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The acid form of 2-hydroxyatorvastatin (2-OH-ATV) can be con... Show undefined attributes

created	[InstanceEdit:9756889] Jassal, Bijay, 2021-10-19
dbId	9756890
displayName	The acid form of 2-hydroxyatorvastatin (2-OH-ATV) can be con...
literatureReference	[LiteratureReference:9757268] Statin induced myotoxicity: the lactone forms are more potent than the acid forms in human skeletal muscle cells in vitro [LiteratureReference:9757277] The UGT1A32 polymorphism affects atorvastatin lactonization and lipid-lowering effect in healthy volunteers [LiteratureReference:9757284] UGT1A128 is associated with decreased systemic exposure of atorvastatin lactone
modified	[InstanceEdit:9761519] D'Eustachio, Peter, 2022-01-14
schemaClass	Summation
text	The acid form of 2-hydroxyatorvastatin (2-OH-ATV) can be converted to its lactone form (2-OH-ATVL) primarily by UDP-glucuronosyltransferase 1A3 (UGT1A3), with small contributions from UGT1A1 and 2B7 (Prueksaritanont et al. 2002, Schirris et al. 2015). The lactonization process involves the formation of an unstable acyl glucuronide intermediate (not described here). Increased generation of ATVL due to polymorphisms in UGT1A1, 1A3, and 2B7 may be contributing factors in statin-induced myopathies (Riedmaier et al. 2010). In vitro, the lactone forms of ATV show a higher potency to induce myotoxicity in human skeletal cells than their acid counterparts (Skottheim et al. 2008, Cho et al. 2012). Carriers of less strongly expressed alleles of UGT enzymes may have decreased exposure to the suspected muscle-toxic metabolite atorvastatin lactone (Stormo et al. 2013).

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[BlackBoxEvent:R-HSA-9756134] UGT1A3 lactonizes 2-OH-ATV to 2-OH-ATVL

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