Gastrointestinal varices laboratory findings: Difference between revisions

Editor-In-Chief: C. Michael Gibson, M.S., M.D. [1]; Associate Editor(s)-in-Chief: Syed Hassan A. Kazmi BSc, MD [2]

Overview

Cirrhosis of the liver is the most common cause of portal hypertension worldwide. A range of laboratory values may be obtained in the evaluation of cirrhosis, in order to determine disease severity and causation. Liver function tests, complete blood count, basic metabolic panel and coagulation factors are standard in the evaluation of cirrhosis. More specific testing for markers and serum enzymes may be performed when certain etiologies are suspected.

Laboratory Findings

Markers of chronic liver disease/cirrhosis

• Laboratory abnormalities may be the first indication of cirrhosis.

• Common abnormalities include:^{[1][2][3][4][5]}
  • Increased serum bilirubin levels^[6]
  • Abnormal aminotransferase levels ^{[7][3][8][9][10][11][12][13][14][15][16]}
  • Elevated alkaline phosphatase 
  • Elevated gamma-glutamyl transpeptidase 
  • Prolonged prothrombin time/INR
  • Thrombocytopenia
  • Hyponatremia 

Liver function tests:

•  Aminotransferases:^{[17][18][19][20][21][22][23]}
  • LFTs may be normal in cirrhosis patients
  • Aspartate aminotransferase (AST) and alanine aminotransferase (ALT) are usually moderately elevated
  • AST is more often elevated than ALT
  • Alcoholic liver disease - AST and ALT are both elevated but less than 300 IU/L with a AST: ALT ratio > 2.0
• Alkaline phosphatase: ^[24]
  • Alkaline phosphatase is usually elevated
  • Usually less than two to three times the upper limit
  • High levels may be seen in patients with underlying cholestatic liver disease such as:
    • Primary biliary cirrhosis
    • Primary sclerosing cholangitis
• Gamma-glutamyl transpeptidase:^[24][25][26]
  • Non specific
  • Correlates with ALP levels
  • Higher in chronic liver disease (CLD) due to alcohol use:
  • Mechanism of raised GGT in alcoholic liver disease:
    • Alcohol induces microsomal GGT in liver
    • Alcohol causes GGT release from hepatocytes
  • Albumin:
    • Albumin levels reflect synthetic function of the liver
    • Serum albumin levels helps grade the severity of cirrhosis
    • Hypoalbuminemia is non specific for liver disease and may be seen in:
      • Heart failure
      • Malnutrition
      • Protein-losing enteropathy
      • Nephrotic syndrome

• Bilirubin:
  • Bilirubin levels may be normal or raised
• Prothrombin time: ^[27]
  • Prothrombin time reflects the degree of hepatic synthetic function.
  • Worsening coagulopathy correlates with the severity of hepatic dysfunction.
• Metabolic panel:
  • Hyponatremia^[28]
    • common in patients with cirrhosis and ascites and is related to an inability to excrete free water.
    • Reflects poor prognosis
    • Due to ADH elevation
  • Progressive rise in serum creatinine: may be indicative of hepatorenal syndrome

Hematologic abnormalities:  ^[29]

• Thrombocytopenia: most common hematologic abnormality in cirrhosis
  • Rarely results in a platelet count < 50,000/mL
  • Mechanism of thrombocytopenia:
    • Caused by portal hypertension with congestive splenomegaly: sequesters circulating platelets
    • Decreased thrombopoietin levels

• Anemia
  • Mechanism of anemia:
  • Acute and chronic gastrointestinal blood loss 
  • Folate deficiency
  • Hemolysis
  • Anemia of chronic disease
  • Direct toxicity due to alcohol 
  • Hypersplenism 
  • Bone marrow suppression ( hepatitis-associated aplastic anemia) 
• Leukopenia/neutropenia: due to hypersplenism with splenic margination
• Coagulation defects - the liver produces most of the coagulation factors and coagulopathy correlates with worsening liver disease

• Other abnormalities :
  • Globulins: increase due to shunting of bacterial antigens away from the liver to lymphoid tissue which induces immunoglobulin production.^[30]
  • Disseminated intravascular coagulation 
  • Vitamin K deficiency
  • Diabetes: seen in patients with hemochromatosis ^[31][32]
  • Insulin resistance: seen in nonalcoholic fatty liver disease
  • Dysfibrinogenemia
  • Fibrinolysis

• Ascitic fluid analysis:
  • A diagnostic paracentesis may be performed if the ascites is new or if the patient with ascites is being admitted to the hospital.
  • The fluid is analysed for the following:
    • Gross appearance
    • Protein level
    • Albumin
    • WBC, RBC counts
    • Gram stain
    • cytology^[33]
  • Serum-ascites albumin gradient (SAAG) is probably a better discriminant than older measures (transudate versus exudate) for the causes of ascites.^[34]
  • A high gradient (> 1.1 g/dL) indicates the ascites is due to portal hypertension
  • A low gradient (< 1.1 g/dL) indicates ascites of non-portal hypertensive etiology
  • Ascites is broadly classified as two types based on the Serum-ascites albumin gradient (SAAG):
    • Transudate - SAAG > 1.1 g/dL (indicates the ascites is due to portal hypertension)
    • Exudate - SAAG < 1.1 g/dL (indicates the ascites is due to non-portal hypertension etiology)

AST to platelet ratio index (APRI)

• APRI value of less than equal to 0.5 rules out significant fibrosis and cirrhosis, and a value of greater than equal to 1.5 rules in significant fibrosis^[35][36]

FibroTest

• A validated and patented combination of six serum markers as non-invasive biomarkers of fibrosis are included in the FibroTest.^[37]
• The FibroTest score is correlated with the degree of liver damage in people with a variety of liver diseases
• FibroTest score is calculated combining the following six serum markers with the age and gender of the patient:
  • Alpha-2-macroglobulin
  •  Haptoglobin
  •  Apolipoprotein A1
  •  Gamma-glutamyl transpeptidase (GGT)
  • Total bilirubin
  • Alanine transaminase (ALT)

Other laboratory studies performed in newly diagnosed cirrhosis may include:

• Serology for hepatitis viruses.
• Autoantibodies
  • ANA - present in autoimmune hepatitis
  • Anti-smooth muscle antibody - present in autoimmune hepatitis
  • Anti-mitochondrial antibody - present in primary biliary cirrhosis
  • Anti-LKM
• Total iron, TIBC, transferrin saturation, and ferritin - elevated totat iron, reduced TIBC, elevated transferrin saturation, and elevated ferritin in hemochromatosis.
• Serum ceruloplasmin- low in Wilson's disease
• Immunoglobulin levels (IgG, IgM, IgA) - these are non-specific but may assist in distinguishing various causes.
  • Chronic hepatitis B - Chronic hepatitis B can be diagnosed with detection of HBsAg > 6 months after initial infection.
  • HBeAg and HBV DNA are determined to assess whether or not patients will need antiviral therapy.
• Serum protein electrophoresis - alpha-1 band absent in alpha-1 antitrypsin deficiency.
• Cholesterol and glucose
• Alpha 1-antitrypsin - reduced in alpha-1 antitrypsin deficiency.

Combination of tests

• Clinical prediction rules exist to help diagnosis cirrhosis according to a systematic review by the Rational Clinical Examination project.^[2]
• Pohl's Index:
  • Cirrhosis is very likely when AST/ALT ratio ≥1 and platelet count ≤ 150,000/mm^{3 [38]}

• The Bonacini score is based on the ALT/AST ratio, platelet count, and INR.^[39]
  • A score of > 7 or 8 makes cirrhosis more likely.^[40]
  • A score of < 3 makes cirrhosis less likely.^[40]

• Another method is the Lok index^[41]

• Online calculators are available (link 1 and link 2).

• In diagnosis of cirrhosis (Ishak scores, 5-6) in patients with hepatitis C, the aspartate aminotransferase to platelet ratio index (APRI) ratio > 1 suggests cirrhosis with an accuracy of:^[42]
  • Sensitivity = 79%
  • Specificity = 78%

• A more recent meta-analysis has focused on the diagnosis of cirrhosis among patients with hepatitis C^[43] using the Lok index:
  • < 0.2 has negative likelihood ratio of 0.21
  • > 0.6 has positive likelihood ratio of 4.4

References

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