RALES study brings good news about spironolactone
RALES study brings good news about spironolactone
Published report makes results official
Over the past year, you may have been hearing good news about spironolactone, but now it’s official: A team of international investigators from the Randomized Aldactone Evalua tion Study (RALES) have found that the drug lowers morbidity and mortality in patients with advanced congestive heart failure (CHF).
Spironolactone had been on the market for decades — long before the new buzz began on what it can do for CHF patients. But its success in RALES sparked several early announcements. First, the trial was stopped early. It was originally scheduled to follow patients for three years, but after two years had passed, interim analysis showed the spironolactone group had a treatment advantage over the controls: a 30% reduction in risk of death from both progression of heart failure and sudden death from cardiac causes. It also can improve CHF symptoms and reduce hospitalization.
Reports rolled in for nearly a year
Clinicians began to hear about the RALES results and learned more about the new use for spironolactone at the American Heart Association meetings in November 1998. From that point, cardiologists like Americo Simonini, MD, of the new CHF clinic at Cedars-Sinai Medical Center in Los Angeles likened the discovery of new uses for old drugs to finding "buried treasure."
The report on RALES was published September 2 in The New England Journal of Medi cine, but the journal’s editors broke their own embargo on the story and made it available on their Web site in July. The success and surrounding excitement may take spironolactone from virtual obscurity in cardiovascular circles to the established ranks of standard CHF medicines like ACE inhibitors, beta- blockers, diuretics, and digitalis.
It may take more than an initial look at a drug before its usefulness is established, says lead RALES researcher Bertram Pitt, MD, from the University of Michigan Medical Center in Ann Arbor. Beta-blockers also have been around for decades, he says, and were first believed not to be useful for treating CHF. Doctors once were too concerned with the initial worsening of CHF symptoms to think that the drugs could help these patients. Studies of those drugs proved otherwise: They can be helpful in treating the disease and increasing survivability.
In the same way, Pitt says, doctors may have been concerned to put patients on both an ACE inhibitor and a drug like spironolactone to add to aldosterone blockade because of the concern for hyperkalemia. It took initial safety studies to show spironolactone used with the other CHF drugs did not contribute to significantly high potassium levels, defined as 6.0 mmol/L or higher. (Spironolac tone was given in a daily dose of 12.5 mg to 25 mg along with the CHF patient’s other medications.)
Pitt became interested in studying spironolactone during the time he lectured on diuretics. Doctors knew aldosterone contributed to fibrosis and the cardiovascular decline CHF patients experience, and they knew that ACE inhibitors did not suppress aldosterone completely.
Studies continued to show that spironolactone not only acted like a diuretic, but it also had effects on the endothelium and other vascular benefits. He talked with manufacturer Searle of Skokie, IL, and began to test the drug’s safety in patients. "All these things gave us increasing enthusiasm," Pitt says.
The double-blind study recruited more than 1,600 patients with severe CHF. Patients could be in the study if they:
• had a left-ventricular ejection fraction under 35% within six months of enrollment;
• were in New York Heart Association class IV disease within six months before the enrollment and were in class III or IV during enrollment;
• were diagnosed with heart failure at least six weeks before enrollment;
• were not receiving potassium-sparing diuretics;
• did not have operable disease of the heart valves (other than mitral or tricuspid regurgitation with clinical symptoms due to left-ventricular systolic heart failure);
• did not have congenital heart disease, unstable angina, primary hepatic failure, active cancer, or life-threatening disease other than CHF;
• were not transplant candidates or recipients;
• did not have a serum creatinine concentration more than 2.5 mg/dL (221 µmol/L);
• did not have a serum potassium concentration of more than 5.0 mmol/L.
Patients also were receiving ACE inhibitors and a loop diuretic, and some patients also were being treated with digoxin. In the control group, 841 patients received a placebo and were compared with a group of 822 patients that received 25 mg of spironolactone each day.
Doctors compared the death rate from all causes in these groups. By the mean follow-up of two years into the study, 35% of the patients in the spironolactone group had died, compared with 46% of the participants in the placebo group. The drug group also had 35% lower rates of rehospitalization for worsening CHF symptoms — and the CHF symptoms among the patients in the spironolactone group improved in NYHA class.
Details on dosage
Patients in the spironolactone group took 25 mg of the drug (brand name Aldactone) once a day for two months. The dose could be doubled after that time if it appeared the CHF was getting worse as long as there was no sign of hyperkalemia. If high potassium developed, the treating physician was encouraged to adjust the other medications first, but if that didn’t help, the dose of spironolactone could be reduced to 25 mg once every other day.
Cardiologist Karl T. Weber, MD, from the University of Missouri Health Sciences Center in Columbia, says the drug has many benefits: It’s cheap; it’s effective, and if used appropriately, it’s safe. "It’s an old friend," says Weber, author of the companion editorial on aldosterone and spironolactone in heart failure.
But the drug must be used properly. The RALES investigators permitted patients to participate in the study only if the baseline renal serum creatinine was less than 2.5 mg/dL. Weber says he prefers patients to have a level lower than 2.0. The risk of hyperkalemia can be minimal, he notes, "but it has to be monitored." Patients often are on a diuretic like Lasix, so doctors may be in the mode of thinking about replacing the potassium often lost through diuresis. But spironolactone keeps the body from losing potassium, so supplementation may not be needed any longer or a patient may need less of it. The physician also may be able to reduce the loop diuretic, depending on how the patient is responding to therapy.
Pitt also warns that potassium levels can get too high. Overall, his group reported the incidence of serious hyperkalemia was minimal in both the drug and placebo groups.
Other observers say it’s important to remember that the conditions of the RALES participants won’t always match those of the patients doctors treat every day. If the participants had a serum creatinine concentration more than 2.5 mg/dL, they were eliminated from the study, says David S. Roffman, PharmD, BCPS, associate professor at the University Maryland School of Pharmacy and cardiac care unit therapeutic consultant with the university’s medical system. Most patients with advanced CHF don’t have normal renal function.
Roffman says it’s also important to recognize that nearly a third of the RALES patients who received spironolactone, on top of using ACE inhibitors, still needed potassium supplementation. "You would think that this cohort would have too much potassium," he says, "But 29% still needed extra." Since patients are probably on substantial doses of loop diuretics, that’s the most likely reason for why they still are losing potassium.
Subscribe Now for Access
You have reached your article limit for the month. We hope you found our articles both enjoyable and insightful. For information on new subscriptions, product trials, alternative billing arrangements or group and site discounts please call 800-688-2421. We look forward to having you as a long-term member of the Relias Media community.