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. Author manuscript; available in PMC: 2010 Apr 6.
Published in final edited form as: Am J Cardiovasc Drugs. 2008;8(6):373–418. doi: 10.2165/0129784-200808060-00004

Table II.

Evidence For, and Suggestive Of, Dose/Potency Dependence of Statin Adverse Effects (AEs)

AE Comment
All AEs - OR 1.4; 95% CI 1.09-1.80, p=0.008 statin therapy vs placebo175 (meta-analysis of placebo-controlled RCTs).
- OR 1.44; 95% CI 1.33-1.55, p<0.001 intensive- vs moderate-dose statin therapy176 (meta-analysis of RCTs).
AEs Leading to
Discontinuation of
Therapy		 - OR 1.28; 95% CI 1.18-1.39, p<0.001 intensive- vs moderate-dose statin therapy176 (meta-analysis of RCTs).
Note: Though intensive-dose statins lead to more discontinuation due to AEs than moderate-dose statins,
moderate-dose statins do not necessarily lead to more discontinuation due to AEs than placebo177 (meta-analysis
of RCTs).
CK Elevation Although some meta-analyses fail to show significant CK elevations with statins (usually moderate dose) vs
placebo,177 meta-analysis of head-to-head RCTs of high- vs low- potency statins showed a significant increase in
CK elevation with high-dose statins:

  • CK elevation OR 6.12 with higher- vs lower- dose statin therapy (95% CI 1.36-27.5).178 The odds appeared to be greater for lipophilic statins, which can more readily enter muscle tissue.

  • CK elevation OR 9.97 with intensive vs less intensive statins (95% CI 1.3-77.9, p=0.028).176
LFT Elevation - Meta-analyses of RCTs show significant increases in LFTs with statin vs placebo (risk difference per 1000
patients 4.2, 95% CI 1.5-6.9).177
- Meta-analysis of head-to-head RCTs of higher- vs lower- potency statins showed significant increase in LFT
elevation with higher-dose statins:

  • LFT (transaminase) elevation OR 2.7 (1.5-5.0) with higher vs lower dose statins.178 The effect appeared to be greater for hydrophilic statins (pravastatin, the most hydrophilic, is actively taken up into the liver).

  • LFT elevation (alanine or aspartate aminotransferase ≥3 times the ULN) OR 4.5 (95% CI 3.3-6.2) with intensive- vs nonintensive- statin therapy.176


- In a different study design, looking not at dose, but LDL-C reduction, the magnitude of LDL-C drop was not
related to AE risk. In contrast, the higher the statin dose needed to achieve a given LDL-C reduction, the higher
the rates of elevated LFTs.181 For many reasons, this type of study is less interpretable from a dose-response
standpoint.a
Rhabdomyolysis - Excess rhabdomyolysis cases on cerivastatin primarily involved high-potency use and/or combination with
gemfibrozil, which increases the effective dose.170, 171, 179
- Drugs that inhibit the CYP3A4 system and thereby increase statin concentrations (e.g. for atorvastatin,
simvastatin, lovastatin, and cerivastatin) increase risk for statin AEs (including rhabdomyolysis) 6-fold,167
supporting a dose relationship of statins to AEs.
- In a VA database, when statins were combined with agents that inhibit their clearance (CYP3A4 inhibitors) the
rate of rhabdomyolysis was increased 3- to 5-fold.185
- US FDA Advisory advised caution with high-dose (40mg) rosuvastatin due to elevated risk of
rhabdomyolysis.180
- In a meta-analysis of RCTs, the percent LDL-C reduction was not associated with rhabdomyolysis risk.
(However, LDL-C reduction is a problematic metric – see footnote a; and footnote b in Table IV – and more so
across trials since sample differences can swamp dose effects.181a)
- In the SEARCH trial in which 12,064 subjects were randomized to 20 or 80mg simvastatin, there were 49
cases of “definite myopathy” in the simvastatin 80mg group and 2 in the simvastatin 20mg group.186b There
were 49 of “incipient myopathy” in the simvastatin 80mg group and 6 in the simvastatin 20mg group.b
- See also Table IV, ‘Risk Factors for Statin Adverse Effects (AEs).’
Non-CK Elevating
Muscle Symptoms		 Recurrence of statin AEs was significantly higher when subjects were rechallenged with an equivalent expected
potency statin, relative to a lower potency statin (~95% vs 55%, p<0.01).37
Cancer According to a meta-analysis of statin RCTs, achieved LDL-C levels were significantly inversely related to
cancer risk (p=0.009), though LDL-C reduction was not.181 On average statins do not increase cancer in those
under age 70 years in clinical trials (see Table VII). One could postulate a relation to LDL-C transport of
antioxidants or cholesterol status as a precursor to vitamin D.
Proteinuria FDA Advisory: “Mild, transient proteinuria (or protein in the urine, usually from the tubules), with and without
microscopic hematuria (minute amounts of blood in the urine), occurred with Crestor [rosuvastatin], as it has
with other statins, in Crestor's pre-approval trials. The frequency of occurrence of proteinuria appeared dose-
related.” 180
Glycemia - Atorvastatin 80mg increased glycemia significantly on average in the PROVE-IT –TIMI trial.184
- Rosuvastatin 20mg vs placebo significantly increased HbA1c (p=0.001), and increased newly diagnosed
diabetes mellitus (relative risk 1.25; p=0.01) in the JUPITER trial.187
- Lower statin potencies have led to reproducible elevations in glucose in individual subjects,182 but elevations in
glucose or HbA1c have usually not been reported on average in RCTs of low- or moderate-dose statins
(although in one RCT the statin group exhibited a modest but statistically significant increase in HbA1c183).

ALT = alanine aminotransferase; CK = creatine kinase; CYP = cytochrome P450; HbA1c = glycosylated hemoglobin; JUPITER = Justification for the Use of Statins in Prevention: an Intervention Trial Evaluating Rosuvastatin; LDL-C = low-density lipoprotein cholesterol; LFTs = liver function tests; OR = odds ratio; PROVE-IT–TIMI = Pravastatin or Atorvastatin Evaluation and Infection Therapy – Thrombolysis in Myocardial Infarction trial; RCT = randomized controlled trial; SEARCH = Study of the Effectiveness of Additional Reductions in Cholesterol and Homocysteine; ULN = upper limit of normal; VA = US Department of Veterans Affairs.

a

Statin use is associated with transcriptional upregulation of HMG-CoA reductase.188 We suggest that persons on statins with more unfavorable antioxidant/oxidant state may (on average) upregulate HMG-CoA reductase especially strongly in response to statins. Lesser LDL-C reduction for the same dose may signal a less favorable oxidant/antioxidant milieu on average,189 which in turn may be associated with higher risk of statin AEs.51-53 Consistent with this, LDL-C tachyphylaxis occurred with high-dose atorvastatin, but not if coenzyme Q10 was concurrently administered (2005 International Coenzyme Q10 Association Meeting presentation190). LDL-C reduction for a given dose may not be a good way to examine dose effects. For some persons, the same statin dose may confer a lesser LDL-C reduction due to factors that promote oxidation and thus may also increase AE risk. In contrast, for some persons, the same statin dose may confer greater LDL-C reduction due to factors that increase statin assimilation or reduce clearance, which may also, by causing functionally greater statin ‘dose,’ increase AE risk. (See also Table IV, footnote b.)

b

“Definite myopathy” was defined as muscle symptoms with CK elevations exceeding 10× ULN (meeting definitions of rhabdomyolysis that do not require renal involvement); “incipient myopathy” was defined as CK exceeding 3× ULN and more than 5× baseline CK, coupled with an ALT elevation exceeding 1.7× baseline ALT without an isolated ALT elevation at any other visit, irrespective of muscle symptoms.186 (Note that ALT elevation reflects liver compromise and is not a characteristic of myopathy. However, concurrent muscle and liver dysfunction may signal widespread cellular consequences of statins.)