hydration, correct electrolyte imbalances, provide nutritional support (especially protein if there is significant hepatic dysfunction), and manage pruritus.

B. Pre-hepatic Jaundice

  • Treat Hemolysis:
    • Autoimmune hemolysis: Corticosteroids or immunosuppressive therapy; in refractory cases, splenectomy.
    • Enzyme deficiencies (e.g., G6PD): Avoid precipitating agents, manage infections promptly.
    • Sickle cell crisis: Hydroxyurea, hydration, pain control, exchange transfusion if needed.

C. Hepatic Jaundice

  • Viral Hepatitis:
    • Hepatitis A/E: Usually supportive (antiemetics, rest); rarely need hospitalization for acute liver failure.
    • Hepatitis B: Antiviral therapy (e.g., tenofovir, entecavir) if severe or chronic.
    • Hepatitis C: Direct-acting antivirals (DAAs) such as sofosbuvir-ledipasvir regimens, based on genotype and liver fibrosis stage.
  • Alcoholic Hepatitis: Abstinence from alcohol, nutritional supplementation (thiamine, folate), corticosteroids in severe cases (Maddrey’s discriminant function >32).
  • NAFLD/NASH: Lifestyle modifications—weight loss through diet and exercise, control of diabetes and dyslipidemia; Vitamin E or pioglitazone in selected NASH patients.
  • Drug-Induced: Discontinue offending drug; N-acetylcysteine for acetaminophen overdose; treat acute liver failure in ICU or transplant center if indicated.
  • Autoimmune Hepatitis: Prednisone ± azathioprine to achieve remission; monitor LFTs and IgG levels.
  • Genetic Disorders:
    • Wilson’s disease: Chelation therapy (penicillamine, trientine) and zinc acetate.
    • Hemochromatosis: Phlebotomy; chelation (deferoxamine) if severe.
    • Alpha-1 antitrypsin deficiency: Supportive; liver transplant in end-stage disease.

D. Post-hepatic (Obstructive) Jaundice

  • Gallstone Obstruction (Choledocholithiasis):
    • ERCP with sphincterotomy and stone extraction; if unsuccessful, percutaneous transhepatic cholangiography (PTC) for drainage.
    • Cholecystectomy after resolution of acute obstruction to prevent recurrence.
  • Benign Strictures: Endoscopic balloon dilatation with or without stenting; surgical reconstruction if refractory.
  • Malignant Obstruction:
    • Decompression by ERCP-guided biliary stent placement (plastic or metal stent).
    • Surgical resection if early-stage (e.g., Whipple procedure for resectable pancreatic head carcinoma).
    • Palliative options: Percutaneous transhepatic biliary drainage (PTBD), photodynamic therapy or radiofrequency ablation for cholangiocarcinoma.
  • Cholangitis (Ascending):
    • Emergent broad-spectrum antibiotics covering Gram-negative rods and anaerobes (e.g., piperacillin-tazobactam, ceftriaxone + metronidazole).
    • Urgent biliary decompression (ERCP or PTBD) once stabilized.

7. Complications and Prognosis

  1. Acute Liver Failure (in fulminant hepatic causes)
    • Encephalopathy, coagulopathy, cerebral edema; high mortality without liver transplant.
  2. Chronic Liver Disease
    • Progression to cirrhosis, portal hypertension, variceal bleeding, ascites, hepatic encephalopathy, hepatocellular carcinoma.
  3. Cholangitis / Sepsis
    • Untreated biliary obstruction can lead to ascending cholangitis, sepsis, and multi-organ failure.
  4. Nutritional Deficiencies
    • Chronic cholestasis can cause fat‐soluble vitamin deficiency (A, D, E, K).
  5. Pruritus and Quality of Life
    • Severe pruritus in cholestatic jaundice often requires medications (e.g., cholestyramine, rifampin, sertraline, or UVB phototherapy).

Prognostic Factors

  • Underlying cause (e.g., Gilbert syndrome has excellent prognosis; acute fulminant hepatitis may require transplant).
  • Degree and duration of bilirubin elevation; rapid progression of coagulopathy or encephalopathy suggests poor outcome.
  • Presence of comorbidities (e.g., HIV/HCV co-infection, alcoholic cirrhosis).

8. Prevention and Patient Education

  1. Vaccination
    • Hepatitis A vaccine for travelers to endemic regions or high-risk groups.
    • Hepatitis B vaccine for all infants and unvaccinated adults at risk (healthcare workers, hemodialysis patients, sexual exposure).
  2. Lifestyle Modifications
    • Moderation or abstinence from alcohol; limit hepatotoxic substances.
    • Healthy diet and regular exercise to prevent NAFLD/NASH.
    • Avoidance of drugs and herbal supplements known to cause liver injury.
  3. Safe Practices
    • Safe blood transfusion/screening to prevent transfusion-transmitted viral hepatitis.
    • Use of barrier protection and safe needle practices to reduce risk of hepatitis B/C.
  4. Screening in High-Risk Populations
    • Periodic LFTs and ultrasound for patients with chronic hepatitis B/C to detect early cirrhosis or hepatocellular carcinoma.
    • Family screening for hereditary conditions when indicated (e.g., hemochromatosis, Wilson’s disease).
  5. Prompt Evaluation of Symptoms
    • Early medical attention for unexplained jaundice, dark urine, clay-colored stools, severe abdominal pain, or pruritus to detect reversible causes.

9. Summary

  • Jaundice is a hallmark of disrupted bilirubin metabolism, appearing yellowish once serum bilirubin exceeds roughly 2.5–3 mg/dL.
  • It is classified by site of dysfunction: pre-hepatic (hemolytic), hepatic (hepatocellular or metabolic), and post-hepatic (cholestatic/obstructive).
  • History and physical exam, combined with laboratory tests (bilirubin fractions, liver enzymes, hemolysis workup) and imaging (ultrasound, MRCP, ERCP as needed), usually pinpoint the cause.
  • Management involves treating the underlying cause (e.g., antivirals for hepatitis, ERCP for obstructive stones), providing supportive measures, and preventing complications.
  • Preventive strategies include vaccination (hepatitis A/B), safe practices to avoid blood-borne infections, lifestyle changes for metabolic and alcoholic liver disease, and early evaluation of symptoms.

By understanding the mechanisms, forms, and appropriate workup of jaundice, clinicians can tailor investigations and interventions—ranging from simple observation in mild Gilbert syndrome to urgent biliary decompression in ascending cholangitis—to optimize outcomes and prevent long-term sequelae.

 

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