The anti-anginal and anti-ischemic properties of ranolazine are not dependent on reductions in heart rate or blood pressure. Ranolazine was approved on January 27, 2006, for the treatment of chronic angina. Because ranolazine prolongs the QT interval, it should be reserved for patients who have not achieved an adequate response with other anti-anginal drugs.
RanolazineCV TherapeuticsAnti-anginal agent approved for patients not responsive to other therapies
The anti-anginal and anti-ischemic properties of ranolazine are not dependent on reductions in heart rate or blood pressure. Ranolazine was approved on January 27, 2006, for the treatment of chronic angina. Because ranolazine prolongs the QT interval, it should be reserved for patients who have not achieved an adequate response with other anti-anginal drugs.
Efficacy. The efficacy of ranolazine in the treatment of angina was evaluated in patients with chronic angina who remained symptomatic despite treatment with the maximum dose of an anti-anginal agent. In the ERICA (Efficacy of Ranolazine in Chronic Angina) trial, 565 patients were randomized to receive an initial dose of ranolazine 500 mg bid or placebo for 1 week, followed by 6 weeks of treatment with ranolazine 1,000 mg bid or placebo in addition to concomitant treatment with amlodipine 10 mg qd. The mean number of angina attacks per week was 3.3 in the ranolazine group compared with 4.3 in the placebo group (P=.028). Likewise, the mean number of nitroglycerin doses per week was 2.7 in the ranolazine group compared with 3.6 in the placebo group (P=.014). In the CARISA (Combination Assessment of Ranolazine In Stable Angina) study, 823 chronic angina patients were randomized to receive 12 weeks of treatment with twice-daily ranolazine 750 mg, 1,000 mg, or placebo while continuing daily doses of atenolol 50 mg, amlodipine 5 mg, or diltiazem 180 mg. Statistically significant (P<.05) increases in modified Bruce treadmill exercise duration and time to angina were observed for each ranolazine dose versus placebo, at both trough (12 h after dosing) and peak (4 h after dosing) plasma levels. For the treadmill test, the mean difference from placebo in exercise duration at peak plasma levels was 34 seconds for the 750-mg ranolazine dose compared with 26 seconds for the 1,000-mg dose (P≤.05). Likewise, the mean difference from placebo in time to angina at peak plasma concentration was 38 seconds for both doses (P≤.005). The mean number of angina attacks per week in this study was 2.5 and 2.1 for the 750- and 1,000-mg ranolazine groups, respectively, compared with 3.3 for placebo (P=.006 and <.001, respectively). The mean number of nitroglycerin doses per week was 2.1 and 1.8 for the 750- and 1,000-mg ranolazine groups, respectively, compared with 3.1 for placebo (P=.016 and <.001, respectively).
Dosing. Ranolazine should be initiated at 500 mg bid and increased to 1,000 mg bid as needed, based on clinical symptoms. The maximum recommended daily dose of ranolazine is 1,000 mg bid. Baseline and follow-up ECGs should be obtained to evaluate effects on the QT interval. The concomitant administration of ranolazine and other commonly administered cardiovascular medications (amlodipine, beta blockers, nitrates, antihypertensive agents) is well tolerated. Ranolazine may be taken with or without meals.
David Calabrese of OptumRx Talks Top Three Drugs in Pipeline, Industry Trends in Q2
July 1st 2020In this week's episode of Tuning Into The C-Suite podcast, MHE's Briana Contreras chatted with David Calabrese, R.Ph, MHP, who is senior vice president and chief pharmacy officer of pharmacy care services company, OptumRx. David is also a member of Managed Healthcare Executives’ Editorial Advisory Board. During the discussion, he shared the OptumRx Quarter 2 Drug Pipeline Insights Report of 2020. Some of the information shared includes the three notable drugs currently being reviewed or those that have been recently approved by the FDA. Also discussed were any interesting industry trends to watch for.
Listen
ICER Finds Insurers Struggled to Provide Fair Access for Obesity Drugs
December 19th 2024The Institute for Clinical and Economic Review assessed the formularies of 11 payers, covering 57 million people, to determine access for drugs that the organization had reviewed in 2022 for cost-effectiveness.
Read More