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(Top) 1 Heart potential 2 The ion currents 3 Pharmacology 4 Pharmacokinetics 5 References

Azimilide

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This article may be too technical for most readers to understand. Please help improve ittomake it understandable to non-experts, without removing the technical details. (April 2021) (Learn how and when to remove this message)

Azimilide
Clinical data

ATC code	none
Identifiers
IUPAC name 1-({(E)-[5-(4-chlorophenyl)furan-2-yl]methylidene}amino)-3-[4-(4-methylpiperazin-1-yl)butyl]imidazolidine-2,4-dione
CAS Number	149908-53-2^N
PubChem CID	9571004
IUPHAR/BPS	2588
ChemSpider	7845470^Y
UNII	74QU6P2934
ChEMBL	ChEMBL123558^Y
CompTox Dashboard (EPA)	DTXSID10869988
Chemical and physical data
Formula	C₂₃H₂₈ClN₅O₃
Molar mass	457.96 g·mol⁻¹
3D model (JSmol)	Interactive image
SMILES Clc4ccc(c3oc(\C=N\N1C(=O)N(C(=O)C1)CCCCN2CCN(C)CC2)cc3)cc4
InChI InChI=1S/C23H28ClN5O3/c1-26-12-14-27(15-13-26)10-2-3-11-28-22(30)17-29(23(28)31)25-16-20-8-9-21(32-20)18-4-6-19(24)7-5-18/h4-9,16H,2-3,10-15,17H2,1H3/b25-16+^Y Key:MREBEPTUUMTTIA-PCLIKHOPSA-N^Y
^NY (what is this?) (verify)

Azimilide is a class ΙΙΙ antiarrhythmic drug (used to control abnormal heart rhythms). The agents from this heterogeneous group have an effect on the repolarization, they prolong the duration of the action potential and the refractory period. Also they slow down the spontaneous discharge frequency of automatic pacemakers by depressing the slope of diastolic depolarization. They shift the threshold towards zero or hyperpolarize the membrane potential. Although each agent has its own properties and will have thus a different function.

Heart potential

[edit]

Azimilide dihydrochloride is a chlorophenylfuranyl compound, which slows repolarization of the heart and prolongs the QT interval of the electrocardiogram. Prolongation of atrial or ventricular repolarization can provide an anti-arrhythmic benefit in patients with heart rhythm disturbances, and this has been the primary interest in the clinical development azimilide. In rare cases, excessive prolongation of ventricular repolarization by azimilide can result in predisposition towards severe ventricular arrhythmias. Most recent clinical trials have investigated the use of azimilide in reducing the frequency and severity of arrhythmias in patients with implanted cardiac pacemakers-defibrillators, where rare pro-arrhythmic events are rescued by the device.

The ion currents

[edit]

The action of azimilide is directed to the different currents present in atrial and ventricular cardiac myocytes. It principally blocks I_Kr, and I_Ks, with much weaker effects on I_Na, I_Ca, I_NCX and I_K.Ach. The I_Kr(rapid)and I_Ks (slow) are inward rectifier potassium currents, responsible for repolarizing cardiac myocytes towards the end of the cardiac action potential. A somewhat higher concentration of azimilide is needed to block the IKs current. Both blockages result in an increase of the QT interval and a prolongation of atrial and ventricular refractory periods.

Azimilide blocks hERG channels (which encode the I_Kr current) with an affinity comparable to that with which KvLQT1 / minK channels (which encode the I_Ks current) are blocked. This block exhibits reverse use-dependence, i.e. the channel blocking effect wanes at faster pulsing rates of the cell. A possible explanation is an interaction of azimilide with K⁺ close to its binding site in the ion channel. However, there is an agonist effect as well, which is a voltage-dependent effect. This is a dual effect, a low voltage depolarization near the activation threshold will increase the current amplitude and higher depolarizing voltages will suppress the current amplitude. The effect comes from outside of the cell membrane and does not depend on G-proteins or kinase activity inside the cell. Azimilide binds on the extracellular domain of the hERG channel, this propagates a conformational change and inhibits the current. This change makes the activation gate open more easily by low voltage depolarization. Azimilide has two separate binding sites in hERG channel, one for its antagonist function and the other for the agonist function.

Pharmacology

[edit]

Azimilide has been studied for its anti-arrhythmic effects: its converts and maintains sinus rhythm in patients with atrial arrhythmias; and it reduces the frequency and severity of ventricular arrhythmias in patients with implanted cardioverter-defibrillators. Azimilide's most important adverse effect is torsades de pointes, which is a form of ventricular tachycardia.

Pharmacokinetics

[edit]

The drug is administered orally and will be completely absorbed. It shows none or very minor interactions with other drugs and it will be eventually cleared by the kidney. A peak in concentration in the blood is observed seven hours after the administration of Azimilide. The metabolic clearance is mediated through several pathways:

10% is found unchanged in the blood
30% will cleared by cleavage
25% by CYP 1A1 pathway
25% by CYP 3A4

F-1292 is the major metabolite of azimilide, it is formed cleavage of the aromethine bond. Unlike desmethyl azimilide, azimilide N-oxide and azimilide carboxylate F-1292 has no cardiovascular activity while the other three minor metabolites have a class ΙΙΙ antiarrhythmic activity. They only make out 10% of azimilide in the blood, so their contribution is not measurable.

References

[edit]

Nishida A, Reien Y, Ogura T, Uemura H, Tamagawa M, Yabana H, Nakaya H (November 2007). "Effects of azimilide on the muscarinic acetylcholine receptor-operated K+ current and experimental atrial fibrillation in guinea-pig hearts". Journal of Pharmacological Sciences. 105 (3): 229–39. doi:10.1254/jphs.fp0070940. PMID 17965539.

Watanabe Y, Koide Y, Kimura J (September 2006). "Topics on the Na⁺/Ca²⁺: pharmacological characterization of Na+/Ca2+ exchanger inhibitors". Journal of Pharmacological Sciences. 102 (1): 7–16. doi:10.1254/jphs.fmj06002x2. PMID 16990699.

Hanna IR, Langberg JJ (December 2004). "The shocking story of azimilide". Circulation. 110 (24): 3624–6. doi:10.1161/01.CIR.0000151357.36405.72. PMID 15596558.

Lombardi F, Borggrefe M, Ruzyllo W, Lüderitz B (September 2006). "Azimilide vs. placebo and sotalol for persistent atrial fibrillation: the A-COMET-II (Azimilide-CardiOversion MaintEnance Trial-II) trial". European Heart Journal. 27 (18): 2224–31. doi:10.1093/eurheartj/ehl209. PMID 16935870.

Braunwald E, Zipes P, Libby P (2001). Heart Disease A Textbook of Cardiovascular Medicine (6th ed.). W.B. Saunders Company. pp. 717–736. ISBN 0-7216-8561-7.

Busch AE, Eigenberger B, Jurkiewicz NK, Salata JJ, Pica A, Suessbrich H, Lang F (January 1998). "Blockade of HERG channels by the class III antiarrhythmic azimilide: mode of action". British Journal of Pharmacology. 123 (1): 23–30. doi:10.1038/sj.bjp.0701575. PMC 1565134. PMID 9484850.

Jiang M, Dun W, Fan JS, Tseng GN (December 1999). "Use-dependent 'agonist' effect of azimilide on the HERG channel". The Journal of Pharmacology and Experimental Therapeutics. 291 (3): 1324–36. PMID 10565858.

Corey AE, Agnew JR, Valentine SN, Parekh NJ, Powell JH, Thompson GA (November 2002). "Effect of severe renal impairment on the pharmacokinetics of azimilide following single dose oral administration". British Journal of Clinical Pharmacology. 54 (5): 449–52. doi:10.1046/j.1365-2125.2002.01664.x. PMC 1874454. PMID 12445022.

v t e Piperazines
Simple piperazines (no additional rings)	Aminoethylpiperazine Diethylcarbamazine HEPPS Midafotel Piperazine PIPES
Phenylpiperazines	2C-B-PP 3,4-CFP Acaprazine Antrafenine Aripiprazole Batoprazine Bifeprunox BRL-15,572 Ciprofloxacin CSP-2503 Dapiprazole DCPP DMPP Diphenylpiperazine Dropropizine EGIS-12,233 Elopiprazole Eltoprazine Enpiprazole Ensaculin Etoperidone Flesinoxan Fluanisone Flibanserin Fluprazine Itraconazole Ketoconazole Levodropropizine Lorpiprazole mCPP Mefway MeOPP Mepiprazole Naftopidil Naluzotan Naphthylpiperazine Nefazodone Niaprazine Oxypertine Pardoprunox pCPP pFPP Posaconazole S-14,506 S-14,671 S-15,535 SB-258,585 SB-271,046 SB-357,134 SB-399,885 Sonepiprazole TFMPP Tolpiprazole Trazodone Urapidil Vesnarinone Vilazodone Vortioxetine WAY-100,135 WAY-100,635
Benzylpiperazines	2C-B-BZP 3-Methylbenzylpiperazine Befuraline Bifeprunox Buclizine BZP Chlorbenzoxamine DBZP Fipexide Imatinib MBZP MDBZP Meclozine Methoxypiperamide NSI-189 Piberaline Piribedil RN-1747 Sunifiram Trimetazidine Vesnarinone
Diphenylalkylpiperazines (benzhydrylalkylpiperazines)	AD-1211 Almitrine Amperozide BRL-15,572 Buclizine BW373U86 Cetirizine Chlorbenzoxamine Chlorcyclizine Cinnarizine Clocinizine Cyclizine DBL-583 Diphenpipenol Diphenylmethylpiperazine Dotarizine DPI-221 DPI-287 DPI-3290 GBR-12,783 GBR-12,935 GBR-13,069 GBR-13,098 GBR-13,119 Hydroxyzine Lidoflazine Manidipine Meclozine MT-45 Oxatomide SNC-80 Vanoxerine
Pyrimidinylpiperazines	Buspirone Dasatinib Eptapirone Gepirone Ipsapirone Piribedil Prazitone Pyrimidinylpiperazine Revospirone Tandospirone Tirilazad Trimazosin Umespirone Zalospirone
Pyridinylpiperazines	Atevirdine Azaperone Delavirdine Mirtazapine ORG-12962 Pyridinylpiperazine
Benzo(iso)thiazolyl piperazines	Lurasidone Perospirone Revospirone Tiospirone Ziprasidone
Tricyclics (piperazine attached via side chain)	Amoxapine Clopenthixol Clorotepine Clozapine Cyanothepin Doclothepin Docloxythepin Flupentixol Fluphenazine Isofloxythepin Loxapine Meperathiepin Metitepine Octomethothepin Olanzapine Opipramol Oxyclothepin Oxyprothepin Peradithiepin Perathiepin Perazine Perphenazine Pirenzepine Prochlorperazine Thiethylperazine Thiothixene Trifluoperazine Trifluthepin Zuclopenthixol
Others/Uncategorized	6-Nitroquipazine AP-238 Azimilide Bucinnazine Cinepazet Cinepazic acid Cinepazide CPD-1 Cyclohexylpiperazine EGIS-7625 Hexocyclium Indinavir JNJ-7777120 Lodenafil MK-212 Mirodenafil PB-28 Quipazine Ranolazine SA-4503 Sildenafil Tadalafil Vardenafil VUF-6002 WY-46824 Zipeprol

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