Alkaline Phosphatase – Levels, Causes and Significance
Alkaline phosphatase (ALP) is an enzyme found in the blood that provides important information about the health of the liver, bones, and bile ducts. Elevated or decreased levels may indicate various medical conditions.
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Alkaline phosphatase (ALP) is an enzyme found in the blood that provides important information about the health of the liver, bones, and bile ducts. Elevated or decreased levels may indicate various medical conditions.
What is Alkaline Phosphatase?
Alkaline phosphatase (ALP) is an enzyme present in several tissues throughout the body, most notably the liver, bones, kidneys, intestines, and placenta. In clinical practice, ALP levels are routinely measured in blood serum and serve as a key diagnostic marker for liver disease, bile duct disorders, and bone metabolism conditions. The enzyme is most active at an alkaline pH (approximately 8–10), which is reflected in its name.
Biological Function
Alkaline phosphatase catalyzes the removal of phosphate groups from various molecules. Depending on the tissue of origin, it serves different physiological roles:
- Liver ALP: Involved in bile secretion and bile duct metabolism.
- Bone ALP: Plays a crucial role in bone formation and mineralization.
- Intestinal ALP: Supports fat digestion and the intestinal barrier function.
- Placental ALP: Elevated during pregnancy, particularly in the third trimester.
Reference Values
Normal ALP levels vary by age and sex. Generally accepted reference ranges for adults are:
- Women: approximately 35–105 U/L
- Men: approximately 40–130 U/L
In children and adolescents, ALP levels are physiologically much higher due to active bone growth. Exact reference ranges may vary slightly between laboratories.
Elevated Alkaline Phosphatase – Causes
An elevated ALP level (hyperphosphatasemia) can indicate a range of conditions:
Liver and Bile Duct Disorders
- Cholestasis (bile flow obstruction)
- Gallstones or bile duct blockage
- Primary biliary cholangitis (PBC)
- Primary sclerosing cholangitis (PSC)
- Hepatitis (liver inflammation)
- Liver cirrhosis
- Liver metastases or liver cancer
Bone Disorders
- Paget disease of bone
- Bone metastases
- Osteomalacia (softening of the bones)
- Rickets
- Bone fractures (transiently elevated)
- Hyperparathyroidism (overactive parathyroid glands)
Other Causes
- Pregnancy (physiological, especially in the third trimester)
- Heart failure
- Thyroid disorders
- Certain medications (e.g., antiepileptics, antibiotics, corticosteroids)
Low Alkaline Phosphatase – Causes
A decreased ALP level is less common but can also be clinically significant:
- Hypophosphatasia: A rare inherited metabolic disorder characterized by a genetic deficiency of ALP
- Severe anemia
- Hypothyroidism (underactive thyroid)
- Zinc or magnesium deficiency
- Certain cardiac conditions
Diagnosis and Differentiation
Since ALP originates from multiple tissues, an elevated result often prompts isoenzyme testing to identify the specific source of the elevated enzyme. Additional laboratory values are used in the diagnostic workup:
- Gamma-GT (GGT): When both are elevated, a liver origin is strongly suggested.
- AST and ALT: Additional liver enzymes for differentiation.
- Bilirubin: Indicates possible cholestasis or liver disease.
- Bone metabolism markers (e.g., osteocalcin, crosslinks) when a bone disorder is suspected.
Imaging techniques such as ultrasound, CT, or MRI, and in some cases a liver biopsy, may be used for further evaluation.
Clinical Significance and Treatment
Alkaline phosphatase is an important diagnostic parameter, but it is not a disease in itself. Treatment is always directed at the underlying cause:
- For bile duct disorders: endoscopic or surgical procedures to relieve bile flow obstruction
- For liver disease: pharmacological therapy, lifestyle modification, or in severe cases liver transplantation
- For bone disorders: depending on the diagnosis, bisphosphonates, vitamin D and calcium supplementation, or condition-specific therapies
- For hypophosphatasia: enzyme replacement therapy with asfotase alfa
References
- European Association for the Study of the Liver (EASL): Clinical Practice Guidelines on the management of cholestatic liver diseases. Journal of Hepatology, 2009; 51(2): 237–267.
- Kasper DL et al. – Harrison's Principles of Internal Medicine, 21st edition, McGraw-Hill Education (2022).
- Mornet E. – Hypophosphatasia. Orphanet Journal of Rare Diseases, 2007; 2:40. Available at: https://ojrd.biomedcentral.com (accessed 2024).
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