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Disease Categories > Gastrointestinal Disease

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Liver Disease Evaluation

In most cases, the diagnosis of liver disease can be made using a carefully obtained history, physical examination and a few laboratory tests.

Biochemical tests of liver function
- Do not usually suggest a specific disease
- Do suggest a category of liver disease (eg cholestatic versus hepatocellular patterns)
- Can be normal in the presence of liver disease
- Do not accurately assess the functionality of the liver
- Best used in groups as a battery of tests to assess:
  - Hepatocellular damage
  - Cholestasis
  - Excretory function
  - Biosynthetic function
Tests of hepatocellular damage
- Laboratory testing
  - Aspartate aminotransferase (AST)
    - Found in numerous tissues including the liver, cardiac muscle, skeletal muscle, kidneys, brain and pancreas
  - Alanine aminotransferase (ALT)
    - Found primarily in the liver
- Pathophysiology
  - Release of enzymes into the blood occurs when the liver cell membrane is damaged
    - Poor correlation exists between the degree of liver damage and the level of aminotransferases
    - Level of aminotransferases does not provide prognosis for liver necrosis or permanent damage
- Elevated enzymes
  - Modest (<300 U/L – seen in any type of liver disorder)
    - Alcoholism
    - Gallstone-induced
    - Metabolic diseases
    - Acute and chronic hepatitis
  - Striking (>1000U/L)
    - Acute hepatitis
    - Toxin/Drug-induced hepatitis
    - Ischemic damage to the liver
Tests of cholestasis
- Laboratory testing
  - Alkaline phosphatase (ALP)
    - Isoenzymes include liver, bone, placental, and intestinal forms of ALP
    - Usually increased during periods of growth (eg, children, teenagers)
    - Elevated enzymes
      - Up to 3-fold elevation may be seen in any liver disease – not specific for cholestasis
      - Sole elevation of ALP should lead to isoenzyme testing or gammaglutamyl transferase and 5’ nucleotidase testing
      - Isolated elevation of the liver isoenzyme is suspicious for early cholestasis, but may also reflect tumor or granulomatous disease
      - Level of elevation is not helpful in distinguishing intrahepatic from extrahepatic causes of cholestasis
  - Gammaglutamyl transferase (GGT)
    - Very sensitive to small liver insults (e.g. alcohol consumption)
    - May be elevated in hepatocellular disease
  - 5’ nucleotidase (5’NT)
    - Very sensitive and specific for hepatobiliary disease
    - Can distinguish isolated elevations of ALP as liver related
  - Elevated ALT, AST, GGT and 5’NT
    - Highly suggestive of liver as source of disease
Tests of excretory function
- Laboratory testing
  - Serum bilirubin
    - 3 fractions – conjugated, unconjugated, and delta bilirubin (albumin-bound)
    - Elevated total bilirubin due to primarily
      - Unconjugated bilirubin – rarely reflects liver disease, commonly found in hemolytic disease
      - Conjugated bilirubin – almost always reflects hepatobiliary disease
      - Delta bilirubin – reflects hepatobiliary disease and remains elevated longer than other bilirubin fractions during the convalescent phase of liver disease
    - Causes jaundice when concentrations exceed 1.5 mg/dL
  - Urine bilirubin
    - Performed qualitatively using a urine dipstick
    - Any bilirubin found in the urine is the water-soluble conjugated fraction and its presence implies hepatobiliary disease
  - Blood ammonia
    - Liver converts ammonia to urea
      - Significant liver dysfunction results in elevated serum ammonia
    - Poor correlation between ammonia level and degree of liver disease
Tests of biosynthetic function
- Laboratory testing
  - Albumin – see Nutritional Assessment-Proteins (ARUP Consult topic)
  - Globulins
  - Coagulation factors
    - All factors except for factor VIII are produced in the liver
    - Factors II, V, VII and X are vitamin K sensitive (meaning they require adequate quantities of vitamin K for production)
    - Prothrombin time (PT) is a collective measure of factors II, V, VII and X
      - Elevated PT unresponsive to vitamin K supplementation suggests poor liver functionality
Diagnosis
- Initial screening for suspected liver disease should include AST, ALT, ALP and total bilirubin
  - Further testing based on results from initial screening battery
  - Prior to initiation of exhaustive evaluation of modestly elevated liver function tests (<2 times above normal for AST< ALT, ALP), recommend repeat serum testing

Indications for Ordering

Tests generally appear in the order most useful for common clinical situations
Click on number for test-specific information in the ARUP Laboratory Test Directory

Test Name and Number	Recommended Use	Follow Up
Hepatic Function Panel 0020416 Method: Refer to individual components.	Initial screening test for hepatobiliary problems This panel includes testing for albumin (serum or plasma), alkaline phosphatase (serum or plasma), aspartate aminotransferase (serum or plasma), alanine aminotransferase (serum or plasma), bilirubin, direct (serum or plasma), protein, total (plasma or serum), and bilirubin, total (serum or plasma)
Aspartate Aminotransferase, Serum or Plasma 0020007 Method: Enzymatic	Initial screening test for hepatobiliary problems
Alanine Aminotransferase, Serum or Plasma 0020008 Method: Enzymatic	Initial screening test for hepatobiliary problems
Alkaline Phosphatase, Serum or Plasma 0020005 Method: Enzymatic	Initial screening test for hepatobiliary problems
Gamma Glutamyl Transferase, Serum or Plasma 0020009 Method: Enzymatic	Determine if enzyme elevation is due to hepatocellular pattern
5'Nucleotidase 0080235 Method: Enzymatic	Use if alkaline phosphatase is elevated and fractionated alkaline phosphatase shows both bone and liver fractions	If 5'nucleotidase is normal but alkaline phosphatase is elevated, perform bone-specific alkaline phosphatase testing
Bilirubin, Direct & Total, Serum or Plasma 0020426 Method: Spectrophotometry	Initial screening test for hepatobiliary problems

Additional Tests Available

Click on number for test-specific information in the ARUP Laboratory Test Directory

Test Name and Number	Comments
Alkaline Phosphatase Isoenzymes 0021020 Method: Heat Inactivation/Enzymatic
Bone Specific Alkaline Phosphatase 0070053 Method: Chemiluminescent Immunoassay
Bilirubin, Direct, Body Fluid 0020511 Method: Spectrophotometry
Bilirubin, Direct, Serum or Plasma 0020033 Method: Spectrophotometry
Bilirubin, Total (Neonatal), Plasma or Serum 0020114 Method: Spectrophotometry
Albumin, Serum by Nephelometry 0050671 Method: Nephelometry
Prothrombin Time 0030215 Method: Electromagnetic Mechanical Clot Detection
Prothrombin Time with Reflex to PT 1:1 Mix 0030163 Method: Electromagnetic Mechanical Clot Detection
Ammonia, Plasma 0020043 Method: Colorimetry
Alkaline Phosphatase Isoenzymes 0021020 Method: Heat Inactivation/Enzymatic
Lactate Dehydrogenase, Isoenzymes 0020413 Method: Enzymatic/Electrophoresis

General References

Adams LA, Talwalkar JA. Diagnostic evaluation of nonalcoholic fatty liver disease. J Clin Gastroenterol. 2006;40(3 Suppl 1):S34-S38. (Link to PubMed)

Astegiano M, Sapone N, Demarchi B, Rossetti S, Bonardi R, Rizzetto M. Laboratory evaluation of the patient with liver disease. Eur Rev Med Pharmacol Sci. 2004;8(1):3-9. (Link to PubMed)

Burke MD. Liver function: test selection and interpretation of results. Clin Lab Med. 2002;22(2):377-390. (Link to PubMed)

Gressner OA, Weiskirchen R, Gressner AM. Biomarkers of liver fibrosis: clinical translation of molecular pathogenesis or based on liver-dependent malfunction tests. Clin Chim Acta. 2007;381(2):107-113. (Link to PubMed)

Grigorescu M. Noninvasive biochemical markers of liver fibrosis. J Gastrointestin Liver Dis. 2006;15(2):149-159. (Link to PubMed)

Heidelbaugh JJ, Bruderly M. Cirrhosis and chronic liver failure: part I. Diagnosis and evaluation. Am Fam Physician. 2006;74(5):756-762. (Link to PubMed)

Henderson AR and Moss DW. Enzymes. In Burtis CA and Ashwood ER, eds. Tietz Fundamentals of Clinical Chemistry, 5th ed. Philadelphia: WB Saunders, 2001. pp. 352-389.

Knight JA. Liver function tests: their role in the diagnosis of hepatobiliary diseases. J Infus Nurs. 2005;28(2):108-117. (Link to PubMed)

Luxon BA. Noninvasive tests for liver fibrosis. Postgrad Med. 2006;119(3):8-13. (Link to PubMed)

Moitra V, Diaz G, Sladen RN. Monitoring hepatic and renal function. Anesthesiol Clin. 2006;24(4):857-8ix. (Link to PubMed)

Plebani M, Basso D. Non-invasive assessment of chronic liver and gastric diseases. Clin Chim Acta. 2007;381(1):39-49. (Link to PubMed)

Ritchie AH, Williscroft DM. Elevated liver enzymes as a predictor of liver injury in stable blunt abdominal trauma patients: case report and systematic review of the literature. Can J Rural Med. 2006;11(4):283-287. (Link to PubMed)

Schneider PD. Preoperative assessment of liver function. Surg Clin North Am. 2004;84(2):355-373. (Link to PubMed)

Sotil EU, Jensen DM. Serum enzymes associated with cholestasis. Clin Liver Dis. 2004;8(1):41-54, vi. (Link to PubMed)

Reviewed by

Grenache, David G., Ph.D. Medical Director, Special Chemistry at ARUP Laboratories; Assistant Professor, Clinical Pathology, University of Utah

Lehman, Christopher M., M.D. Co-Medical Director, University Hospital Clinical Laboratory; Associate Professor, Clinical Pathology, University of Utah

Roberts, William L. , M.D., Ph.D. Medical Director, Automated Core Laboratory at ARUP Laboratories; Professor, Pathology, University of Utah

Comprehensive Review: November 2007
Last Update: May 2008