GASTROENTEROLOGY,  LIVER DISEASE

Liver Function Tests (LFTs)

June 15, 2024 / No Comments

from : https://www.ncbi.nlm.nih.gov/books/NBK482489/

Liver Anatomy and Function

  • Located in the right upper quadrant of the body, below the diaphragm.
  • Responsible for:
    • Primary detoxification of various metabolites.
    • Synthesizing proteins.
    • Producing digestive enzymes.
    • Metabolism regulation.
    • Regulation of red blood cells (RBCs).
    • Glucose synthesis and storage.

Liver Function Tests (LFTs)

  • Tests typically include:
    • Alanine aminotransferase (ALT)
    • Aspartate aminotransferase (AST)
    • Alkaline phosphatase (ALP)
    • Gamma-glutamyl transferase (GGT)
    • 5’nucleotidase
    • Total bilirubin
    • Conjugated (direct) bilirubin
    • Unconjugated (indirect) bilirubin
    • Prothrombin time (PT)
    • International normalized ratio (INR)
    • Lactate dehydrogenase
    • Total protein
    • Globulins
    • Albumin
  • These tests help determine the area of hepatic injury and organize a differential diagnosis.

Patterns of Liver Injury

  • Hepatocellular Disease: Elevated ALT and AST out of proportion to ALP and bilirubin.
  • Cholestatic Pattern: Elevated ALP and bilirubin out of proportion to ALT and AST.
  • Mixed Injury Pattern: Elevation of both ALP and AST/ALT levels.
  • Isolated Hyperbilirubinemia: Elevation of bilirubin with normal ALP and AST/ALT levels.

Etiology and Epidemiology

  • Elevated liver function tests are found in ~8% of the general population.
  • Transient elevations may resolve after three weeks in asymptomatic patients.
  • Interpretation should be cautious to avoid unnecessary testing.
  • Borderline AST and/or ALT elevation: <2 times the upper limit of normal (ULN).
  • Mild elevation: 2-5 times ULN.
  • Moderate elevation: 5-15 times ULN.
  • Severe elevation: >15 times ULN.
  • Massive elevation: >10,000 IU/L.

Differential Diagnosis Based on Elevated LFTs

  • Hepatocellular Pattern: Elevated aminotransferases out of proportion to alkaline phosphatase.
    • ALT-Predominant Causes:
      • Acute or chronic viral hepatitis
      • Steatohepatitis
      • Acute Budd-Chiari syndrome
      • Ischemic hepatitis
      • Autoimmune hepatitis
      • Hemochromatosis
      • Medications/toxins
      • Alpha1-antitrypsin deficiency
      • Wilson disease
      • Celiac disease
    • AST-Predominant Causes:
      • Alcohol-related liver disease
      • Steatohepatitis
      • Cirrhosis
      • Non-hepatic causes (hemolysis, myopathy, thyroid disease, exercise)
  • Cholestatic Pattern: Elevated alkaline phosphatase + gamma-glutamyl transferase + bilirubin out of proportion to AST and ALT.
    • Hepatobiliary Causes:
      • Bile duct obstruction
      • Primary biliary cirrhosis
      • Primary sclerosing cholangitis
      • Medication-induced cholestasis
      • Infiltrating diseases (sarcoidosis, amyloidosis, lymphoma)
      • Cystic fibrosis
      • Hepatic metastasis
    • Non-Hepatic Causes:
      • Bone disease
      • Pregnancy
      • Chronic renal failure
      • Lymphoma or other malignancies
      • Congestive heart failure
      • Childhood growth
      • Infection or inflammation

Components of Liver Function Test

Hepatocellular Labs

  • Aminotransferase:
    • Includes AST (Aspartate Aminotransferase) and ALT (Alanine Aminotransferase).
    • Markers of hepatocellular injury.
    • Participate in gluconeogenesis:
      • AST: Catalyzes transfer of amino group from aspartic acid to ketoglutaric acid, producing oxaloacetic acid.
      • ALT: Catalyzes transfer of amino group from alanine to ketoglutaric acid, producing pyruvic acid.
  • AST (Aspartate Aminotransferase):
    • Exists as cytosolic and mitochondrial isoenzymes.
    • Found in liver, cardiac muscle, skeletal muscle, kidneys, brain, pancreas, lungs, leukocytes, and red cells.
    • Less sensitive and specific for liver injury compared to ALT.
    • Elevation may occur due to nonhepatic causes.
    • AST activity is higher in neonates and infants, declining to adult levels by approximately six months.
  • ALT (Alanine Aminotransferase):
    • Cytosolic enzyme, highly concentrated in the liver.
    • Half-life: Approximately 47 ± 10 hours.
    • Typically higher than AST in most liver diseases where enzyme activity is from hepatocyte cytosol.
    • Hepatocellular injury (not necessarily cell death) triggers the release of these enzymes into circulation.
    • Higher values in normal males compared to females.
    • Correlates with obesity; normal reference range higher in individuals with higher body mass index.

Cholestasis Labs

  • Alkaline Phosphatase (ALP):
    • Family of zinc metalloenzymes concentrated in the microvilli of the bile canaliculus and other tissues (bone, intestines, placenta).
    • Four isozymes:
      • Placental ALP (hPLALP)
      • Germ Cell ALP (GCALP or PLALP-like)
      • Intestinal ALP (IALP)
      • Tissue-Nonspecific ALP (TNALP)
    • Heat stability:
      • PLALP and GCALP: Most heat stable at 65°C.
      • Bone ALP: Least heat stable.
    • In healthy non-smokers, PLALP and GCALP < 1% of total ALP activity in serum.
    • Benign transient hyperphosphatasemia:
      • Marked rise in ALP, often several thousand IU/L.
      • Associated with concurrent infections in >60% of cases.
      • Characteristic pattern on polyacrylamide gel electrophoresis.
      • Benign condition, ALP returns to normal in 6-8 weeks.
  • Gamma-Glutamyltransferase (GGT):
    • Located on cell membranes with high secretory or absorptive activities.
    • Catalyzes the transfer of a gamma-glutamyl group from peptides to other amino acids.
    • Specific for biliary disease, not present in bone.
    • Increased in obstructive liver disease (average 12-fold compared to ALP’s 3-fold increase).
    • Useful in distinguishing idiopathic cholestasis with or without bile duct involvement.
    • Levels affected by breastfeeding due to high GGT in breast milk postpartum.
    • Higher levels in individuals with BMI > 30 kg/m² due to liver fat deposition (steatosis).
    • Raised in liver diseases causing fibrosis/cirrhosis, space-occupying lesions, granulomatous disease.
  • 5′-Nucleotidase (5′NT):
    • Associated with canalicular and sinusoidal plasma membranes.
    • Found in intestine, brain, heart, blood vessels, and endocrine pancreas.
    • Identifies the organ source of isolated ALP elevation.
    • Not increased in bone disease, primarily elevated in hepatobiliary disease.
  • Lactate Dehydrogenase (LDH):
    • Commonly included in liver panels.
    • Poor diagnostic specificity for liver disease.
    • Markedly increased in hepatocellular necrosis, shock liver, lymphoma, or hemolysis associated with liver disease.
  • Bilirubin:
    • End product of heme catabolism (80% from hemoglobin).
    • Unconjugated bilirubin:
      • Transported to the liver bound to albumin.
      • Water-insoluble, not excreted in urine.
    • Conjugated bilirubin:
      • Water-soluble, appears in urine.
      • Conjugated to bilirubin glucuronide in the liver, secreted into bile and gut.

Synthetic Function Tests

  • Albumin:
    • Synthesized by hepatic parenchymal cells.
    • Synthesis rate dependent on colloidal osmotic pressure and dietary protein intake.
    • Feedback regulation by plasma albumin concentration.
    • Maintenance possible with only 10% of normal hepatocyte mass.
    • Half-life: 21 days.
    • Found in almost all extracellular body fluids.
    • Catabolized in various tissues via pinocytosis and intracellular proteolysis.
    • Low serum albumin in liver disease indicates decreased synthesis.
    • Normal liver function with low serum albumin may indicate:
      • Poor protein intake (malnutrition).
      • Protein loss (nephrotic syndrome, malabsorption, protein-losing enteropathy).
  • Prothrombin Time (PT):
    • Measures rate of conversion of prothrombin to thrombin.
    • Dependent on factors II, V, VII, and X, all synthesized in the liver.
    • Delayed PT with normal liver function may indicate:
      • Warfarin treatment.
      • Consumptive coagulopathy (e.g., disseminated intravascular coagulopathy).
      • Vitamin K deficiency.

Serological Tests

  • Autoantibodies for Autoimmune Liver Diseases:
    • Autoimmune Hepatitis Type 1 (AIH-1):
      • Anti-nuclear antibody (ANA).
      • Smooth muscle antibody (SMA).
    • Autoimmune Hepatitis Type 2 (AIH-2):
      • Antibody to liver kidney microsomal antigen type-1 (anti-LKM1).
      • Anti-liver cytosol type 1 (anti-LC1).
    • Primary Biliary Cirrhosis (PBC):
      • Antimitochondrial antibodies (AMA).
      • ANA reacting with nuclear pore gp210 and nuclear body sp100.
    • Sclerosing Cholangitis:
      • Primary Sclerosing Cholangitis (PSC): Atypical perinuclear anti-neutrophil cytoplasmic antibody (p-ANCA).
      • Autoimmune Sclerosing Cholangitis (ASC): Serological features resembling AIH-1.

Secondary Biochemical Liver Tests

  • Alpha-Fetoprotein (AFP):
    • Tumor marker for primary hepatocellular malignancies (e.g., hepatoblastoma, HCC).
    • Raised in regenerating liver, especially in chronic viral hepatitis.
  • Carbohydrate Deficient Transferrin:
    • High-specificity test for detecting excess alcohol intake causing liver damage.
  • Carbohydrate Antigen CA19-9:
    • Monitors activity of PSC, which may progress to cholangiocarcinoma.
  • Serum Ferritin:
    • Useful for identifying hemochromatosis.
    • Positive acute phase reactant, raised in many illnesses and acute hepatic failure due to hepatocyte damage.

Results, Reporting, and Critical Findings

Correlation with Patient History and Physical Examination

  • Important aspects to review:
    • Patient’s age
    • Past medical history (e.g., diabetes, obesity, hyperlipidemia, inflammatory bowel disease, celiac sprue, thyroid disorders, autoimmune hepatitis, acquired muscle disorders)
    • Alcohol use disorder
    • Medication use
    • Toxin exposure
    • Family history of genetic liver conditions (Wilson disease, alpha-1-antitrypsin deficiency, hereditary hemochromatosis)
  • Review of systems for signs and symptoms of chronic liver disease:
    • Jaundice
    • Ascites
    • Peripheral edema
    • Hepatosplenomegaly
    • Gynecomastia
    • Testicular hypotrophy
    • Muscle wasting
    • Encephalopathy
    • Pruritus
    • Gastrointestinal bleeding
  • Additional tests to determine cause of elevated transaminase levels:
    • Fasting lipid levels
    • Hemoglobin A1C level
    • Fasting glucose
    • Complete blood count with platelets
    • Complete metabolic panel
    • Iron studies
    • Hepatitis C antibody
    • Hepatitis B surface antigen testing

Reference Ranges for Liver Function Tests (LFTs)

  • Variations depending on laboratory, sex, and body mass index (BMI)
  • Each laboratory should establish its own reference interval based on methodology
  • Typical reference ranges:
    • Alanine transaminase (ALT): 4 to 36 IU/L
    • Aspartate transaminase (AST): 5 to 30 IU/L
    • Alkaline phosphatase (ALP): 30 to 120 IU/L
    • Gamma-glutamyltransferase (GGT): 6-50 IU/L
    • Bilirubin: 2 to 17 µmol/L
    • Direct bilirubin: 0 to 6 µmol/L
    • Prothrombin time (PT): 10.9 to 12.5 seconds
    • Albumin: 35-50 g/L
    • Total protein: 60 to 80 g/L
    • Lactate dehydrogenase (LDH): 50 to 150 IU/L

Clinical Significance

  • Alcohol:
    • AST to ALT ratio ≥ 2:1 suggests alcoholic liver disease
    • Elevated GGT also suggests alcohol abuse, but GGT alone is not specific
  • Medications:
    • Many medications can cause liver damage (e.g., NSAIDs, antibiotics, statins, anti-seizure drugs, tuberculosis treatment drugs)
    • Acute hepatocellular injury linked to drugs like acetaminophen, allopurinol, NSAIDs, anti-tuberculosis medications, statins, antifungals, antibiotics, anti-seizure drugs, antidepressants, antipsychotics, antivirals
    • Acute cholestasis linked to drugs like anabolic steroids, NSAIDs, tricyclic antidepressants, alcohol, antibiotics
    • Long-term use of certain drugs (e.g., methotrexate) can lead to chronic liver damage
  • Viral Hepatitis:
    • Common cause of hepatitis and elevated LFTs
    • Hepatitis B, C, and D can cause chronic hepatitis; Hepatitis A and E cause acute hepatitis
    • Other viruses (HIV, EBV, CMV) can also cause hepatitis
  • Autoimmune Hepatitis:
    • Chronic disease with ongoing hepatocellular inflammation, necrosis, potential progression to cirrhosis
    • More common in young women
    • Positive autoantibodies (ANA, SMA, anti-LKM1, anti-LC1)
  • Hepatic Steatosis and Nonalcoholic Steatohepatitis (NASH):
    • Overweight individuals, type II diabetes, dyslipidemia
    • Elevated AST and ALT with a 1:1 ratio, other liver function tests normal
  • Hemochromatosis:
    • Abnormal iron accumulation leading to organ toxicity
    • Clinical manifestations: diabetes, liver disease, cutaneous hyperpigmentation
    • Diagnosis: Raised serum ferritin, transferrin saturation > 45%, HFE mutations
  • Wilson Disease:
    • Autosomal-recessive disorder of copper metabolism
    • Clinical clue: Kayser-Fleischer rings (not always present)
    • Diagnosis: Low serum ceruloplasmin, 24-hour urinary copper excretion, liver biopsy
  • Alpha-1 Antitrypsin Deficiency (AATD):
    • Genetic condition leading to obstructive pulmonary disease and liver disease
    • Common among Caucasians, often undiagnosed
  • Celiac Disease:
    • Gluten sensitivity disorder with modest elevations in liver transaminases
    • Screening: tissue transglutaminase IgA, serum IgA level, anti-deamidated gliadin peptide IgG
  • Thyroid Disorders:
    • Hypothyroidism and hyperthyroidism associated with abnormal liver enzymes
    • Screening: thyroid stimulating hormone, selective testing of free T4 and free/total T3

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