Negative inotropic agents are often administered to decrease the left ventricular (LV) pressure gradient in patients with obstructive hypertrophic cardiomyopathy (HC). Little information is available regarding comparisons of the effects on LV pressure gradient among negative inotropic agents. The present study compared the decrease in the LV pressure gradient at rest in patients with obstructive HC after treatment with pilsicainide versus treatment with disopyramide or cibenzoline. The LV pressure gradient and LV function were assessed before and after the intravenous administration of each drug. In 12 patients (group A, mean pressure gradient 90 ± 24 mm Hg), the effects of disopyramide, propranolol, and verapamil were compared. In another 12 patients (group B, mean pressure gradient 98 ± 34 mm Hg), a comparison was performed among disopyramide, cibenzoline, and pilsicainide. In group A, the percentage of reduction in the LV pressure gradient was 7.7 ± 9.9% with verapamil, 19.0 ± 20.2% with propranolol, and 58.6 ± 15.0% with disopyramide, suggesting that disopyramide was more effective than either verapamil or propranolol. In group B, the percentage of reduction in the LV pressure gradient was 55.3 ± 26.6% with disopyramide, 55.3 ± 20.6% with cibenzoline, and 54.7 ± 15.4% with pilsicainide, suggesting an equivalent effect on the LV pressure gradient for these 3 agents. In conclusion, these results indicate that the acute efficacy for the reduction of the LV pressure gradient at rest by pilsicainide (a pure sodium channel blocker) was equivalent to that of disopyramide or cibenzoline (combined sodium and calcium channel blockers). Accordingly, sodium channel blockade might be more important for reducing the LV pressure gradient at rest in patients with obstructive HC than calcium channel blockade or β blockade.
The present study compared the acute reduction of the left ventricular (LV) pressure gradient at rest produced by disopyramide versus that produced by propranolol or verapamil and that produced by pilsicainide (a pure sodium channel blocker) versus that produced by cibenzoline or disopyramide in patients with obstructive hypertrophic cardiomyopathy (HC).
Methods
We prospectively studied 24 patients with symptomatic obstructive HC who had a LV pressure gradient of ≥30 mm Hg at rest without provocation. All 24 participants had severe symptoms (angina in 12 [50%], dyspnea in 20 [87%], and presyncope in 3 [13%]) and were undergoing either a diagnostic pharmacologic or preoperative evaluation. The diagnosis of HC was determined by the identification using 2-dimensional echocardiography of a hypertrophic, nondilated left ventricle in the absence of another cardiac or systemic disease capable of causing a similar extent of hypertrophy. All patients had a septal thickness >15 mm without any apparent cause of hypertrophy, and they had obstruction of the left ventricular outflow tract due to systolic anterior motion of the mitral valve with a peak instantaneous gradient of ≥30 mm Hg with at rest conditions on the continuous-wave Doppler echocardiogram. We excluded patients who had systemic hypertension, significant valvular heart disease, other systemic conditions that might cause cardiac hypertrophy, or midventricular obstruction (≥30 mm Hg) at rest. The present study was performed according to the principles of the Declaration of Helsinki, and all patients gave informed consent after receiving a written explanation.
All 24 participants underwent baseline assessment of the LV function and LV pressure gradient during hospitalization and were then divided into 2 groups of 12 patients each. The first group (group A, mean LV pressure gradient at rest 90 ± 24 mm Hg) was used to evaluate the effects of propranolol, verapamil, and disopyramide. The second group (group B, mean LV pressure gradient at rest 98 ± 34 mm Hg) was used to evaluate the effects of pilsicainide, disopyramide, and cibenzoline.
Each drug was administered intravenously for a 5-minute period at the following dosages in a random order: propranolol, 0.20 mg/kg ; verapamil 0.10 mg/kg ; disopyramide 1.0 mg/kg ; cibenzoline 1.4 mg/kg ; and pilsicainide 1.0 mg/kg. Echocardiography was performed at the beginning of the study and at 5 minutes after the end of the intravenous administration of each drug. The interval between the intravenous administration of each drug during hospitalization was >24 hours (mean 30). Acute efficacy was defined as a significant reduction in the LV pressure gradient at rest by >50% after intravenous administration. All cardiac medications were withheld for 48 hours before the study.
Echocardiography was conducted using a Hewlett-Packard Sonos 5500 and a 3.5-MHz transducer. Standard techniques were used to obtain M-mode, 2-dimensional, and Doppler measurements. The severity and distribution of LV hypertrophy was assessed in short-axis views by dividing the LV wall into 4 segments (anterior septum, posterior septum, anterolateral wall, and posterior wall) at the level of the mitral valve and at the papillary muscles. The E-wave velocity/A-wave velocity (E/A) ratio and the deceleration time (DcT) were calculated from the transmitral Doppler recordings. Simultaneous recording of the phonocardiogram and Doppler echocardiogram was done to assess the isovolumic relaxation time (IRT). LV outflow tract obstruction was quantified by continuous-wave Doppler echocardiography under at rest conditions. In the present study, all echocardiographic data were obtained by an experienced sonographer and interpreted by 2 experienced echocardiographers who were unaware of the study drugs and that the patients were participating in the present study.
Analyses were performed using Statistical Analysis Systems, version 9.1, software (SAS Institute, Cary, North Carolina). The data are presented as the mean ± SD. A paired t test was used to compare the 2 groups. The Tukey-Kramer multiple comparison procedure was used for the continuous variables showing a normal distribution. Pearson’s correlation coefficient and a linear regression model was applied to evaluate the relation between 2 continuous variables. p Values <0.05 (2-tailed) were considered to indicate statistical significance. All analyses were performed by an independent biostatistics and data center (STATZ Institute, Tokyo, Japan).
Results
The changes in the LV pressure gradient at the end of the administration of each drug are listed in Tables 1 and 2 , and Figure 1 . In group A, the percentage of the reduction in the LV pressure gradient was −19.0 ± 20.2% with propranolol (p = 0.005), −7.7 ± 9.9% with verapamil (p = 0.030), and −58.6 ± 15.0% with disopyramide (p <0.001), suggesting that disopyramide was more effective than verapamil or propranolol (p <0.001 and p <0.001, respectively). In group B, the percentage of the reduction in the LV pressure gradient was −55.3 ± 26.6% with disopyramide (p <0.001), −55.3 ± 20.6% with cibenzoline (p <0.001), and −54.7 ± 15.4% with pilsicainide (p <0.001), suggesting that the acute effect of pilsicainide (a pure sodium-channel blocker) on the LV pressure gradient at rest was almost equal to that of disopyramide and cibenzoline ( Figure 1 ). The percentage of the reduction in the LV pressure gradient in each patient is shown in Figure 2 . Disopyramide reduced the LV pressure gradient at rest more than did either propranolol or verapamil in all 12 patients ( Figure 2 ). Regarding the acute effect of class I antiarrhythmic drugs on the LV pressure gradient at rest, however, 4 patients (33%) had a decrease in the LV pressure gradient by >50% or an LV pressure gradient of <30 mm Hg with 2 drugs, and 5 patients (42%) did so with all 3 drugs, suggesting that the acute efficacy of each drug varied among patients with HC ( Figure 2 ). Regarding the acute effect of these agents on the systolic blood pressure and heart rate, all 3 of the class I antiarrhythmic drugs (disopyramide, cibenzoline, and pilsicainide) significantly increased the systolic blood pressure (from 126 ± 11 to 138 ± 10, 128 ± 10 to 140 ± 11, and 125 ± 10 to 139 ± 12 mm Hg, respectively; p <0.001), although the heart rate was not changed significantly (from 74 ± 8 to 71 ± 11, 73 ± 6 to 70 ± 10, and 72 ± 8 to 68 ± 9 beats/min, respectively). After the intravenous administration of propranolol, the systolic blood pressure and heart rate did not change significantly (from 129 ± 11 to 131 ± 12 mm Hg and from 75 ± 6 to 73 ± 9 beats/min, respectively). The acute intravenous administration of verapamil caused a significant decrease in the systolic blood pressure from 128 ± 12 to 119 ± 9 mm Hg (p<0.001), although the heart rate was not changed significantly (from 74 ± 7 to 72 ± 9 beats/min).
| Pt. No. | Age (yrs) | VST (mm) | PWT (mm) | LVDd (mm) | FS (%) | LVPG (mm Hg) | ||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Disopyramide | Propranolol | Verapamil | ||||||||||||
| Before | After | Change | Before | After | Change | Before | After | Change | ||||||
| 1 | 25 | 32 | 13 | 36 | 47 | 64 | 30 | 34 | 70 | 70 | 0 | 70 | 68 | 2 |
| 2 | 26 | 18 | 14 | 28 | 39 | 75 | 10 | 65 | 70 | 60 | 10 | 60 | 50 | 10 |
| 3 | 38 | 18 | 14 | 50 | 41 | 81 | 49 | 32 | 100 | 100 | 0 | 84 | 84 | 0 |
| 4 | 45 | 16 | 14 | 40 | 40 | 125 | 35 | 90 | 100 | 92 | 8 | 100 | 100 | 0 |
| 5 | 48 | 28 | 15 | 47 | 43 | 108 | 57 | 51 | 100 | 100 | 0 | 100 | 100 | 0 |
| 6 | 53 | 26 | 12 | 36 | 56 | 100 | 23 | 27 | 130 | 128 | 2 | 100 | 100 | 0 |
| 7 | 56 | 16 | 12 | 40 | 40 | 40 | 15 | 25 | 74 | 40 | 34 | 40 | 40 | 0 |
| 8 | 58 | 16 | 16 | 40 | 50 | 108 | 60 | 48 | 121 | 85 | 46 | 100 | 100 | 0 |
| 9 | 58 | 30 | 20 | 32 | 30 | 134 | 81 | 53 | 130 | 108 | 22 | 125 | 100 | 25 |
| 10 | 58 | 24 | 16 | 48 | 38 | 96 | 42 | 54 | 80 | 63 | 17 | 75 | 53 | 22 |
| 11 | 61 | 16 | 16 | 46 | 32 | 71 | 25 | 46 | 81 | 40 | 41 | 81 | 70 | 11 |
| 12 | 70 | 15 | 13 | 43 | 49 | 70 | 28 | 42 | 71 | 36 | 35 | 108 | 100 | 8 |
| Median | 55 (42–58) | 18 (16–27) | 14 (13–16) | 40 (36–47) | 41 (39–48) | 89 (71–108) | 33 (24–53) ⁎ | 47 (33–53) | 91 (73–111) | 78 (50–100) † | 14 (0–35) | 92 (73–100) | 92 (61–100) † | 1 (0–10) |
| Pt. No. | Age (yrs) | VST (mm) | PWT (mm) | LVDd (mm) | FS (%) | LVPG (mm Hg) | ||||||||
|---|---|---|---|---|---|---|---|---|---|---|---|---|---|---|
| Disopyramide | Cibenzoline | Pilsicainide | ||||||||||||
| Before | After | Change | Before | After | Change | Before | After | Change | ||||||
| 13 | 21 | 26 | 14 | 44 | 48 | 71 | 31 | 40 | 100 | 16 | 84 | 100 | 16 | 84 |
| 14 | 25 | 32 | 12 | 36 | 47 | 64 | 16 | 48 | 70 | 16 | 54 | 81 | 23 | 58 |
| 15 | 38 | 33 | 12 | 42 | 48 | 176 | 108 | 68 | 169 | 74 | 85 | 181 | 67 | 114 |
| 16 | 45 | 20 | 18 | 40 | 68 | 40 | 6 | 34 | 40 | 20 | 20 | 40 | 20 | 20 |
| 17 | 48 | 16 | 14 | 40 | 48 | 125 | 25 | 100 | 100 | 81 | 19 | 71 | 16 | 55 |
| 18 | 54 | 22 | 14 | 36 | 39 | 40 | 35 | 5 | 40 | 30 | 10 | 44 | 22 | 22 |
| 19 | 58 | 22 | 16 | 50 | 43 | 96 | 46 | 50 | 67 | 25 | 42 | 96 | 85 | 11 |
| 20 | 65 | 22 | 14 | 42 | 48 | 101 | 101 | 0 | 144 | 72 | 72 | 135 | 81 | 54 |
| 21 | 68 | 23 | 13 | 41 | 36 | 125 | 46 | 79 | 112 | 16 | 96 | 94 | 35 | 59 |
| 22 | 70 | 26 | 17 | 44 | 32 | 90 | 17 | 73 | 100 | 50 | 50 | 100 | 50 | 50 |
| 23 | 70 | 17 | 14 | 44 | 34 | 116 | 52 | 64 | 125 | 64 | 61 | 121 | 81 | 40 |
| 24 | 73 | 16 | 12 | 32 | 44 | 100 | 36 | 64 | 144 | 64 | 80 | 117 | 60 | 57 |
| Median | 56 (42–69) | 21 (18–26) | 14 (13–15) | 42 (38–44) | 46 (38–48) | 98 (68–120) | 36 (21–49) ⁎ | 57 (37–71) | 100 (69–135) | 40 (18–68) ⁎ | 58 (31–82) | 98 (76–119) | 42 (21–74) ⁎ | 55 (31–59) |
