Diabetes Mellitus Clinical Trial
Official title:
Living With Statins - The Impact of Cholesterol Lowering Drugs on Health, Lifestyle and Well-being
Background Statins are cholesterol lowering drugs that are prescribed to lower the risk of
cardio-vascular diseases. The use of statins has increased markedly and it is now one of the
most prescribed drugs in the world. 600,000 people in Denmark are taking statins on a daily
basis, 40 % of these are taking the medication without having any other risk factors for
cardio-vascular diseases than elevated blood-cholesterol i.e. they are in primary
prevention.
Statins are not without side effects and studies have shown that there is an elevated risk
of developing diabetes when taking statins. This has led to an increased debate about the
use of statins in primary prevention. Furthermore a large meta-analysis has shown that to
prevent one event of cardio-vascular disease, it is necessary to treat 200 people for 3-5
years. These data suggest that more conservative use of statins to prevent CVD in otherwise
healthy individuals at low risk for future CVD may be warranted.
Other side effects of statins are muscle myalgia, muscle cramps and fatigue which
potentially can prevent a physically active lifestyle. The biomedical background of these
side effects is not fully elucidated but it has been shown that there is a link to
decreasing levels of an important enzyme, Q10, which plays a role in muscle energy
metabolism.
Hypothesis
The overarching research question is: why does statin treatment cause muscle pain? Does
statin treatment impair (or even prevent) physical exercise training? Furthermore we would
like to answer the following questions:
1. Does statin treatment impair (or even prohibit) physical exercise training?
2. Does statin treatment cause:
- Decreased muscle strength?
- Skeletal muscle inflammation?
- Decreased mitochondrial respiratory function?
3. Abnormal glucose homeostasis?
Background
HYPERCHOLESTEROLEMIA AND STATIN USE IN DENMARK
Simvastatin is the most commonly prescribed statin, a class of drugs that inhibit
hydroxyl-methyl-glutaryl (HMG) coenzyme A reductase, and thereby blocking biosynthesis of
cholesterol in the liver. Simvastatin is prescribed for individuals with elevated
low-density lipoprotein cholesterol (LDL-C) and/or total cholesterol, because these clinical
parameters are viewed as a risk factor for cardiovascular-disease (CVD), even in the absence
of other health problems or risk factors, such as previous myocardial infarction, diabetes
or hypertension.
Approximately 40% of the prescriptions for statins are issued for primary prevention of
elevated cholesterol by general practitioners to patients without bodily symptoms or signs.
Only the "cholesterol number" makes the risk of heart attack and stroke visible. The lack of
symptoms is likely to be of importance for patients' adherence to treatment as is adverse
effects. A number of factors, such as information in mass media and changes in daily life,
may affect the decision to take the treatment
TREATMENT GUIDELINES FOR HYPERCHOLESTEROLEMIA
The guidelines (8; 10) indicate preventive treatment with statins is appropriate in
individuals with >10% predicted risk of a major vascular event within 5 years, while, some,
but not all opinion-leaders advocate a 5% threshold (2; 8). Nevertheless, statin therapy
failed to reduce all-cause mortality in a meta-study of 65,229 patients without CVD, some of
whom had diabetes (11). Similarly, a Cochrane review analysis, which included some studies
in which more than 10% of the patients had history of CVD, showed only 0.5% reduction in
all-cause mortality, indicating that for every 200 patients taking statins daily for 5
years, 1 death would be prevented (13). These data suggest that more conservative use of
statins to prevent CVD in otherwise healthy individuals at low risk for future CVD may be
warranted.
THE DOWN-SIDE
Rhabdomyolysis (skeletal muscle cell death) is an infrequent but serious side-effect of
statin use, that can on rare occasion lead to acute renal failure and death (i.e., 1.5
deaths per 106 prescriptions (9)). Statin use is much more frequently associated with muscle
dysfunction, including myalgia (muscle pain), cramps, and weakness. The reported incidence
of myalgia varies from 1% (pharmaceutical company reports) to as high as 75% in
statin-treated athletes (7; 9). Mild to severe myalgia is a strong disincentive to regular
exercise, and because regular exercise is one of the critical life-style approaches to
preventing CVD and reducing blood cholesterol, this is a significant down-side of statin
use. Regular exercise is also effective in preventing and treating obesity and type 2
diabetes, which themselves are risk factors for CVD (16).
The mechanism behind the myalgia is not known. However, we have recently demonstrated that
muscle mitochondrial function is impaired with statin treatment and the Q10 protein may play
a key role in this (6). In addition, the statins also negatively affect the glucose
tolerance (6), increasing the risk of type 2 diabetes.
RESEARCH QUESTIONS:
The overarching research question is: why does statin treatment cause muscle pain? We are
not the only research group in the world that try to answer that question, but we are the
only one that has indeed provided a mechanistic explanation, and provided a proof-of-concept
(6). We will now test this in a larger patient population.
Our background in muscle and exercise physiology and in bioenergetics makes it natural to
further ask:
1. Does statin treatment impair (or even prohibit) physical exercise training?
2. Does statin treatment cause:
- Decreased muscle strength?
- Skeletal muscle inflammation?
- Decreased mitochondrial respiratory function?
3. Abnormal glucose homeostasis?
Re question B & C: If so, can physical training counteract this effect of statin treatment?
Methodology
COHORT
Patients that fulfil defined inclusion and exclusion criteria will be recruited from General
Practice clinics in Copenhagen and news paper advertisements. The vast majority of these
patients are being treated on basis of the HeartScore risk estimation system that offers
direct estimation of the ten-year risk of fatal cardiovascular disease in a format suited to
the constraints of clinical practice (14) (www.HeartScore.org).
60 patients both men and women (age: 40-70 years; BMI: 25-35 kg/m2) taking Simvastatin as
primary prevention are recruited. No other risk factors for CVD except elevated total
cholesterol and/or elevated LDL cholesterol and mild hypertension (<145/100 mm Hg) must be
present.
The patients will be allocated (randomization by drawing a lot) to one of two groups:
- Simvastatin 40 mg/day and Q10-supplementation 400 mg/day
- Simvastatin 40 mg/day and Q10-placebo The intervention period is 8 weeks with a series
of experimental days before and after.
Experimental days (identical before and after the interventions):
Day 1 (½ day - overnight fasting):
- Medical history; clinical examination + ECG. Measurements: Blood pressure, weight,
height, W/H-ratio, thigh circumference.
- Dual Energy X-ray Absorptiometry-scan (DXA) (body composition and body fat).
- FatMax test and maximal oxygen uptake test (VO2-max) or ergometer bike.
Day 2 (½ day - overnight fasting):
- Oral glucose tolerance test + score questionnaire for muscle pain/discomfort (Visual
Analog Scale) and a questionnaire regarding the extent of muscle pain/discomfort.
- Isokinetic strength and Rate of Force Development (PowerRig and KinCom dynamometer).
- Repeated VO2-max-test
Day 3 (1 day - overnight fasting):
- Muscle biopsy, vastus lateralis (before and after clamp), fat biopsy from subcutaneus
adipose tissue in the abdomen.
- Intravenous glucose tolerance test (IVGTT)
- Euglycemic, hyperinsulinaemic clamp.
Statistical considerations
The major end-points are all end-point which we have tested before in other clinical
populations. In general, in order to detect a 10% difference in these parameters before vs.
after a training program or between statin users and control, requires 15-20 subjects in
each group if an alpha level of <0.05 and risk of type 2 error is set to 10%. 10-15 subjects
are necessary if the "conventional" 20% type 2 error risk is implemented. Thus, the present
study has a considerable safety-margin in terms of statistical power.
;
Allocation: Randomized, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Investigator), Primary Purpose: Basic Science
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