Ranolazine shortened the QTc interval from 509±41 to 451±26 ms (P=0.012) in patients with LQT3 carrying the D1790G mutation.
Cohort (n=8)
Does ranolazine reduce the QTc interval in patients with LQT3 carrying the D1790G mutation?
Ranolazine effectively blocks late sodium current and shortens the QTc interval in patients with LQT3 harboring the SCN5A-D1790G mutation.
Effect estimate: mean decrease of 56 ms
Absolute Event Rate: 451% vs 509%
p-value: p=0.012
Background— The basic defect in long-QT syndrome type III (LQT3) is an excessive inflow of sodium current during phase 3 of the action potential caused by mutations in the SCN5A gene. Most sodium channel blockers reduce the early (peak) and late components of the sodium current ( I Na and I NaL ), but ranolazine preferentially reduces I NaL . We, therefore, evaluated the effects of ranolazine in LQT3 caused by the D1790G mutation in SCN5A . Methods and Results— We performed an experimental study of ranolazine in TSA201 cells expressing the D1790G mutation. We then performed a long-term clinical evaluation of ranolazine in LQT3 patients carrying the D1790G mutation. In the experimental study, I NaL was significantly higher in D1790G than in wild-type channels expressed in the TSA201 cells. Ranolazine exerted a concentration-dependent block of I NaL of the SCN5A-D1790G channel without reducing peak I Na significantly. In the clinical study, among 8 patients with LQT3 and confirmed D1790G mutation, ranolazine had no effects on the sinus rate or QRS width but shortened the QTc from 509±41 to 451±26 ms, a mean decrease of 56±52 ms (10.6%; P =0.012). The QT-shortening effect of ranolazine remained effective throughout the entire study period of 22.8±12.8 months. Ranolazine reduced the QTc at all heart rates but less so during extreme nocturnal bradycardia. A type I Brugada ECG was never noticed. Conclusions— Ranolazine blocks I NaL in experimental models of LQT3 harboring the SCN5A-D1790G mutation and shortened the QT interval of LQT3 patients. Clinical Trial Registration— URL: https://clinicaltrials.gov ; Unique identifier: NCT01728025.
Chorin et al. (Sat,) conducted a cohort in Congenital Long-QT Syndrome Type III (n=8). Ranolazine vs. Baseline was evaluated on QTc interval (mean decrease of 56 ms, p=0.012). Ranolazine shortened the QTc interval from 509±41 to 451±26 ms (P=0.012) in patients with LQT3 carrying the D1790G mutation.