FDA Approves Dangerous and Worthless Cholesterol Drug - Brownstein

FDA Approves Dangerous and Worthless Cholesterol Drug

by Dr. David Brownstein

On May 3, 2013, the FDA approved a Big Pharma Cartel founding member Merck drug Liptruzet.  Liptruzet is a combination drug of Zetia and Lipitor.  I wrote to you about the failure of Zetia in three separate blog posts.  They can all be found by clicking here:  http://blog.drbrownstein.com/?s=zetia.
Zetia is a failed drug.  It should never be prescribed and should have been pulled from the market years ago.  There is no excuse for any doctor prescribing Zetia for any condition.  Zetia works by blocking cholesterol absorption in the gut.  Conventional doctors believe that drug therapies that lower cholesterol levels reduce the risk of heart disease.  However, Zetia, which has been around for over 10 years, has never been shown to lower the risk of developing a heart attack or stroke.  Furthermore, Zetia has never been shown to prolong life.

Why the FDA would approve this combination of Zetia and Lipitor is beyond belief.  The previous combination of Zetia and Zocor, known as Vytorin, was proven to be a colossal failure in multiple studies—see my previous blog posts.

FDA’s action is a perfect example of why we spend more money on health care than any other people on the planet.  Liptruzet will cost $5.50 per pill.  This means a patient prescribed Liptruzet will spend over $2,000.00 per year on a worthless drug that will be associated with side effects such as muscle aches and pains, memory loss, and neurological disorders.  We take too many ineffective drugs that are too expensive.  Do all of these drugs translate into better healthcare outcomes?  Heck no.  As compared to every other wealthy Western country, we finish last or near the bottom on every single health indicator.  In Liptruzet’s case, there is no justifiable reason for the FDA to approve it.  This is another example, amongst many, of why the FDA should be disbanded.  The FDA gives false credibility to Big Pharma.

If you are on Zetia, I suggest talking to your doctor about stopping it.  Ask him/her for any studies showing a clinical benefit such as a significantly lowered risk for heart disease, heart attack, stroke, or increased longevity.  I can assure you that you won’t be getting any articles from your doctor since they don’t exist.   More information about cholesterol-lowering medications can be found in my book, Drugs That Don’t Work and Natural Therapies That Do. 
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Statins Flop in Sepsis and COPD - MedPage

Statins Flop in Sepsis and COPD

By Crystal Phend, Senior Staff Writer, MedPage Today Published: May 18, 2014

 

SAN DIEGO -- Statins don't prevent chronic obstructive pulmonary disease exacerbations or improve outcomes in sepsis-related respiratory failure, a series of trials showed. For patients with acute respiratory distress syndrome (ARDS) from sepsis in the ICU, rosuvastatin (Crestor) didn't cut 60-day in-hospital mortality compared with placebo (28.5% versus 24.9%, P=0.21) or boost ventilator-free days (mean 15.1 in both groups, P=0.96).

Putting patients on the lipid-lowering drug actually contributed to hepatic and renal failure, Jonathon D. Truwit, MD, of the Medical College of Wisconsin in Milwaukee, and colleagues found in the ARDS Clinical Trials Network study.

In the STATCOPE trial, simvastatin (Zocor) didn't prevent COPD exacerbations compared with placebo (1.36 versus 1.39 mean per person-year, P=0.54) or delay them (median 223 versus 231 days to first exacerbation, P=0.34), Gerard Criner, MD, of Temple University in Philadelphia, reported at the meeting.

Both National Heart, Lung, and Blood Institute-sponsored trials were reported at a late-breaking clinical trials session here at the American Thoracic Society meeting and released simultaneously online in the New England Journal of Medicine.
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Read the complete article here. See also NEJM article here.

The controversial study that started the War on Cholesterol - Watson

The controversial study that started the War on Cholesterol…

      

Alan Watson | June 14, 2012   

Revisiting the Coronary Primary Prevention Trial (CPPT) – 1973 to 1984

Using "relative risk statistics" and changing the study's design, the CPPT researchers declared success and the War on Cholesterol began in earnest

 

Launched in 1973 by the National Institutes of Health, the Coronary Primary Prevention Trial (CPPT) set out to prove that lowering blood cholesterol with a drug and a low cholesterol, low saturated fat diet would reduce the risk of coronary heart disease and extend the lives of the study participants.

(As part of the study, twelve new Lipid Research Clinics were set up by the Heart Institute at large universities throughout the country including Baylor, Stanford, Johns Hopkins and the University of Washington in Seattle.)

The researchers were looking for middle-aged men with total cholesterol levels exceeding those of 95 percent of Americans. (Only men with the highest 0.8 percent total cholesterol qualified.) The CPPT researchers screened 480,000 applicants in order to select 3,806 high risk men between the ages of 35 and 59.

This meant that many of the participants had familial hypercholesterolemia, a rare genetic defect in cholesterol metabolism present in about 1 percent of the population. The trials chance of success was therefore greatly increased by focusing on this particular group of presumably vulnerable men.
In their preliminary report, CPPT researchers announced that they would study two separate outcomes:  (1) Nonfatal heart attacks and (2) fatal heart attacks or deaths from coronary heart disease. The CPPT directors emphasized that they would be satisfied with nothing less than the strongest statistical proof of their findings; they had to be “99 percent certain that the results were not due to chance.”

The researchers also announced their goal of reducing blood cholesterol in the treatment group by 25 percent and reducing the risk of heart disease in the treatment group by at least 50 percent.
Approximately half of the 3,806 men were provided low cholesterol, low saturated fat dietary advice and were treated with cholestyramine, a cholesterol-lowering bile acid resin (Questran).

(Cholestyramine lowers cholesterol by interfering with digestion. Statins such as Lipitor, Mevacor and Zocor were not available yet.)

The control group was provided the same dietary advice and an unpleasant tasting placebo – an indigestible mixture of sand, sugar and food coloring. Both trial groups suffered with moderate to severe gastrointestinal distress. There were eight gastrointestinal cancer deaths in the treatment group (out of 21 cases) and one in the placebo group (out of 11 cases).

(There were more deaths from cancer, intestinal disease, stroke, violence and suicide in the group taking the cholesterol-lowering drug, and overall mortality was essentially the same for both groups.)

Disappointing Results

In 1984, the disappointing results were tabulated. Cholesterol levels in the treatment group had decreased by no more than 7 percent. Cholestyramine and the low cholesterol, low saturated fat diet had failed to lower cholesterol enough to prove that lowering cholesterol would reduce the risk of heart disease and extend the lives in the treatment group.

The difference in nonfatal heart attacks was not statistically significant. In the treatment group, 130 participants (6.8 percent) had a heart attack versus 158 in the placebo group (8.3 percent). After 7 years, the fraction of the treatment group that had benefited was less than 2 percent.

                                       Nonfatal heart attacks               Fatal heart attacks/coronary deaths
1,900 Control Group:         158 or 8.3 percent                               38 or 2.0 percent
1,906 Treatment Group:     130 or 6.8 percent                              30 or 1.6 percent

The difference in fatal heart attacks was not significant either. In the treatment group, 30 participants (1.6 percent) suffered a fatal heart attack compared to 38 in the placebo group (2.0 percent) Again – after 7 years of taking an unpleasant drug (and following a low fat diet), the fraction of the treatment group that benefited was less than 1 percent.

However, by applying relative risk statistics (a percentage of a percentage), the CPPT researchers improved their results. They took the number of people who presumably didn’t have a heart attack because of taking the drug (28) and looked at it as a percentage of the people who did have heart attacks (158) but didn’t take the drug:

The less than 2 percent absolute difference in nonfatal heart attacks rose to a reported 19 percent reduction in risk of a heart attack!

 

In similar statistical fashion, the researchers announced a 24 percent reduction in the risk of dying from a heart attack. The 8 men or 1.6 percent out of 1,900 who presumably did not have a fatal heart attack because they took the drug became the same 24 percent who reduced their risk of mortality compared to those in the control group who did die (38) but did not take the drug.

Additional study design changes

To prop up their victory, the CPPT researchers decided to exclude  “uncertain” nonfatal heart attacks from the treatment group while including  “uncertain” fatal heart attacks in the placebo group. Also, using the original 99 percent standard, the small favorable trend in either group could only be explained by chance (as defined by the researchers themselves at the start of the trial.)
By applying the less stringent 95 percent standard and by combining the two groups into one (nonfatal and fatal heart attacks), the CPPT researchers improved their results – declared victory – while the press responded with unbridled enthusiasm.

In 1984, the press and medical journals portrayed CPPT as the long sought proof that animal fats were the cause of heart disease. It was widely reported that for the first time:

“It had been proven that lowering cholesterol would reduce the mortality from heart disease and lower the risk of having a heart attack.”

 

Much of what we hear today about diet and heart disease can be traced back to this notorious failed study. When other scientists voiced their objections to the trial’s design changes, the CPPT directors simply denied that they had ever embraced the original more stringent standards.

In January 1984, the Journal of the American Medical Association (JAMA) dutifully reported:

“The trial’s implications…could and should be extended to other age groups and women, and to others with more modest elevations of cholesterol levels. The benefits that could be expected from cholestyramine treatment are considerable.”

 

George Mann, M.D., professor in medicine and biochemistry at Vanderbilt University, severely criticized the CPPT directors and the trial’s unsupportable results:

“The managers at the National Institutes of Health have used Madison Avenue hype to sell this failed trial in the way the media people sell an underarm deodorant…”

 

 Giving cholestyramine for over seven years to 1,906 middle age men – many with a genetic predisposition to atherosclerosis – had only saved the lives of eight but the Heart Institute was now recommending that cholesterol-lowering drug treatment be extended to patient groups that had not been part of the trial.

Even without the solid evidence they sought, the medical elite in the American Heart Association and the National Institute of Health decided to push ahead with cholesterol-lowering drugs and the still unproven low cholesterol, low saturated fat diet:

 “Now we have proved that it is worthwhile to lower blood cholesterol; no more trials are necessary. Now is the time for treatment.”

 

 The long War on Cholesterol had begun
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Read the complete article here.

Statin Therapy: Risks vs Benefit - Medscape

Statin Therapy: Risks vs Benefit: An Expert Interview With Eliot A. Brinton, MD

 

Editor's Note: Dr. Brinton is Director of the Metabolism Section of Cardiovascular Genetics, and Associate Professor at the University of Utah School of Medicine, Salt Lake City, Utah. He is board certified in internal medicine and endocrinology.
                       
Dr. Brinton's areas of clinical interest include the management of dyslipidemia and prevention of atherosclerosis and the treatment of diabetes mellitus and metabolic syndrome. He also has research interests in lipoprotein metabolism and HDL-cholesterol metabolism in vivo and in vitro, including the effects of estrogen and other agents.
                       
The author of numerous original scientific studies, Dr. Brinton has received many peer-reviewed research grants, and has held numerous leadership and advisory positions in scientific and governmental organizations, and in the pharmaceutical industry. He is a founding board member of the National Lipid Association. Dr. Brinton was interviewed for Medscape by Linda Brookes, MSc.
                       
Medscape: Why is the safety of statins such a widely discussed issue at the moment?
                       
Dr. Brinton: The safety of statins is of great interest to the public, as well as to clinicians and policy makers, in part because of the problems with the safety of cerivastatin (Baycol, Bayer), which ultimately led to its withdrawal from the market. With the recent advent of a new statin, rosuvastatin (Crestor, AstraZeneca), these concerns have resurfaced. Medication safety is always an issue, but especially so with the statins, for several reasons. First, and perhaps most importantly, they are prescribed frequently. Statins are the single most prescribed category of agents, in dollar value, in the United States today. Second, they are prescribed for long periods of time. Over the many years that a typical patient takes a statin, there are many chances for adverse events, including unforeseen changes in the patient's health status. A third and very important factor is that statins are most commonly used in middle-aged or elderly patients, who tend to be taking many other medications for other problems. This heightens safety concerns, both because the polypharmacy typical of these age groups greatly increases the overall risk of drug-drug interactions and because many of the diseases common in older patients contribute to drug safety concerns, and finally, because advanced age itself, even with excellent health, probably increases the risk of drug toxicity.

Medscape: There has been much discussion about myopathy in relation to statins. What is the difference between myopathy, myalgia, and rhabdomyolysis?
                       
Dr. Brinton: There are 4 interrelated terms for muscle problems that can occur with statins. Unfortunately, they are often confused even by healthcare professionals.

Myopathy is a general term for disease of the muscles, and it is usually characterized by weakness. In the setting of statin treatment, myopathy is used to describe any muscle problem, whether or not it is actually related to the statin use.

Myalgia refers specifically to pain in the muscles. Muscle pain is often seen with statin-based myopathy; however, painless myopathy from statin therapy is also quite common and may be rather dangerous because it is often ignored. If the healthcare provider has not instructed the patient to look for this, the patient may not report it or, if the patient reports weakness without pain, the healthcare provider may not recognize it as constituting a true myopathy.

Myositis is inflammation of the muscle confirmed by histologic findings of muscle biopsy. We rarely know whether the patient has myositis because we rarely perform muscle biopsies. These are very accurate and, in many ways, they are the gold standard for diagnosing a statin-induced myopathy; however, the pain, inconvenience, and cost of biopsies make them impractical for most clinical and research settings. Since the word myositis is probably best reserved for biopsy-proven myopathy, it is not of much use. A recent study^[1] showed that patients without an elevation of their serum creatine phosphokinase (CPK) level can nevertheless have myositis on biopsy. Thus, we need to have a fairly high index of suspicion for myopathy, realizing that it may be more common than we think, especially if we are looking only for myalgia or only for an elevated CPK.

Finally, rhabdomyolysis is the extreme type of myopathy, in which the muscle tissue is so inflamed that it breaks down in large quantities. It brings large amounts of myoglobin, the predominant muscle protein, to the circulation from which it then has to be removed by the kidney. Since the kidney is not well equipped to handle large amounts of myoglobin, it can become overwhelmed and damaged. Although the kidney usually recovers over time, rhabdomyolysis may be fatal due to acute renal failure and sequelae to other organs. Thankfully, most cases of rhabdomyolysis do not result in death, although they usually require hospitalization. Due to its seriousness, rhabdomyolysis is better prevented than treated, so we must do our best to see that myopathy does not progress to rhabdomyolysis.

Medscape: How often does myopathy occur?
                       
Dr. Brinton: In most clinical trials involving statins, less than 1% of subjects are reported to develop myopathy. In clinical practice, however, far more than 1% of patients will experience at least 1 symptom of myopathy. The much lower rate reported in clinical trials may be because eligibility criteria usually exclude patients with significant potential for drug-drug interactions or concurrent health problems, whereas healthcare providers cannot usually exclude those patients in clinical practice. Some studies have suggested that a quarter or even upwards of a third of patients who take statins will sooner or later develop a clinically significant myopathy.

Medscape: What are the risk factors for myopathy?
                       
Dr. Brinton: The main risk factors for myopathy are: female gender, advanced age (> 60 years) dehydration, underlying renal or liver disease, and concomitant medications. There is a fairly long list of medications that increase the risk of myopathy. Some of these are relatively specific for one statin vs another, but most of them appear to apply to all statins.

Medscape: How do you monitor patients for myopathy?
                       
Dr. Brinton: The first and best step is to ask about symptoms, but we have to be careful to ask about the right ones. We must ask not only about muscle pain, but about weakness and stiffness. Sometimes there can be stiffness without identifiable weakness or pain. When I start patients on a statin, I mention that they may experience any 1 or a combination of these 3 symptoms. I always make it a point to ask my patients about those 3 symptoms as I follow them in the clinic.

I measure CPK prior to starting statin treatment, and then, rather than measuring follow-up CPK levels routinely, I do so only when a patient presents with symptoms suggestive of myopathy. The reason for this is that CPK levels vary tremendously from day to day, and one may see a spurious elevation of CPK that has nothing to do with statin-based myopathy. If a patient has convincing myopathic symptoms but a normal CPK, I will defer to the patient and treat it as a true case of myopathy. If, in contrast, the CPK is clearly elevated but the muscle symptoms are somewhat equivocal, then the CPK elevation can be helpful to determine whether or not the patient has a true myopathy. Also, the degree of CPK elevation can be useful in estimating the severity of a myopathy.
Some physicians and lipidologists do not measure CPK at all, because the correlation is fairly poor between CPK levels and symptoms, but I find it useful for the above reasons. In any case, however, one should not rely on the CPK level to diagnose myopathy, because even a relatively severe case of myopathy may have normal or minimally elevated CPK.

Medscape: Can CPK be used to exclude patients from starting a statin?
                       
Dr. Brinton: A patient with a very high CPK elevation initially should not be started on a statin. This is another reason to measure CPK at baseline. The upper threshold for a clinically significant CPK is quite high, 10 times the upper limit of normal, because CPK levels are so variable. If a patient develops a CPK over 10 times the upper limit of normal on statin use, you should stop statin therapy, at least temporarily, and consider either lowering the dose or switching to a different statin. In rare cases, for example, in a patient with a history of rhabdomyolysis, one may need to abandon the statin class altogether, even perhaps without trying other available statins.

Medscape: Are there other signs that would exclude a patient from treatment with a statin?
                       
Dr. Brinton: Individuals with chronic active hepatitis are not good candidates for statin therapy. But one subset of patients with hepatitis -- those with nonalcoholic steatohepatitis (NASH), where the hepatitis is due to fatty infiltration of the liver -- may actually improve with a statin or other lipid-lowering agent.

Medscape: If CPK levels become elevated once a patient has started on a statin, do you always stop the drug?
                       
Dr. Brinton: There are several different levels of action one can take if one suspects myopathy. If the myopathy appears to be mild or equivocal, the best action may simply be to continue the statin and monitor the patient without reducing the dose.

A second option, for slightly more severe but still relatively mild cases, is to stop the statin temporarily and allow the symptoms to resolve. This also will allow a CPK elevation, if present, to normalize. Later one can rechallenge the patient at the same dose of the same drug. This approach can be useful in cases where the statin may not have been responsible for the myopathy.

In a third scenario, where the symptoms are more severe and the case is more troubling biochemically and/or clinically, one may conclude that the particular dose of that particular statin is no longer tenable. If this occurs at a high statin dose, one can consider giving a lower dose of the same statin or switching to a different statin. There are few published data about switching statins in this way, and most of our experience is anecdotal, but I can say that switching to a different statin often resolves the symptoms.

Finally, as I mentioned earlier, there are cases of myopathy so severe that one does not dare go back to any dose of any statin.

Medscape: How often are the symptoms of myopathy simply due to negative expectations on the part of the patient?
                       
Dr. Brinton: One very interesting aspect of statin therapy is that physicians are pretty much required to create an adverse expectation, or negative placebo effect, when initiating statin therapy. This is true primarily for myopathy but can occur with other safety questions as well. Most of our patients know already that statin safety is an issue, but whether they do or not, as we start a patient on a statin for the first time, we are obligated to point out its possible adverse symptoms and effects. We must describe the symptoms of myopathy and ask patients to watch out for them. We also need to inform the patient of the possibility of liver dysfunction and perhaps other potential adverse events. Such warnings give patients the expectation that they are going to have a problem, and probably make it more likely that they will have adverse symptoms.

Patients' heightened awareness of the risks of statin therapy is good in the sense that if something truly bad happens, they are more likely to notice it early and contact us promptly. But it also means that when a patient reports muscle symptoms, we do not always know if myopathy is really present. Everyone has aches and pains; and so their association with drug treatment is often open to question. So we are setting up our patients to find something that may not truly exist. The good news, however, is that we can turn the effects of our suggestions to our advantage when and if a patient reports symptoms of myopathy. We do this by explaining that the myopathy often resolves with whatever course of action we have chosen from the several options I mentioned earlier. Whether we have the patient continue, temporarily stop, reduce the dose, change drugs, or stop statins altogether, we suggest that his/her symptoms will improve soon. We thus create a positive placebo situation. When the patient hears from his trusted healthcare provider that his symptoms are likely to get better, it becomes much more likely to occur.

Obviously we will not ignore a true myopathy, but it is reasonable to try to reverse any negative anticipation on the part of the patient, which may worsen any symptoms otherwise present.

Medscape: How do the statins compare in their propensity for inducing myopathy?
                       
Dr. Brinton: First, we have to acknowledge that despite the clinical importance of statin-induced myopathy, we understand very little about its causes, which makes it hard to develop good treatments or preventive strategies.

Statin-induced myopathy is strongly dose related, so low doses of a given statin are usually much less likely to cause myopathy than high doses. For this reason, and perhaps because muscle benefits from statin-free periods of recovery, every-other-day dosing of a statin can be helpful in reducing muscle symptoms. This dosing regimen may be especially attractive for a statin with a longer half-life, or for a sustained-release formulation, where the longer dosing interval may still provide relatively continuous suppression of hepatic cholesterol synthesis, and hence still provide effective cholesterol lowering.

There are differences among the statins in terms of their propensity to cause myopathy. The statins that carry a higher than average overall risk are among the more potent: lovastatin (Mevacor, Merck; Altocor, Andrx; and generic) and simvastatin (Zocor, Merck). Myopathy risk is not, however, simply directly proportional to cholesterol-lowering efficacy, since it appears to be relatively low with atorvastatin (Lipitor, Pfizer), and may not be elevated with rosuvastatin (Crestor, AstraZeneca), which are the most effective for LDL cholesterol lowering. By contrast, the 2 statins that appear to have lower-than-average risk of myopathy are fluvastatin (Lescol, Reliant) and pravastatin (Pravachol, Bristol-Myers Squibb). These can be especially useful in patients with symptoms or risk of myopathy.

Pravastatin has been considered by many as the only safe statin with regard to myopathy. Evidence in the scientific literature, however, is actually stronger for fluvastatin as having the lowest myopathy risk. There are few comparative data between fluvastatin and pravastatin, but in the Assessment of Lescol in Renal Transplantation (ALERT)^[2] study, fluvastatin passed perhaps the most severe test of myopathy risk. That trial included more than 2000 patients who had undergone renal transplantation and were taking cyclosporine. Half of these, or about 1000 patients, also took fluvastatin.
Surprisingly, over several years of follow-up, the patients receiving both cyclosporine and fluvastatin were at no higher risk for myopathy than those on placebo. This is impressive evidence for a low myopathy risk with fluvastatin. We are often looking to use statins in such high-risk patients, and so the ALERT data are very encouraging with regard to the use of full-dose fluvastatin for atheroprevention when the risk of drug-drug interaction is high.

Medscape: What about other drug interactions?
                       
Dr. Brinton: Fluvastatin and pravastatin each appears to have fewer drug-drug interactions than other statins. Although some clinicians have felt that the safety of pravastatin was primarily due to its water solubility, the other water-soluble statin, rosuvastatin, has yet to be fully proven as safe. Moreover, fluvastatin, which is not water soluble, has excellent safety data, few potential adverse drug-drug interactions, and appears to be as safe as, or even safer in many contexts than pravastatin.
Mention has been made in the scientific literature about the risk of myopathy when the dosage of a statin is increased in patients concurrently receiving niacin. Interestingly, however, there is a Food and Drug Administration (FDA)-approved tablet (Advicor, Kos) that combines extended-release niacin (Niaspan, Kos) and generic lovastatin, and appears to carry no excess myopathy risk. Use of any combination therapy for lipid disorders should not be done in a cavalier manner, but the added risk of myopathy with niacin plus a statin appears to be at least as low as it is for fenofibrate.
Gemfibrozil is a very commonly used fibrate that is inexpensive and well proven to reduce coronary heart disease (CHD) events. However, it increases circulating statin levels and possibly CPK levels and muscle symptoms when administered with all the statins except fluvastatin. So fluvastatin is particularly useful in this situation. By contrast, the other fibrate available in the United States, fenofibrate, appears to be safe in combination with all statins. Unfortunately, it is more expensive and less widely available on managed care formularies. Also, its ability to reduce CHD events is not as well proven.

I should also mention that the bile acid sequestrants have a likely adverse interaction with statins in that if they are taken at the same time as the statin, they may reduce its absorption. This is also true of many other medications. Otherwise, however, there are no safety or toxicity issues surrounding the concurrent use of bile-acid sequestrants and statins. The intestinal cholesterol absorption inhibitor ezetimibe (Zetia, Merck/Schering Plough) has no adverse interaction with statins. Specifically, the likelihood of statin myopathy is not increased by concurrent ezetimibe use and any effects on liver dysfunction are very small. If anything, ezetimibe may reduce myopathy risk by allowing a reduction in the statin dose needed for a given patient.

Medscape: How do you follow transaminases in patients on statins?
                       
Dr. Brinton: We measure transaminases at baseline, either alanine aminotransferase or aspartate aminotransferase or both. If one reading is > 3 times the upper limit of normal, a statin should not be started except to treat NASH. Follow-up usually consists of another transaminase at the next visit, usually after 2 or 3 months. If a transaminase elevation occurs, it usually happens early in the course of the statin use, so a single measurement after starting the statin is usually sufficient. The one exception to this rule is a patient with underlying liver disease or a high risk of it, such as a binge drinker. In lower-risk patients, transaminases need be measured in follow-up primarily only if the statin dose is increased, if the patient is switched to another statin, or if another medication like niacin, a fibrate, or ezetimibe is added.

Medscape: Which patients are more likely to have elevations of transaminases while on statins?
                        
Dr. Brinton: Risk factors for transaminase elevation are advanced age, female gender, alcohol use, and prior history of hepatitis.

Medscape: What do you do in a case of transaminase level elevation?
                       
Dr. Brinton: The approach is much the same as it is for myopathy. One has several options. If the elevation is minor, one can continue the statin and check the transaminase levels again. If the elevation is more significant, one can stop the drug and then consider rechallenging the patient at the same dose. If it is more severe, one can lower the dose of the same statin since transaminase elevations are usually dose-related. Finally, one can switch to a different statin. Of course, one can always try to reduce or eliminate the adverse effects of other hepatically adverse factors, such as other hepatotoxic drugs. There does not appear to be any large difference among statins in terms of risk of transaminase elevations.

Medscape: What are the properties of statins that affect their safety profile?
                       
Dr. Brinton: The statins that are metabolized through the cytochrome P450 3A4 systems are more prone to drug-drug interactions because so many medications use the same pathway. Other cytochrome P450 pathways are much less problematic. Two statins are available in extended-release formulation: fluvastatin (Lescol XL, Reliant) and lovastatin (Altocor, Andrx). Both probably reduce the tendency for systemic complications of the drug, such as myopathy and possibly other drug-drug interactions. This is especially important when choosing a statin for a patient who may be at elevated risk of 1 or more drug-drug interactions, due to polypharmacy, frailty, or advanced age.
Both fluvastatin and rosuvastatin are metabolized primarily by the cytochrome P450 2C9 pathway, yet they appear to have different safety profiles. We do not know why this might be. We have much safety evidence for fluvastatin, but little so far for rosuvastatin. Recent concerns about an apparent excess of myopathy induced by high-dose rosuvastatin have prompted the European Union (EU) to make its label for rosuvastatin more conservative regarding the recommended starting doses. Although this only brings the EU label closer to the existing US label for this agent, the FDA has felt the need to alert healthcare practitioners to carefully follow US label instructions to reduce myopathy risk.

Medscape: Are there other safety concerns with the statins?
                       
Dr. Brinton: Just about any drug can cause headache, skin rash, fatigue, and malaise, but statins do not cause these any more than placebo. One or two earlier studies suggested that statins increase the risk of cancer, but more recent reviews show no increase in any cancer with any statin.^[3]
                       
Medscape: What is the rationale for combination therapy in treating dyslipidemia?
                       
Dr. Brinton: Combination therapy is, I believe, the wave of the future for the management of dyslipidemia. First, we are learning more and more about the benefits of LDL-cholesterol lowering. We have long known that LDL-cholesterol levels strongly predict CHD risk, but we are continually seeing new data suggesting that the lower the level of LDL-cholesterol, the better. Which is not to say that we should treat every patient to lower his or her LDL-cholesterol to, say, 40 or 50 mg/dL, but in patients at unacceptably high risk, more aggressive LDL-cholesterol lowering can be useful.
Even with more effective statins, cost, safety, and logistical concerns often make it impossible to attain the desired level of LDL cholesterol with statin monotherapy. The problem is that doubling the dose of any statin gives only about an additional 6% LDL-cholesterol-lowering effect, while that same doubling may bring a significant increase in cost, and a geometric rise in potential toxicity. An exception to these rules about uptitration is fluvastatin in the extended-release formulation (Lescol XL) at the 80-mg dose, which is the dose and formulation of this agent most often used. In this one case, you actually pay less to uptitrate a statin. Second, there is no increase in safety concerns with this dose and formulation compared to lower doses of fluvastatin or other statins. It may, in fact, be the safest statin of all. Third, as an extended-release formulation, it has more LDL-cholesterol-lowering efficacy than the immediate-release form.

Medscape: Are there benefits of statin combination therapy beyond greater LDL-cholesterol lowering?
                       
Dr. Brinton: There are other, independent benefits of combination therapy in terms of atheroprevention. For example, we know that niacin lowers lipoprotein (a) and that statins do not. So adding niacin to a statin will give that added dimension that you cannot get from a statin. In addition, niacin would be much more effective in raising HDL cholesterol than any statin. For triglyceride lowering, a fibrate is more effective than a statin. Even though niacin is comparable with statins in terms of its triglyceride lowering, adding niacin to a statin will give more triglyceride lowering than a statin alone. Ezetimibe, which is a not a very potent HDL-cholesterol-raising or triglyceride-lowering drug, will add to the HDL-cholesterol-raising effect and the triglyceride-lowering effect of statins, just as it adds to the LDL-cholesterol lowering.

Another advantage for combination treatment is in atheroprevention. Most statins reduce cardiovascular events by 20% to 35%. Studies of combination therapy have generally shown an event reduction of 70% to 90%, and even though we cannot extrapolate directly from this, clinical data strongly suggest that combination therapy is much more efficacious in reducing cardiovascular events, which is not surprising given that the lipid-lowering effect is much greater. Thus, almost without exception, adding an agent to a statin will give at least additive lipid benefit, and in some cases an additional benefit that a statin cannot give. As we learn more and more about atheroprevention and have more targets for therapy and more aggressive goals with those targets, combination therapy will become more and more appealing, not only in terms of efficacy with regard to lipids and atheroprevention, but also from a safety standpoint.

Combination therapy has not been widely used in the past, but it is increasing and I anticipate that it will continue to increase. Only 1 combination tablet is currently available in the United States, lovastatin plus extended-release niacin (Advicor, Kos), which produces more LDL-cholesterol lowering and a greater increase in HDL-cholesterol than either agent alone. There is indirect evidence that it may be effective in terms of event reduction. Another combination tablet that will be available soon in the United States, simvastatin plus ezetimibe (Vytorin, Merck/Schering Plough), is very promising.

Not every patient who needs to be treated for dyslipidemia should get 2 or more drugs, but in general we are undertreating our patients. Combination therapy is often a much better way to increase treatment benefit than uptitration of statin monotherapy.

Medscape: With safety in mind, what is your opinion about the possibility of statins being made available over the counter (OTC)?
                       
Dr. Brinton: The FDA is currently considering whether statins should be made available without a prescription in the United States. OTC status would make statins more widely accessible and more widely used, which would address one of the biggest single problems with statins in this country, which is that they tend to be underutilized.

Despite that major advantage, however, there are a number of serious objections to making them available over the counter, the first of which is the safety issue. Although statins are quite safe, the safety issues are best addressed by a physician or other licensed healthcare provider. Even though I am confident that the vast majority of patients would have no safety problems with OTC statins, I believe that many significant and even severe safety problems would arise that could not be handled by laypersons. Another disadvantage is that statin use is always based on baseline lipid levels and the availability of OTC lipid testing is somewhat limited and problematic. I am certain that cholesterol testing performed by regular laboratories in a controlled setting with proper standards and controls is far superior to the type of testing that a patient could do at home.

Other issues that would arise with OTC status are related to coordination of treatment of dyslipidemia with other atheropreventive measures. I believe that there is much benefit in having healthcare professionals involved in issues such as diet and exercise, smoking cessation, treatment of obesity, insulin resistance, diabetes, and hypertension, and in the screening for progression of disease. Other serious concerns would be that statins might be used inappropriately, such as by someone who does not need them, or there could be overtreatment or inappropriate choice of a statin. This currently happens only rarely.

And so there are many reasons why the movement to make statins available over the counter is a bad idea. I am very much in favor of patient empowerment and involvement, but I believe that because of the complexities of atheroprevention in general and lipid treatment in particular, we are ill-advised to make these very powerful medications available to the general public without proper supervision by a physician.

Conclusion

As a class, the statins are remarkably safe and their use in patients who need LDL lowering for atheroprevention has a very high benefit/risk ratio. But because they are most commonly used in older patients with complicated health histories, and because of heightened public concerns, we must always remember to address several safety issues when prescribing statins. Although there is increasing impetus toward more and more aggressive lipid-lowering therapy, we need to keep the following always in mind:

Safety, cost, and efficacy considerations often point to: Use of lower doses of a given statin and/or Use of safer statins such as fluvastatin and pravastatin; and Use of other agents (ezetimibe, niacin, fibrates, and/or sequestrants) in combination with statins for greater LDL-lowering and/or other lipid benefits When starting statins, patients must always be informed of potential safety risks, and any symptoms or signs of adverse effects must be taken seriously and handled properly. ===================================================================== Read the complete article here.

Women on Statins and diabetes risk.- Eades

Dr Michael Eades discusses the remarks of Dr. JoAnn Manson, who is describing the analysis of data from the Women's Health Initiative study showing an association between statin drugs and the development of diabetes.

Watch this video!



http://www.youtube.com/watch?v=hbSnE5ald-s&desktop_uri=/watch%3Fv%3DhbSnE5ald-s&nomobile=1

Cholesterol and Why Statin Drugs are Harmful

Cholesterol and Why Statin Drugs are Harmful

 

 

For decades, health experts have told us to watch our cholesterol levels, lower our intake of saturated fats, and consume low-fat diets.

An estimated 102 million Americans have cholesterol levels higher than 200. More than 20 million Americans are on statin drugs to lower cholesterol.

In theory, if we were following recommendations from doctors, dietitians, fitness experts, and dutifully taking our medications, we should be see a reduction in disease.

But the fact is…
We don’t.

So, it’s important to ask…

• Does eating high cholesterol foods correlate to rising cholesterol levels?

• Do high cholesterol levels necessarily mean you are at higher risk for cardiovascular disease or heart attack?

• Is the use of statin drugs safe and useful in reducing the levels of cholesterol in the body, thus lowering our disease risk?

A recent government study shows that raising levels of HDL “good” cholesterol using a drug did not diminish the chance of heart disease.
From the NY Times:

“Patients taking the medicine along with Zocor had higher levels of H.D.L. and lower levels of triglycerides, a fat in the blood. Despite these seeming improvements, the patients fared no better and may have done slightly worse than those taking Zocor alone. That is why the entire theory behind trying to increase H.D.L. levels in patients with heart disease may need rethinking.

In 2010 the British Medical Journal published a study revealing that the use of statin drugs was connected to liver, muscle, eye, and kidney problems. The results showed increased risk of moderate or serious liver dysfunction, acute renal failure, moderate or serious myopathy and cataracts.

Dietary cholesterol levels are not related to serum cholesterol levels

According to Nora Gedgaudas, of Primal Body – Primal Mind:

“No study to date has adequately shown any significant link between dietary and serum cholesterol levels…or any significant causative link between cholesterol and actual heart disease. Other than in uncommon cases of genetically based ‘familial hypercholesterolemia’ (where natural mechanisms which regulate cholesterol production fail and the body cannot stop overproduction-even here the proof of the problematic nature of cholesterol is dubious, at best), cholesterol is perhaps only potentially deleterious in and of itself in oxidized forms, occurring as a result of food processing methods (such as in “reduced fat” milks, powdered milk/eggs) and high heat cooking/frying. Inflammatory processes can also be oxidizing of cholesterol in the body. Other than this, ALL cholesterol in the body is the same. ‘HDL’ and ‘LDL’ only reflect transport mechanisms for healthy cholesterol and are meaningless measures of coronary heart disease risk (Enig, Ravnskov).

It is also important to realize that ‘HDL’ and ‘LDL’ are NOT actual cholesterol at all, but merely the protein transport mechanism for cholesterol. Again, All cholesterol is exactly the same. LDL takes cholesterol away from the liver to the extremities and other organs for various purposes and HDL merely returns the same cholesterol to the liver where it may be recycled.”

Gedgaudas believes it is more important to find out why your cholesterol levels are up. When we have stress, infections, clogged arteries, high carbohydrate diets which cause insulin resistance and diabetes, weight issues, free radical activity, and low thyroid function, these can cause the liver to produce more cholesterol in order to deal with excess inflammation. If cholesterol levels are rising, it’s always a sign of some underlying problem, but it doesn’t mean cholesterol is causing the problem.

Doctors are missing the problem

Prescriptions for high cholesterol go hand-in-hand with recommendations for low-fat diets. This type of diet is not only tasteless and unsatisfying, it is also grossly deficient in the most nutrient-dense and health supporting foods on the planet: foods with healthy fats and cholesterol.

In the last five years, doctors have started recommending that obese children take statin drugs. Of course, there is little to no thought given to the staples of the Standard American children’s diet: highly processed, increasingly lower and lower in fat ast time goes on, high-carb, sugary foods with little to no nutritional content.

It’s a wonder doctors don’t draw the obvious conclusion that these foods might possibly be the culprit to children’s health and obesity issues. But they don’t. What’s more, they fail to give good, sound nutritional advice. The result is that some children end up on drugs because apparently providing real, healthy foods that support growth and development is not what they believe will solve the problem.

Truths about cholesterol:

• Cholesterol is vital to health. Without it, we have hormonal, brain, heart, endocrine, and nervous system issues and damage. Lack of adequate cholesterol in the body leads to blood sugar imbalance, mineral deficiencies, chronic inflammation, infertility, allergies, and asthma.

• Cholesterol is beneficial to the gastrointestinal environment and lining because it improves cell-membrane integrity and can also help reduce excessive permeability of substances through the intestinal wall and into the bloodstream.

• Every cell in our bodies is made of cholesterol. Without it they would become leaky and porous, causing a flood of cholesterol taken from other parts of the body to repair damage.

• Cholesterol is the precursor to Vitamin D, which is now known to be a hormone rather than a vitamin, and is responsible for helping to digest fats, mineral metabolism, protecting bones, strengthening the immune system

• Cholesterol is a powerful anti-oxidant which protects the body from free-radical damage and aging

• The theory of cholesterol being unhealthy was originally created by food processing industries to villanize animal fats and products, which are direct competitors to vegetable oils, and also from the pharmaceutical industry to develop a market to sell cholesterol-lowering drugs. Lipitor and other Statin drugs are enormous profit-bringers for pharmaceutical companies.

Truths about statin drugs:

• Taking them only masks the problem going on in your body (for a little while) and doesn’t get to the cause of the problem, which is usually chronic inflammation due to poor dietary habits which cause nutritional deficiencies

• They deplete your body of vital nutrients, such as C0Q10, which is essential to heart health. Cardiologist Dr. Peter Langsjoen conducted a study involving 20 patients with completely normal heart function. Six months later, after being on 20 mg daily of Lipitor (a low dose), two-thirds of the patients were found to have abnormalities in the filling phase of the heart. Langsjoen’s conclusion was that this occurred due to the depletion of CoQ10. A lack of C0Q10 causes muscle pain and weakness, due to the prevention of energy being produced in the mitrochondria in the cell.

• These medications can also cause other types of muscle weakness and pain. In Denmark, researchers who studied 500,000 residents (approximately 9 percent of the population) discovered that those taking prescription medications to lower cholesterol were more likely to develop polyneuropathy, characterized as weakness and pain or tingling in the hands or feet and difficulty walking.

• They cause a marked decrease of cholesterol-production in the brain. According to Dr. Barry Sears, this leads to a loss of memory due to diminished production of new synaptic connections and loss of memory.

• They are costly in more ways than one: for your wallet and for your health. Eating healthy foods that naturally maintain normal cholesterol levels in the body costs less.

• They causes other side-effects, one of them being liver damage. Liver damage is dangerous and can lead to other health issues that are very unpleasant, expensive, and time-consuming to treat

Would the real enemies please stand up?

• Industrial fats – industrially-produced, polyunsaturated fats: canola, soybean, cottonseed, corn, peanut, safflower, and sunflower oils, shortening, butter substitutes and spreads, and other fake butter products. Some of these oils come from living things, but they are processed and chemically-altered which transforms them into trans-fats (even though the label may specifically read “no trans fats”), deodorized, and subjected to high- heat temperatures, rendering them nutritionally bankrupt and rancid.

• Sugar - which causes metabolic syndrome and blood sugar imbalance, leading to insulin resistance and diabetes, and heart attacks. In 2009, the United States was ranked 4th in sugar consumption levels in the world.

• Lack of nutrient-dense foods – modern diets are largely represented by nutritionally-deficient and heavily processed convenience foods which do not support the health of the human body. They cause build up in our arteries, liver damage, diabetes, premature aging, and cardiovascular disease.

• Stress - periods of stress deplete nutrients in the body causing inflammation, which triggers disease.

Watch this informative video by Dr. Mark Hyman about cholesterol:

How to keep inflammation and cholesterol levels normal in your body

Real, traditional fats from healthy animals and birds on pasture actually make us healthier because they are easy to digest and are some of the most nutrient-dense foods available. Looking back over the historical past, the human diet has always contained large amounts of fat and cholesterol.
Dr. Weston A. Price, author of Nutrition and Physical Degeneration, analyzed foods consumed by traditional, primitive peoples all over the world. In these populations, health was robust and disease nearly non-existent. He discovered that their diets allowed for at least four times the calcium and other minerals, and at least 10 times the fat-soluble vitamins and amino acids as the modern diet which were obtained from animal foods such as eggs, fish, shellfish, animal fats like butter, lard, and tallow, and organ meats. All these foods were high in cholesterol and fat.
If you want to maintain good health:

• Eat real, grass-fed butter

• Eat olive and coconut oil

• Eat grass-fed meats, poultry and pasture-raised eggs from reputable, local sources that raise their products sustainable

• Eat safe-sourced seafood

• Take cod liver oil

• Eat organic fruits and vegetables

• If you do eat grains, eat them sparingly and prepare them properly through soaking, sprouting, or fermenting. Eat grains with healthy fats such as milk, cream, butter, cheese, and other healthy foods containing fats such as olive oil, coconut oil, lard, tallow, bone marrow, and grass-fed meats and poultry.

• Avoid sugar – that means any refined carbohydrates – crackers, breads, rice cakes, cereals, pretzels, chips, bagels, pasta, desserts, sugary beverages (including juice and power “electrolyte” drinks).

• Avoid processed foods and drinks, and especially those with artificial sweeteners or high-fructose corn syrup

• Avoid unhealthy vegetable oils such as canola, soy, cottonseed, or safflower. These oils are too high in Omega 6s (which cause inflammation, cancer, and heart disease), are highly-processed at high temperatures making them rancid, and many of these oils are also likely to be genetically-modified as well, which has its own set of health risks.

• Lower stress levels with moderate and enjoyable exercise and relaxation strategies. Stress can severely deplete nutrients in the body, leading to heart disease.

For more information:
Importance of Dietary Fats
Cholesterol and Health – Chris Masterjohn
The Benefits of High Cholesterol – Weston A. Price Foundation
Dangers of Statin Drugs: What You Haven’t Been Told About Popular Cholesterol-Lowering Drugs – WAP Foundation
The Oiling of America – Sally Fallon and Dr. Mary G. Enig, PhD
I have high cholesterol, and I don’t care – The Healthy Skeptic
Medication Sense – Dr. Jay S. Cohen
Suggested reading:
Fat and Cholesterol are Good for You by Uffe Ravnskov, MD, PhD
The Cholesterol Delusion by Ernest N. Curtis, M.D.

This post is part of Sarah The Healthy Home Economist’s Monday Mania.

FDA Expands Advice on Statin Risks

Get this hi-resolution art on Flickr1.

 

 

 

 

On this page

• Liver Injury Called Rare
• Reports of Memory Loss
• The Risk of Diabetes
• The Potential for Muscle Damage

If you’re one of the millions of Americans who take statins to prevent heart disease, the Food and Drug Administration (FDA) has important new safety information on these cholesterol-lowering medications.

FDA is advising consumers and health care professionals that:

• Routine monitoring of liver enzymes in the blood, once considered standard procedure for statin users, is no longer needed. Such monitoring has not been found to be effective in predicting or preventing the rare occurrences of serious liver injury associated with statin use.
• Cognitive (brain-related) impairment, such as memory loss, forgetfulness and confusion, has been reported by some statin users.
• People being treated with statins may have an increased risk of raised blood sugar levels and the development of Type 2 diabetes.
• Some medications interact with lovastatin (brand names include Mevacor) and can increase the risk of muscle damage.

This new information should not scare people off statins, says Amy G. Egan, M.D., M.P.H., deputy director for safety in FDA’s Division of Metabolism and Endocrinology Products (DMEP). “The value of statins in preventing heart disease has been clearly established,” she says. “Their benefit is indisputable, but they need to be taken with care and knowledge of their side effects.”

FDA will be changing the drug labels of popular statin products to reflect these new concerns. (These labels are not the sticker attached to a prescription drug bottle, but the package insert with details about a prescription medication, including side effects.)

The statins affected include:

• Altoprev (lovastatin extended-release)
• Crestor (rosuvastatin)
• Lescol (fluvastatin)
• Lipitor (atorvastatin)
• Livalo (pitavastatin)
• Mevacor (lovastatin)
• Pravachol (pravastatin)
• Zocor (simvastatin).

Products containing statins in combination with other drugs include:

• Advicor (lovastatin/niacin extended-release)
• Simcor (simvastatin/niacin extended-release)
• Vytorin (simvastatin/ezetimibe).

Liver Injury Called Rare

FDA has found that liver injury associated with statin use is rare but can occur. Patients are advised to consult their health care professional if they have symptoms that include unusual fatigue, loss of appetite, right upper abdominal discomfort, dark urine or yellowing of the skin or whites of the eyes.

Statins work in the liver to reduce the production of cholesterol, a waxy substance that can form plaque on the walls of the arteries and keep the heart from getting the blood it needs.

Egan explains that there had been signals in early clinical trials of possible liver damage tied to statin use, so health care professionals were advised to regularly test their patients’ liver enzyme levels. However, she says, such damage is rare, and the tests are not effective at predicting or preventing who will develop this rare side effect.

So FDA is now recommending that liver enzyme tests be performed before statin treatment begins and then as needed if there are symptoms of liver damage.

 

Reports of Memory Loss

FDA has been investigating reports of cognitive impairment from statin use for several years. The agency has reviewed databases that record reports of bad reactions to drugs and statin clinical trials that included assessments of cognitive function.

The reports about memory loss, forgetfulness and confusion span all statin products and all age groups. Egan says these experiences are rare but that those affected often report feeling “fuzzy” or unfocused in their thinking.

In general, the symptoms were not serious and were reversible within a few weeks after the patient stopped using the statin. Some people affected in this way had been taking the medicine for a day; others had been taking it for years.

What should patients do if they fear that statin use could be clouding their thinking? “Talk to your health care professional,” Egan says. “Don’t stop taking the medication; the consequences to your heart could be far greater.”

 

The Risk of Diabetes

Diabetes occurs because of defects in the body’s ability to produce or use insulin—a hormone needed to convert food into energy. If the pancreas doesn't make enough insulin or if cells do not respond appropriately to insulin, blood sugar levels in the blood get too high, which can lead to serious health problems.

A small increased risk of raised blood sugar levels and the development of Type 2 diabetes have been reported with the use of statins.

“Clearly we think that the heart benefit of statins outweighs this small increased risk,” says Egan. But what this means for patients taking statins and the health care professionals prescribing them is that blood-sugar levels may need to be assessed after instituting statin therapy,” she says.

 

The Potential for Muscle Damage

Some drugs interact with statins in a way that increases the risk of muscle injury called myopathy, characterized by unexplained muscle weakness or pain. Egan explains that some new drugs are broken down (metabolized) through the same pathways in the body that statins follow. This increases both the amount of statin in the blood and the risk of muscle injury.

FDA is revising the drug label for Lovastatin to clarify the risk of myopathy. The label will reflect what drugs should not be taken at the same time, and the maximum lovastatin dose if it is not possible to avoid use of those other drugs.

Patients and health care professionals should report negative side effects from statin use to FDA’s MedWatch Adverse Event Reporting Program⁶.

This article appears on FDA's Consumer Update page⁷, which features the latest on all FDA-regulated products.

February 27, 2011

Why Women Should Stop Their Cholesterol Lowering Medication - Hyman

Why Women Should Stop Their Cholesterol Lowering Medication

by Dr Mark Hyman   January 19th, 2012

If you are a post-menopausal women with high cholesterol, your doctor will almost certainly recommend cholesterol lowering medication or statins. And it just might kill you. A new study in the Archives of Internal Medicine found that statins increase the risk of getting diabetes by 71 percent in post-menopausal women.

Since diabetes is a major cause of heart disease, this study calls into question current recommendations and guidelines from most professional medical associations and physicians. The recommendation for women to take statins to prevent heart attacks (called primary prevention) may do more harm than good.

Statins have been proven to prevent second heart attacks, but not first heart attacks.

Take it if you already have had one, but beware if your doctor recommends it for you if have never had a heart attack.

This current study adds to an increasing body of literature questioning the benefits of statins, while highlighting their potential risks.

New Study Shows 48 Percent Risk of Diabetes in Women Who Take Statins

This study examined the data from the large government sponsored study called the Women’s Health Initiative, the same study that disabused us of the idea that Premarin prevented heart attacks in postmenopausal women.

In fact, based on this randomized controlled trial, estrogen replacement therapy, once considered the gold standard of medical care for the prevention of heart disease, was relegated to the trash bin of history joining medicine’s many other fallen heroes including DES, Thalidomide, Vioxx, Avandia, and more.

In this new study researchers reviewed the effect of statin prescriptions in a group of 153,840 women without diabetes and with an average age of 63.2 years. About 7 percent of women reported taking statin medication between 1993 and 1996. Today there are many, many more women taking statin medications, thus many more are at risk from harm from statins.

During the 3-year period of the study, 10,242 new cases were reported – a whopping 71 percent increase in risk from women who didn’t take statins. This association stayed strong at a 48 percent increased risk of getting diabetes, even after taking into account age, race/ethnicity, and weight or body mass index. These increases in disease risk were consistent for all statins on the market.
This effect also occurred in those with and without heart disease. Surprisingly disease risk was worse in thin women. Minority women were also disproportionately affected. The risk of diabetes was 49 percent for white women, 57 percent for Hispanic women, and 78 percent for Asian women.
But in a typical “my mind’s made up, don’t confuse me with the facts” statement by the medical establishment, the researchers said we should not change our guidelines for statin use for the primary prevention of heart disease.

In a large meta-analysis published in the Lancet last year, scientists found that statins increased the risk of diabetes by 9 percent. If current guidelines were followed for those who should take statins, and people actually took them (thank God only 50 percent of prescriptions are ever filled by patients), there would be 3 million more diabetics in America. Oops.

Other studies have recently called into question the belief that high cholesterol levels increase your risk of heart disease as you get older. For those over 85 it turns out having high cholesterol will protect you from dying from a heart attack, and, in fact, from death from any cause.

Low Cholesterol May Kill You

A recent study showed that in healthy older persons, high cholesterol levels were associated with lower non-cardiovascular-related mortality. This is extremely concerning because millions of prescriptions are written every day to lower cholesterol in the older population, yet no association has been found between higher cholesterol and heart disease deaths for those aged 55 to 84; and for those over 85, the association seems to be inverse — higher cholesterol predicts lower risk of death from heart disease.

The pharmaceutical industry, medical associations, and academic researchers whose budgets are provided by grants from the pharmaceutical industry continue to preach the wonders of statins, but studies like these should have us look good and hard at our current practices. Are we doing more harm than good?

Cardiologists recommend putting statins in the water and giving them out at fast food restaurants and having them available over the counter. They believe in driving cholesterol as low as possible. Statin prescriptions are handed out with religious fervor, but do they work to prevent heart attacks and death if you haven’t had a heart attack already?

Bottom line: NO! If you want to learn why this is true, read on.

Statins Don’t Work to Prevent First Heart Attacks

Recently, the Cochrane Group did a review of all the major statin studies by an international group of independent scientists. The review failed to show benefit in using statins to prevent heart attacks and death. In addition, many other studies support this and point out the frequent and significant side effects that come with taking these drugs. (i) If scientists found that drinking two glasses of water in the morning prevented heart attacks, even if the evidence was weak, we would jump on board. Big up side, no down side.

But this is not the case with statins. These drugs frequently cause muscle damage, muscle cramps, muscle weakness, muscle aches, exercise intolerance (ii) (even in the absence of pain and elevated CPK – a muscle enzyme), sexual dysfunction, liver and nerve damage and other problems in 10-15 percent of patients who take them. (iii) They can also cause significant cellular, muscle, and nerve injury as well as cell death in the ABSENCE of symptoms. (iv)

There is no lack of research calling into question the benefits of statins. Unfortunately, that research doesn’t get the benefit of billions of dollars of marketing and advertising that statins do. One big trial was touted as proving statins work to prevent heart attacks, but the devil is in the details.

It was the JUPITER (v) trial that showed that lowering LDL (or bad cholesterol) without a reduction in inflammation (measured by C-reactive protein) didn’t prevent heart attacks or death. (vi) Statins happen to reduce inflammation so the study has been touted as proof of the effectiveness of these medications.

Mind you it wasn’t lowering the cholesterol that helped (which is the intended purpose of statins), but the fact that they lower inflammation. What is ignored by people who use this study to “prove” that statins work is the fact that there are so many better ways to lower inflammation than taking these drugs.

Yet other studies have shown no proven benefit for statins in healthy women (vii) with high cholesterol or in anyone over 69 years old. (viii) Some studies even show that aggressive lowering of cholesterol can cause MORE heart disease. The ENHANCE trial showed that aggressive cholesterol treatment with two medications (Zocor and Zetia) lowered cholesterol much more than one drug alone, but led to more arterial plaque and no fewer heart attacks. (ix)

Other research calls into question our focus on LDL or the bad cholesterol. We focus on it because we have good drugs to lower it, but it may not be the real problem. The real problem is low HDL that is caused by insulin resistance (diabesity).

In fact studies show that if you lower the bad (LDL) cholesterol in people with low HDL (good cholesterol) that is a marker of diabesity – the continuum of obesity, prediabetes and diabetes – there’s no benefit. (x)

Most people simply ignore the fact that 50-75 percent of people who have heart attacks have normal cholesterol. (xi) The Honolulu Heart Study showed older patients with lower cholesterol have higher risks of death than those with higher cholesterol. (xii)

Some patients with multiple risk factors, or who have had previous heart attacks do benefit, but when you look closely the results are underwhelming. It’s all in how you spin the numbers. For high-risk males (those who are overweight and have high blood pressure, diabetes, and/or a family history of heart attacks) and are younger than 69 there is some evidence of benefit, but one hundred men would need to be treated to prevent just one heart attack.

That means that 99/100 men who take the drug receive no benefit. Drug ads say the risk is reduced by 33 percent. Sounds good, but that just means the risk of getting a heart attack goes down from 3 percent to 2 percent.

Despite the extensive data showing that statins are a questionable therapy at best, they are still the number one selling drug in the US. What isn’t so well known is that 75 percent of statin prescriptions are written for people who will receive no proven benefit. The cost of these prescriptions? Over $20 billion a year.

Yet somehow the 2004 National Cholesterol Education Program guidelines expanded the previous guidelines to recommend that even more people without heart disease take statins (from 13 million to 40 million) (xiii) What are we thinking?

Why would respected scientists go against the overwhelming research that statins don’t prevent heart disease in people who haven’t already had a heart attack?

You can find the answer if you follow the money. Eight of the nine experts on the panel who developed these guidelines had financial ties to the drug industry. Thirty-four other non-industry affiliated experts sent a petition to protest the recommendations to the National Institutes of Health saying the evidence was weak.

What Should Women Do?
It is time to push the sacred cow of statins overboard.
But first let me say this. If you have had a heart attack, or have heart disease, the evidence shows they do in fact help protect against a second heart attack, so keep taking them. However, you should be aware that most prescriptions for statins are given to healthy people whose cholesterol is a little high. For these folks the risk clearly outweighs the benefit.

The editorial that accompanies the recent study on women taking cholesterol-lowering medication that I opened this article with was quite clear. Dr. Kirsten Johansen from the University of California, San Francisco said that the increased risk of diabetes in women without heart disease has “important implications for the balance of risk and benefit of statins in the setting of primary prevention in which previous meta-analyses show no benefit on all-cause mortality.”

In plain English, she said that we shouldn’t be using statin drugs for women without heart disease because:

1. The evidence shows they don’t work to prevent heart attacks if you never had one.
2. They significantly increase the risk of diabetes.

Treating risk factors like high cholesterol is misguided. We must treat causes – what we eat, how much we exercise, how we handle stress, our social connections and environmental toxins are all more powerfully linked to creating health and preventing disease than any drug on the market.
Remember what you put at the end of your fork is more powerful than anything you will ever find at the bottom of a pill bottle.

My new book The Blood Sugar Solution, which comes out at the end of February, gives exact details on what you should put at the end of your fork to prevent and reverse diabesity. It provides a comprehensive solution to the health problems facing our nation today.

Now I’d like to hear from you …

What do you think of statins?

Have you taken statins? What has your experience been?

Why do you think the medical establishment prescribes drugs that research shows don’t work?
Please leave your thoughts by adding a comment below – but remember, we can’t offer personal medical advice online, so be sure to limit your comments to those about taking back our health!

To your good health,
Mark Hyman, MD

References:

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(i) Abramson J, Wright JM. Are lipid-lowering guidelines evidence-based? Lancet. 2007 Jan 20;369(9557):168-9

(ii) Sirvent P, Mercier J, Lacampagne A. New insights into mechanisms of statin-associated myotoxicity. Curr Opin Pharmacol. 2008 Jun;8(3):333-8.

(iii) Kuncl RW. Agents and mechanisms of toxic myopathy. Curr Opin Neurol. 2009 Oct;22(5):506-15. PubMed PMID: 19680127.

(iv) Tsivgoulis G, et. al, Presymptomatic Neuromuscular Disorders Disclosed Following Statin Treatment, Arch Intern Med. 2006;166:1519-1524

(v) Mora S, Ridker PM. Justification for the Use of Statins in Primary Prevention: an Intervention Trial Evaluating Rosuvastatin (JUPITER)–can C-reactive protein be used to target statin therapy in primary prevention? Am J Cardiol. 2006 Jan 16;97(2A):33A-41A.

(vi) Ridker PM, Danielson E, Fonseca FA, Genest J, Gotto AM Jr, Kastelein JJ, Koenig W, Libby P, Lorenzatti AJ, MacFadyen JG, Nordestgaard BG, Shepherd J, Willerson JT, Glynn RJ; JUPITER Study Group. Rosuvastatin to prevent vascular events in men and women with elevated C-reactive protein. N Engl J Med. 2008 Nov 20;359(21):2195-207.

(vii)Abramson J, Wright JM. Are lipid-lowering guidelines evidence-based? Lancet. 2007 Jan 20;369(9557):168-9

(viii) IBID

(ix) Brown BG, Taylor AJ Does ENHANCE Diminish Confidence in Lowering LDL or in Ezetimibe? Engl J Med 358:1504, April 3, 2008 Editorial

(x) Barter P, Gotto AM, LaRosa JC, Maroni J, Szarek M, Grundy SM, Kastelein JJ, Bittner V, Fruchart JC; Treating to New Targets Investigators. HDL cholesterol, very low levels of LDL cholesterol, and cardiovascular events. N Engl J Med. 2007 Sep 27;357(13):1301-10.

(xi) Hansson GK Inflammation, Atherosclerosis, and Coronary Artery Disease N Engl J Med 352:1685, April 21, 2005

(xii) Schatz IJ, Masaki K, Yano K, Chen R, Rodriguez BL, Curb JD. Cholesterol and all-cause mortality in elderly people from the Honolulu Heart Program: a cohort study. Lancet. 2001 Aug 4;358(9279):351-5.

(xiii) http://www.nhlbi.nih.gov/about/ncep/index.htm

About Dr Mark Hyman

MARK HYMAN, MD is dedicated to identifying and addressing the root causes of chronic illness through a groundbreaking whole-systems medicine approach called Functional Medicine. He is a family physician, a four-time New York Times bestselling author, and an international leader in his field. Through his private practice, education efforts, writing, research, and advocacy, he empowers others to stop managing symptoms and start treating the underlying causes of illness, thereby tackling our chronic-disease epidemic. More about Dr. Hyman or on Functional Medicine. Click here to view all Press and Media Releases

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Should Women take Statin Drugs – ever? - Watson

http://dietheartnews.com/2012/11/should-women-ever-take-statin-drugs/

Should Women take Statin Drugs – ever?

Alan Watson | November 27, 2012 |

 

A true story…

In 1987, Mevacor, the first statin cholesterol-lowering drug, was introduced in record short time. Within a decade, Zocor, Pravachol, Lescol, Lipitor and Baycol were added. In August 2001, after 31 deaths from a muscle-destroying side effect, Bayer of Germany withdrew Baycol.

While clinical studies have demonstrated a small benefit among people with active, late stage heart disease, the threat of muscle-destroying side effects, liver damage and cancer are on the rise.

As reported in the Felix Letter, in the “supposedly successful” Simvastatin trial (Zocor), where the average life extension in the treatment group after 5 years was 24 days, Dr. Louis Krut is quoted as saying:

“If we were to set a very modest goal to extend their average life by only 1 year, it would require them to take simvastatin for 83 years.”

 

According to Dr. Uffe Ravnskov, statin drugs may stimulate cancer. Because the latency period between exposure and incidence is as long as 20 years, we do not know the extent to which the statin drugs will increase the rate of cancer in coming decades.

In the CARE study (Pravachol), 12 women in the treatment group developed breast cancer compared to just one in the control group (not taking the drug). And blood levels in the patients taking statin drugs were close to those that cause cancer in rodents.

Why take a chance with muscle-destroying side effects, liver failure and cancer? That’s what I asked my now deceased mother-in-law several years ago when she started taking Zocor.

Doris’s total cholesterol was 285. She was a little overweight but, at age 72, she was enjoying life and had no history of chronic illness. She drove a car, went shopping, and was even looking for a boyfriend!

As she lay in ICU one year later with elevated liver enzymes and a serious blood infection, her doctor took her off of Zocor. Once she stabilized, suspecting the drug had caused harm, we asked her doctor to recheck her cholesterol.

Yes – Doris was dying, but why not see if the drug treatment nonetheless had succeeded in lowering her cholesterol. When the doctor reluctantly complied – it took a letter from the family – Doris’s cholesterol was 130 – a drop of 155 mg/dl in less than a year.

After a few more agonizing hospitalizations, Doris was dead – Zocored within a year of starting the drug. Her doctor said she died of leukemia. Women – don’t let this happen to you. There are no circumstances – ever – when a woman should take a drug to lower cholesterol.

Women with higher cholesterol – live longer. Also, you must ask your doctor for a complete lipid evaluation. Just focusing on total cholesterol is a serious medical mistake. The ultimate price you may pay is an agonizingly slow death from cancer, liver failure or leukemia.
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