GASTROENTEROLOGY,  LIVER DISEASE

Mild, Asymptomatic Elevations of ALT and AST

June 15, 2024 / No Comments

gathered from : https://www.aafp.org/pubs/afp/issues/2017/1201/p709.html

Prevalence

  • Estimated prevalence of elevated transaminase levels in primary care: ~10%
  • Less than 5% of these patients have serious liver disease

General Guidelines

  • Mild elevations: Less than five times the upper limit of normal (ULN)
  • Immediate evaluation warranted for elevations greater than five times ULN

Causes of Elevated Liver Transaminase Levels

  • Hepatocellular Damage:
    • ALT and AST released during hepatocellular damage
    • ALT elevations more specific for liver injury
    • AST elevations can be caused by extrahepatic disorders (e.g., thyroid disorders, celiac sprue, hemolysis, muscle disorders)

Normal ALT Levels

  • Males: 29 to 33 IU/L (0.48 to 0.55 μkat/L)
  • Females: 19 to 25 IU/L (0.32 to 0.42 μkat/L)

AST Ratio

  • Alcoholic Liver Disease:
    • AST ratio > 2
    • Mean AST values: 152:70
    • Positive likelihood ratio (LR+): 17
    • Negative likelihood ratio (LR–): 0.49
  • Nonalcoholic Fatty Liver Disease (NAFLD):
    • ASTratio < 1
    • Mean ASTvalues: 66:91
    • LR+: 80
    • LR–: 0.2

Categorization of Causes for Mild, Asymptomatic Elevation of Transaminase Levels

  • Common Causes:
    • Nonalcoholic fatty liver disease (NAFLD)
    • Chronic hepatitis B and C
    • Alcoholic liver disease
    • Medications (e.g., statins, NSAIDs, acetaminophen)
    • Metabolic syndrome
  • Uncommon Causes:
    • Hemochromatosis
    • Wilson disease
    • Alpha-1 antitrypsin deficiency
    • Autoimmune hepatitis
    • Celiac disease
  • Rare Causes:
    • Hemolysis
    • Muscle disorders (e.g., polymyositis, muscular dystrophy)
    • Thyroid disorders (e.g., hypothyroidism, hyperthyroidism)
    • Adrenal insufficiency

Nonalcoholic Fatty Liver Disease (NAFLD):

  • Prevalence: Most common cause of asymptomatic transaminase elevation (25% to 51%).
  • Subtypes:
    • Nonalcoholic Fatty Liver (NAFL): Hepatic steatosis without inflammation.
      • Treatment: Lifestyle modifications (weight loss, diet, exercise).
    • Nonalcoholic Steatohepatitis (NASH): Hepatocyte injury with ballooning, inflammation, potential fibrosis.
      • Risk: Progression to cirrhosis and hepatocellular carcinoma.
      • Prevalence: 3% to 5% of the adult population.
  • Risk Factors:
    • Metabolic syndrome (waist circumference, elevated BP, high triglycerides, low HDL, insulin resistance).
    • Type 2 diabetes mellitus.
  • Diagnosis:
    • Imaging: Ultrasonography preferred; does not differentiate NAFL and NASH.
    • NAFLD Fibrosis Score: Assesses risk of liver-related complications using clinical data (age, BMI, AST/ALT ratio, platelets, albumin, presence of diabetes).
    • Vibration-Controlled Transient Elastography: Noninvasive assessment of hepatic fibrosis, limited by operator experience and high BMI.
  • Clinical Management:
    • High-risk patients or those with coexisting liver diseases should be referred to a gastroenterologist.

Alcoholic Liver Disease:

  • Primary Cause: Liver-related mortality in Western countries.
  • Overlap with NAFLD: Similar disease spectrum and histopathology.
  • Diagnostic Tool: Alcoholic liver disease/NAFLD index (ALT level, AST level, height, MCV, sex, weight).
    • Validation: Positive likelihood ratio (LR+) = 12, negative likelihood ratio (LR–) = 0.07.

Drug-Induced Liver Injury (DILI):

  • Incidence: Estimated at 19.1 cases per 100,000 persons annually.
  • Identification: Detailed history of prescription, over-the-counter medications, and supplements.
  • Common Drugs:
    • Acetaminophen, statins, antibiotics (tetracyclines, fluoroquinolones), NSAIDs, anti-seizure drugs (valproic acid, phenytoin), anti-tuberculosis drugs (isoniazid, rifampin).
    • Herbal supplements also contribute to DILI (9% of cases).
  • Resources: Liver-Tox for clinical information on DILI.
  • Statins: Safe in stable chronic liver diseases like NAFLD and hepatitis C; FDA recommends only baseline ALT/AST before initiation

Viral Hepatitis:

  • Prevalence in the US:
    • Hepatitis C: ~3.5 million persons.
    • Hepatitis B: Up to 2.2 million persons.
  • Screening: Hepatitis B surface antigen and hepatitis C virus antibody testing for high-risk patients (USPSTF guidelines).

Hereditary Hemochromatosis:

  • Genetics: Autosomal recessive; common in Northern European Caucasians (1 in 150 to 250 persons).
  • Phenotypic Expression: Severe iron overload in ~10% of those with genotype.
  • Diagnosis:
    • Initial Tests: Transferrin saturation (>45%) and serum ferritin (>250-300 ng/mL in men, >200 ng/mL in women).
    • Genetic Testing: HFE mutations (C282Y, H63D).
    • Higher Predictive Thresholds: Transferrin saturation >60% in men, >50% in women for 95% predictive accuracy.

Alpha1-Antitrypsin Deficiency (AATD):

  • Prevalence: 1 in 3,000 to 5,000 persons; only 10% diagnosed.
  • Clinical Presentation: Early-onset emphysema, unexplained liver enzyme elevation, advanced liver disease.
  • Diagnosis:
    • Initial Test: Serum alpha1-antitrypsin levels.
    • Follow-Up: Protein phenotyping or genotyping for PiZZ variant if levels are low.

Autoimmune Hepatitis:

  • Prevalence: 11 to 17 per 100,000 persons.
  • Demographics: More common in young women; associated with other autoimmune disorders.
  • Diagnosis:
    • Tests: Hypergammaglobulinemia (IgG levels), serum protein electrophoresis, antinuclear antibody (ANA), smooth muscle antibody (SMA), liver/kidney microsome type 1 antibody (anti-LKM1).

Wilson Disease:

  • Prevalence: 1 in 30,000 persons; autosomal recessive.
  • Clinical Clues: Kayser-Fleischer rings, neuropsychiatric symptoms.
  • Diagnosis:
    • Initial Test: Serum ceruloplasmin.
    • Further Testing: 24-hour urine copper levels, genetic testing, liver biopsy if ceruloplasmin is low.

Extrahepatic Causes

  • Thyroid Disorders:
    • Patterns: Both hypo- and hyperthyroidism can cause elevated transaminase levels.
    • Screening: Thyroid-stimulating hormone (TSH), free T4, free/total T3.
  • Celiac Disease:
    • Association: Modest elevations in transaminase levels.
    • Screening: Tissue transglutaminase IgA, serum IgA level, anti-deamidated gliadin peptide IgG.
  • Other Considerations:
    • Hemolysis: Consider if clinical picture suggests.
    • Strenuous Exercise: Temporary elevation in transaminase levels.
    • Rhabdomyolysis and Polymyositis: Creatine kinase or aldolase measurements in patients with significant myalgias.

Suggested Diagnostic Evaluation

  • Large Prospective Study (UK):
    • Evaluated nearly 1,300 primary care patients with abnormal transaminase levels.
    • Findings:
      • 38% had fatty liver disease.
      • Less than 5% had significant liver disease.
      • Serious liver disease in 1.3% (viral hepatitis, hereditary hemochromatosis).
      • 84% of abnormal liver enzyme results remained abnormal after one month, 75% after two years.
  • Evaluation Recommendations:
    • Initial Assessment:
      • Thorough patient history and physical examination.
      • Consider common, uncommon, and rare causes.
    • Diagnostic Tools:
      • Imaging (ultrasonography, transient elastography).
      • Clinical scores (NAFLD fibrosis score).
      • Specific lab tests (autoantibodies, genetic testing).

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