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 Jaundice in Adults: A Merck Manual of Patient Symptoms podcast
Jaundice is a yellowish discoloration of the skin and mucous membranes caused by hyperbilirubinemia. Jaundice becomes visible when the bilirubin level is about 2 to 3 mg/dL (34 to 51 μmol/L).
Pathophysiology
Most bilirubin is produced when Hb is broken down into unconjugated bilirubin (and other substances). Unconjugated bilirubin binds to albumin in the blood for transport to the liver, where it is taken up by hepatocytes and conjugated with glucuronic acid to make it water soluble. Conjugated bilirubin is excreted in bile into the duodenum. In the intestine, bacteria metabolize bilirubin to form urobilinogen. Some urobilinogen is eliminated in the feces, and some is reabsorbed, extracted by hepatocytes, reprocessed, and re-excreted in bile (enterohepatic circulation—see Approach to the Patient With Liver Disease: Overview of Bilirubin Metabolism ).
Mechanisms of hyperbilirubinemia:
Hyperbilirubinemia may involve predominantly unconjugated or conjugated bilirubin.
Unconjugated hyperbilirubinemia is most often caused by ≥ 1 of the following:
Conjugated hyperbilirubinemia is most often caused by ≥ 1 of the following:
Consequences:
Outcome is determined primarily by the cause of jaundice and the presence and severity of hepatic dysfunction. Hepatic dysfunction can result in coagulopathy, encephalopathy, and portal hypertension (which can lead to GI bleeding).
Etiology
Although hyperbilirubinemia can be classified as predominantly unconjugated or conjugated, many hepatobiliary disorders cause both forms.
Many conditions (see Approach to the Patient With Liver Disease: Mechanisms and Some Causes of Jaundice in Adults ), including use of certain drugs (see Approach to the Patient With Liver Disease: Some Drugs and Toxins That Can Cause Jaundice), can cause jaundice, but the most common causes overall are
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Table 4
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| Mechanisms and Some Causes of Jaundice in Adults |
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Mechanism
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Examples
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Suggestive Findings*
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Unconjugated hyperbilirubinemia
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Increased bilirubin production
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Common: Hemolysis
Less common: Resorption of large hematomas, ineffective erythropoiesis
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Few or no clinical manifestations of hepatobiliary disease; sometimes anemia, ecchymoses
Serum bilirubin level usually < 3.5 mg/dL (< 59 μmol/L), no bilirubin in urine, normal aminotransferase levels
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Decreased hepatic bilirubin uptake
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Common: Heart failure
Less common: Drugs, fasting, portosystemic shunts
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Decreased hepatic conjugation
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Common: Gilbert syndrome
Less common: Ethinyl estradiol, Crigler-Najjar syndrome, hyperthyroidism
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Conjugated hyperbilirubinemia†
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Hepatocellular dysfunction
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Common: Drugs, toxins, viral hepatitis
Less common: Alcoholic liver disease, hemochromatosis, primary biliary cirrhosis, primary sclerosing cholangitis, steatohepatitis, Wilson disease
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Aminotransferase levels usually > 500 U/L
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Intrahepatic cholestasis
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Common: Alcoholic liver disease, drugs, toxins, viral hepatitis
Less common: Infiltrative disorders (eg, amyloidosis, lymphoma, sarcoidosis, TB), pregnancy, primary biliary cirrhosis, steatohepatitis
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Gradual onset of jaundice, sometimes pruritus
If severe, clay-colored stools, steatorrhea
If long-standing, weight loss
Alkaline phosphatase and GGT usually > 3 times normal
Aminotransferase levels < 200 U/L
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Extrahepatic cholestasis
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Common: Common bile duct stone, pancreatic cancer
Less common: Acute cholangitis, pancreatic pseudocyst, primary sclerosing cholangitis, common duct strictures caused by previous surgery, other tumors
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Depending on cause, manifestations possibly similar to those of intrahepatic cholestasis or a more acute disorder (eg, abdominal pain or vomiting due to a common bile duct stone or acute pancreatitis)
Alkaline phosphatase and GGT usually > 3 times normal
Aminotransferase levels < 200 U/L
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Other, less common mechanisms
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Hereditary disorders (mainly Dubin-Johnson syndrome and Rotor syndrome)
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Normal liver enzymes
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*Symptoms and signs of the causative disorder may be present.
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†Bilirubin is present in urine.
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GGT =
γ-glutamyltransferase.
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Table 5
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| Some Drugs and Toxins That Can Cause Jaundice |
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Mechanism
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Drugs or Toxins
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Increased bilirubin production
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Drugs that cause hemolysis (common among patients with G6PD deficiency), such as sulfa drugs and nitrofurantoin
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Decreased hepatic uptake
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Chloramphenicol, probenecid, rifampin
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Decreased conjugation
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Ethinyl estradiol
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Hepatocellular dysfunction
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Acetaminophen (high dose or overdose), amiodarone, isoniazid, NSAIDs, statins, many others, many drug combinations
Amanita phalloides mushrooms, carbon tetrachloride, phosphorus
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Intrahepatic cholestasis
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Amoxicillin/clavulanate, anabolic steroids, chlorpromazine, pyrrolizidine alkaloids (eg, in herbal preparations), oral contraceptives, phenothiazines
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Evaluation
History:
History of present illness should include onset and duration of jaundice.Hyperbilirubinemia can cause urine to darken before jaundice is visible. Therefore, the onset of dark urine indicates onset of hyperbilirubinemia more accurately than onset of jaundice. Important associated symptoms include fever, prodromal symptoms (eg, fever, malaise, myalgias) before jaundice, urine and stool color, pruritus, steatorrhea, and abdominal pain (including location, severity, duration, and radiation). Important symptoms suggesting severe disease include nausea and vomiting, weight loss, and possible symptoms of coagulopathy (eg, easy bruising or bleeding, tarry or bloody stools).
Review of systems should seek symptoms of possible causes, including weight loss and abdominal pain (cancer); joint pain and swelling (autoimmune or viral hepatitis, hemochromatosis, primary sclerosing cholangitis, sarcoidosis); and missed menses (pregnancy).
Past medical history should identify known causative disorders, such as hepatobiliary disease (eg, gallstones, hepatitis, cirrhosis); disorders that can cause hemolysis (eg, hemoglobinopathy, G6PD deficiency); and disorders associated with liver or biliary disease, including inflammatory bowel disease, infiltrative disorders (eg, amyloidosis, lymphoma, sarcoidosis, TB), and HIV infection or AIDS.
Drug history should include questions about use of drugs or exposure to toxins known to affect the liver (see Table 5: Approach to the Patient With Liver Disease: Some Drugs and Toxins That Can Cause Jaundice) and about vaccination against hepatitis.
Surgical history should include questions about previous surgery on the biliary tract (a potential cause of strictures).
Social history should include questions about risk factors for hepatitis (see Table 6: Approach to the Patient With Liver Disease: Some Risk Factors for Hepatitis), amount and duration of alcohol use, injection drug use, and sexual history.
Family history should include questions about recurrent, mild jaundice in family members and diagnosed hereditary liver disorders. The patient's history of recreational drug and alcohol use should be corroborated by friends or family members when possible.
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Table 6
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| Some Risk Factors for Hepatitis |
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Type of Hepatitis
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Risk Factors
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A
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Day care attendance or employment
Residence or employment in a closed institution
Travel to an endemic area
Oral-anal sex
Ingestion of raw shellfish
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B
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Injection drug use
Hemodialysis
Sharing of razor blades or toothbrushes
Tattooing
Body piercing
Absence of vaccination in health care workers
High-risk sexual activity
Birth in areas of high endemicity
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C
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Blood transfusion before 1992
Injection drug use
Hemodialysis
Exposure during health care work or sexual activity
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Physical examination:
Vital signs are reviewed for fever and signs of systemic toxicity (eg, hypotension, tachycardia).
General appearance is noted, particularly for cachexia and lethargy.
Head and neck examination includes inspection of the sclerae and tongue for icterus and the eyes for Kayser-Fleischer rings. Mild jaundice is best seen by examining the sclerae in natural light; it is usually detectable when serum bilirubin reaches 2 to 2.5 mg/dL (34 to 43 μmol/L). Breath odor should be noted (eg, for fetor hepaticus).
The abdomen is inspected for collateral vasculature, ascites, and surgical scars. The liver is palpated for hepatomegaly, masses, nodularity, and tenderness. The spleen is palpated for splenomegaly. The abdomen is examined for umbilical hernia, shifting dullness, fluid wave, masses, and tenderness. The rectum is examined for gross or occult blood.
Men are checked for testicular atrophy and gynecomastia.
The upper extremities are examined for Dupuytren contractures.
Neurologic examination includes mental status assessment and evaluation for asterixis.
The skin is examined for jaundice, palmar erythema, needle tracks, vascular spiders, excoriations, xanthomas (consistent with primary biliary cirrhosis), paucity of axillary and pubic hair, hyperpigmentation, ecchymoses, petechiae, and purpura.
Red flags:
The following findings are of particular concern:
Interpretation of findings:
Severity of illness is indicated mainly by the degree (if any) of hepatic dysfunction. Ascending cholangitis is a concern because it requires emergency treatment.
Severe hepatic dysfunction is indicated by encephalopathy (eg, mental status change, asterixis) or coagulopathy (eg, easy bleeding, purpura, tarry or heme-positive stool), particularly in patients with signs of portal hypertension (eg, abdominal collateral vasculature, ascites, splenomegaly). Massive upper GI bleeding suggests variceal bleeding due to portal hypertension (and possibly coagulopathy).
Ascending cholangitis is suggested by fever and marked, continuous right upper quadrant abdominal pain; acute pancreatitis with biliary obstruction (eg, due to a common duct stone or pancreatic pseudocyst) may manifest similarly.
Cause of jaundice may be suggested by the following:
Other examination findings can also be helpful (see Table 7: Approach to the Patient With Liver Disease: Findings Suggesting a Cause of Jaundice).
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Table 7
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| Findings Suggesting a Cause of Jaundice |
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Finding
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Possible Causes
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Risk factors
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Alcohol use (heavy)
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Alcoholic liver disease, including alcoholic hepatitis and cirrhosis
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GI cancer
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Extrahepatic biliary obstruction
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Hypercoagulable state
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Hepatic vein thrombosis (Budd-Chiari syndrome)
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Inflammatory bowel disease
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Primary sclerosing cholangitis
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Pregnancy
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Intrahepatic cholestasis, steatohepatitis (acute fatty liver due to pregnancy)
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Previous cholecystectomy
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Biliary stricture
Retained or recurrent common duct stone
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Recent surgery
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Ischemic hepatitis
Benign postoperative intrahepatic cholestasis
Lengthy cardiac bypass surgery
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Symptoms
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Colicky right upper quadrant, right shoulder, or subscapular pain (current or previous)
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Choledocholithiasis
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Constant right upper quadrant pain
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Acute alcoholic or viral hepatitis, acute cholangitis
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Dark urine
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Conjugated hyperbilirubinemia
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Joint pain, swelling, or both
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Hepatitis (autoimmune or viral)
Hemochromatosis
Primary sclerosing cholangitis
Sarcoidosis
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Nausea or vomiting before jaundice
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Acute hepatitis
Common bile duct obstruction by a stone (particularly if accompanied by abdominal pain or rigors)
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Pruritus and clay-colored stools
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Intrahepatic or extrahepatic cholestasis, possibly severe if stools are clay-colored
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Viral prodrome (eg, fever, malaise, myalgias)
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Acute viral hepatitis
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Physical examination
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Abdominal collateral vasculature, ascites, and splenomegaly
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Portal hypertension (eg, due to cirrhosis)
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Cachexia in a patient with a hard, lumpy liver
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Metastases (common)
Cirrhosis (less often)
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Diffuse lymphadenopathy in a patient with acute jaundice
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Infectious mononucleosis
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Diffuse lymphadenopathy in a patient with chronic jaundice
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Lymphoma, leukemia
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Dupuytren contractures, palmar erythema, paucity of axillary and pubic hair, and vascular spiders
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Alcoholic liver disease
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Gynecomastia and testicular atrophy
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Alcoholic liver disease, anabolic steroid use
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Hyperpigmentation
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Hemochromatosis, primary biliary cirrhosis
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Kayser-Fleischer rings
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Wilson disease
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Needle marks
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Hepatitis B or C
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Resolving hematoma
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Extravasation of blood into tissues
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Xanthomas
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Primary biliary cirrhosis
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Testing:
The following are done:
Blood tests include measurement of total and direct bilirubin, aminotransferase, and alkaline phosphatase levels in all patients. Results help differentiate cholestasis from hepatocellular dysfunction (important because patients with cholestasis usually require imaging tests):
Also, patients with hepatocellular dysfunction or cholestasis have dark urine due to bilirubinuria because conjugated bilirubin is excreted in urine; unconjugated bilirubin is not. Bilirubin fractionation also differentiates conjugated from unconjugated forms. When aminotransferase and alkaline phosphatase levels are normal, fractionation of bilirubin can help suggest causes, such as Gilbert syndrome or hemolysis (unconjugated) vs Dubin-Johnson syndrome or Rotor syndrome (conjugated).
Other blood tests are done based on clinical suspicion and initial test findings, as for the following:
Suspicion of hemolysis can be confirmed by a peripheral blood smear.
Imaging is done if pain suggests extrahepatic obstruction or cholangitis or if blood test results suggest cholestasis.
Abdominal ultrasonography is usually done first; usually, it is highly accurate in detecting extrahepatic obstruction. CT and MRI are alternatives. Ultrasonography is usually more accurate for gallstones, and CT is more accurate for pancreatic lesions. All these tests can detect abnormalities in the biliary tree and focal liver lesions but are less accurate in detecting diffuse hepatocellular disorders (eg, hepatitis, cirrhosis).
If ultrasonography shows extrahepatic cholestasis, other tests may be necessary to determine the cause; usually, magnetic resonance cholangiopancreatography (MRCP), endoscopic ultrasonography (EUS), or ERCP is used. ERCP is more invasive but allows treatment of some obstructive lesions (eg, stone removal, stenting of strictures).
Liver biopsy is not commonly required but can help diagnose certain disorders (eg, disorders causing intrahepatic cholestasis, some kinds of hepatitis, some infiltrative disorders, Dubin-Johnson syndrome, hemochromatosis, Wilson disease). Biopsy can also help when liver enzyme abnormalities are unexplained by other tests.
Laparoscopy (peritoneoscopy) allows direct inspection of the liver and gallbladder without the trauma of a full laparotomy. Unexplained cholestatic jaundice warrants laparoscopy occasionally and diagnostic laparotomy rarely.
Treatment
The cause and any complications are treated. Jaundice itself requires no treatment in adults (unlike in neonates—see Metabolic, Electrolyte, and Toxic Disorders in Neonates). Itching, if bothersome, may be relieved with cholestyramine 2 to 8 g po bid. However, cholestyramine is ineffective in patients with complete biliary obstruction.
Geriatrics Essentials
Symptoms may be attenuated or missed in the elderly; eg, abdominal pain may be mild or absent in acute viral hepatitis. A sleep disturbance or mild confusion resulting from portosystemic encephalopathy may be misattributed to dementia.
Key Points
Last full review/revision September 2012 by Steven K. Herrine, MD
Content last modified November 2012
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