Table 10.
Case reports of liver function alteration associated with intake of food supplements containing monacolin K from RYR preparations, published in the scientific literature
| Patient data | Daily intake of monacolin Ka | Period of intake | Adverse effects | Reference |
|---|---|---|---|---|
| Female, 63 years old | 15–30 mg | 6 months | Severe lobular necroinflammatory changes at liver biopsy; previous mild hepatotoxicity during therapy with lovastatin | Grieco et al. (2009) |
| Female, 53 years old | 3 mg | 60 days | Increased level of ALT and AST, GGT | Lapi et al. (2008) |
| Male, 49 years old | 5 mg | 60 days | Increased level of ALT and AST | Lapi et al. (2008) |
| Female, 42 years old | 3 mg | 30 days | Acute hepatitis with hospitalisation | Mazzanti et al. (2017) |
| Female, 46 years old | 3 mg | 50 days | Acute hepatitis with hospitalisation | Mazzanti et al. (2017) |
| Female, 58 years old | 3 mg | 60 days | Increased level of AST (2x normal level) | Mazzanti et al. (2017) |
| Female, 68 years old | 3 mg | 15 days | Increased level of pancreas and hepatic enzymes | Mazzanti et al. (2017) |
| Female, 68 years old | 3 mg | 1 year | Increased level of transaminases; previous statin intolerance | Mazzanti et al. (2017) |
| Male, 35 years old | 3 mg | 60 days | Toxic acute hepatitis with hospitalisation | Mazzanti et al. (2017) |
| Male, 36 years old | 3 mg | 76 days | Acute hepatitis with hospitalisation | Mazzanti et al. (2017) |
ALT: alanine aminotransferase; AST: aspartate aminotransferase; GGT: gamma‐glutamyl transpeptidase.
a
Ingredients other than monacolin K may be present in the products.