Poisoning Due to Class IA Antiarrhythmic Drugs Quinidine, Procainamide and Disopyramide

Kim, Susan Y.; Benowitz, Neal L.

doi:10.2165/00002018-199005060-00002

Cited by 81 publications

(35 citation statements)

References 165 publications

(100 reference statements)

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“…It is well-known that class Ia antiarrythmic drugs such as quinidine, disopyramide, and cibenzoline induce a hypoglycemia (1,2,27,28). Several studies have indicated that these drugs increase insulin secretion from pancreatic β-cells by inhibiting K ATP channels in a manner similar to sulfonylurea antidiabetic drugs (3,4,25).…”

Section: Discussionmentioning

confidence: 99%

“…It has been reported that antiarrhythmic drugs with Vaughan Williams class Ia action such as quinidine, cibenzoline and disopyramide induce a hypoglycemia (1,2). Several studies have indicated that the drug-induced hypoglycemia can be ascribed to insulin secretion from pancreatic β-cells resulting from ATP-sensitive K + (K ATP )-channel inhibition (3,4).…”

Section: Introductionmentioning

confidence: 99%

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Inhibition of ATP-Sensitive K+ Channels and L-Type Ca2+ Channels by Amiodarone Elicits Contradictory Effect on Insulin Secretion in MIN6 Cells

et al. 2011

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Abstract. Some class I antiarrhythmic drugs induce a sporadic hypoglycemia by producing insulin secretion via inhibition of ATP-sensitive K + (K ATP ) channels of pancreatic β-cells. It remains undetermined whether amiodarone produces insulin secretion by inhibiting K ATP channels. In this study, effects of amiodarone on K ATP channels, L-type Ca 2+ channel, membrane potential, and insulin secretion were examined and compared with those of quinidine in a β-cell line (MIN6). Amiodarone as well as quinidine inhibited the openings of the K ATP channel in a concentration-dependent manner without affecting its unitary amplitude in inside-out membrane patches of single MIN6 cells, and the IC 50 values were 0.24 and 4.9 μM, respectively. The L-type Ca 2+ current was also inhibited by amiodarone as well as quinidine in a concentration-dependent manner. Although glibenclamide (0.1 μM) or quinidine (10 μM) significantly potentiated the insulin secretion from MIN6 cells, amiodarone (1 -30 μM) failed to increase insulin secretion. Amiodarone (30 μM) and nifedipine (10 μM) significantly inhibited the increase in insulin secretion produced by 0.1 μM glibenclamide. Amiodarone (30 μM) produced a gradual decrease of the membrane potential, but did not produce repetitive electrical activity in MIN6 cells. Glibenclamide (1 μM) produced a slow depolarization, followed by spiking activity which was inhibited by 30 μM amiodarone. Thus, amiodarone is unlikely to produce hypoglycemia in spite of potent inhibitory action on K ATP channels in insulin-secreting cells, possibly due to its Ca 2+ channel-blocking action.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Inhibition of ATP-Sensitive K+ Channels and L-Type Ca2+ Channels by Amiodarone Elicits Contradictory Effect on Insulin Secretion in MIN6 Cells

et al. 2011

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“…The use of procainamide in the management of adult ventricular arrhythmias and atrial fibrillation is well established, as well as the potential for adverse effects with class IA agents. 11 However, safe dosing regimens have been reported in pediatric patients. Using an intravenous dosing regimen similar to that used for older children and adults to achieve therapeutic levels, Moffett et al 12 demonstrated that neonatal recipients did not have hypotension, heart block, GI disturbances, rash, or lupus-like reactions.…”

Section: Discussionmentioning

confidence: 99%

Amiodarone Versus Procainamide for the Acute Treatment of Recurrent Supraventricular Tachycardia in Pediatric Patients

Chang

Silka

Moromisato

et al. 2010

Circ: Arrhythmia and Electrophysiology

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Background-Intravenous amiodarone and procainamide are both used as therapies for refractory supraventricular tachycardia (SVT). However, no studies have compared the efficacy and safety of these agents in pediatric patients. Methods and Results-All patients treated with intravenous amiodarone or procainamide during 25 consecutive months for the following mechanisms of SVT were included: orthodromic reciprocating tachycardia, intra-atrial reentrant tachycardia, and ectopic atrial tachycardia; junctional ectopic tachycardia was excluded. Treatment response was categorized as full success, partial success, or failure. Partial success was defined as clinical improvement and/or arrhythmia control but not meeting full success criteria. Adverse events were classified as major (requiring resuscitation) or minor (management changes). There were 40 episodes of SVT in 37 patients (median age, 34 days; 24 with congenital heart disease). Amiodarone was the initial therapy in 26 cases and procainamide in 14 cases. If partial and full success are combined, procainamide was successful in 71% of cases compared with 34% for amiodarone (Pϭ0.046). If partial success is considered a treatment failure, procainamide was successful in 50% compared with 15% for amiodarone (Pϭ0.029). Ten patients received the second medication after the first failed. Success was achieved in 5 of 8 amiodarone-to-procainamide crossovers compared with 1 of 2 procainamide-to-amiodarone crossovers. One major and 10 minor adverse events occurred in amiodarone patients versus 6 minor adverse events in procainamide patients (PϭNS). Conclusions-In this cohort, procainamide achieved greater success compared with amiodarone in the management of recurrent SVT without statistically significant differences in adverse event frequency. (Circ Arrhythm Electrophysiol.

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“…There are no effective malaria vaccines, and the efficacies of antimalarial drugs continue to decrease as a consequence of the emergence of drugresistant parasites. In addition, the first-line antimalarial drugs, such as quinine, quinidine, and mefloquine (18), are still in use and are reported to have from mild to severe adverse effects (7,10,11,20). Fortunately, many academic centers and organizations, including the U.S. Army, are seeking new antimalarial products (26).…”

mentioning

confidence: 99%

New Potential Antimalarial Agents: Therapeutic-Index Evaluation of Pyrroloquinazolinediamine and Its Prodrugs in a Rat Model of Severe Malaria

Xie

Lin

et al. 2006

Antimicrob Agents Chemother

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Tetra-acetamide pyrroloquinazolinediamine (PQD-A4) and bis-ethylcarbamyl pyrroloquinazolinediamine (PQD-BE) are new derivatives of pyrroloquinazolinediamine (PQD) and are being investigated as potential chemotherapeutic agents for the treatment of malaria. Comparative studies to assess the therapeutic indices of PQD-A4, PQD-BE, and PQD were conducted in Plasmodium berghei-infected rats following daily intragastric dosing for three consecutive days. Artesunate (AS), a standard drug for treatment of severe malaria, was used as a comparator. The minimum doses required to clear malaria parasitemia were 156 mol/kg of body weight for AS and 2.4 mol/kg for PQD, PQD-4A, and PQD-BE. The maximum tolerated dose (MTD) of AS was 625 mol/kg, and its therapeutic index was calculated to be 4. The MTDs of PQD-A4, PQD-BE, and PQD were found to be 190, 77, and 24 mol/kg, respectively, yielding therapeutic indices of 80, 32, and 10, respectively. Although PQD-A4 and PQD-BE are only half as potent as PQD based on their curative effects, the two new derivatives, PQD-4A and PQD-BE, are 8.0-fold and 3.2-fold safer, respectively, than their parent compound when they are dosed for three consecutive days. Oral PQD-A4 and PQD-BE are 44 to 70 times more potent on an mg basis than intravenous AS. As assessed from the therapeutic index over 3 days, PQD-A4, PQD-BE, and PQD administered orally are 20.0, 8.0, and 2.5 times safer than AS given intravenously. The results indicate that PQD-4A is a promising candidate for antimalarial treatment.

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Poisoning Due to Class IA Antiarrhythmic Drugs Quinidine, Procainamide and Disopyramide

Cited by 81 publications

References 165 publications

Inhibition of ATP-Sensitive K+ Channels and L-Type Ca2+ Channels by Amiodarone Elicits Contradictory Effect on Insulin Secretion in MIN6 Cells

Inhibition of ATP-Sensitive K+ Channels and L-Type Ca2+ Channels by Amiodarone Elicits Contradictory Effect on Insulin Secretion in MIN6 Cells

Amiodarone Versus Procainamide for the Acute Treatment of Recurrent Supraventricular Tachycardia in Pediatric Patients

New Potential Antimalarial Agents: Therapeutic-Index Evaluation of Pyrroloquinazolinediamine and Its Prodrugs in a Rat Model of Severe Malaria

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