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Vernakalant

January 01, 1970

Vernakalant, sold under the brand name Brinavess, is a class III antiarrhythmic drug for the acute conversion of atrial fibrillation, a kind of irregular heartbeat, in form of an intravenous infusion. It has been approved for use in the European Union and the United Kingdom since 2010. The US Food and Drug Administration denied approval in 2008 and 2019.

Vernakalant
Clinical data
Trade namesBrinavess
Other namesRSD1235
Routes of
administration		Intravenous,[1]
ATC code
Legal status
Legal status
  • CA: ℞-only[2]
  • EU: Rx-only
  • In general: ℞ (Prescription only)
Pharmacokinetic data
Protein bindinglow
MetabolismCYP2D6, glucuronidation
Elimination half-life3–5.5 hours
Identifiers
  • (3R)-1-{(1R,2R)-2-[2-(3,4-dimethoxyphenyl)
    ethoxy]cyclohexyl}pyrrolidin-3-ol
CAS Number
  • 794466-70-9 Y
  • [https://commonchemistry.cas.org/detail?cas_rn=748810-28-8&title= 748810-28-8 (HCl) 748810-28-8 (HCl)]
PubChem CID
  • 9930049
DrugBank
  • DB06217 Y
ChemSpider
  • 8105680 N
UNII
  • 9G468C8B13
KEGG
  • D06665
CompTox Dashboard (EPA)
  • DTXSID60229659
ECHA InfoCard100.121.790
Chemical and physical data
FormulaC20H31NO4
Molar mass349.471 g·mol−1
3D model (JSmol)
  • Interactive image
  • O(c1ccc(cc1OC)CCO[C@@H]3CCCC[C@H]3N2CC[C@@H](O)C2)C
  • InChI=1S/C20H31NO4/c1-23-19-8-7-15(13-20(19)24-2)10-12-25-18-6-4-3-5-17(18)21-11-9-16(22)14-21/h7-8,13,16-18,22H,3-6,9-12,14H2,1-2H3/t16-,17-,18-/m1/s1 N
  • Key:VBHQKCBVWWUUKN-KZNAEPCWSA-N N
 NY (what is this?)  (verify)

Medical uses edit

The drug is used for the treatment of atrial fibrillation lasting up to three days in adults after heart surgery, or lasting up to seven days in other adults, as an intravenous infusion.[1]

Contraindications edit

Vernakalant is contraindicated in a number of heart conditions:

Vernakalant and other intravenous rhythm control drugs (class I and class III antiarrhythmics) must not be given within four hours of each other.[1]

Side effects edit

The most common adverse effects in studies were dysgeusia (taste disturbance, in 18% of patients), sneezing (13%) and paraesthesia (abnormal skin sensations, 7%); they were transient and rarely led to an abortion of the treatment. Potentially serious side effects included low blood pressure and conversion of the heart rhythm to atrial flutter instead of a normal sinus rhythm; flutter mostly responded to a second dose of vernakalant.[1]

Overdose edit

There is a single case report of a person receiving an infusion of the full vernakalant dose in half the recommended time, resulting in tachycardia (fast heartbeat) without lasting adverse effects.[1]

Interactions edit

Drugs that inhibit the liver enzyme CYP2D6 might theoretically increase vernakalant concentrations in the body, as the latter is metabolized by this enzyme; but this has been found to be of no clinical significance. While the drug itself is a moderate CYP2D6 inhibitor, it is not expected to have a relevant impact on other pharmaceuticals that are broken down by this enzyme, because it only remains in the body for a short time. Vernakalant probably interacts with other antiarrhythmic drugs, although no formal studies have been done.[1]

Pharmacology edit

Mechanism of action edit

Like other class III antiarrhythmics, vernakalant blocks atrial potassium channels, thereby prolonging repolarization. It differs from typical class III agents by blocking a certain type of potassium channel, the cardiac transient outward potassium current, with increased potency as the heart rate increases. This means that it is more effective at high heart rates, while other class III agents tend to lose effectiveness under these circumstances. It also slightly blocks the hERG potassium channel, leading to a prolonged QT interval. This may theoretically increase the risk of ventricular tachycardia, though this does not seem to be clinically relevant.[3]

The drug also blocks atrial sodium channels.[3]

Pharmacokinetics and pharmacogenomics edit

After infusion, the substance is rapidly distributed in the body. In the blood serum, 53–56% are circulating freely and are not bound to plasma proteins. In people with normal CYP2D6 function, the main route of degradation is by O-demethylation via this enzyme. In 2D6 poor metabolizers, vernakalant is mainly inactivated by glucuronidation and excreted by the kidney. Elimination half-life is three hours in 2D6 extensive (normal) metabolizers and 5.5 hours in poor metabolizers. The differences between poor and extensive metabolizers regarding peak concentrations, AUC and half-life are not clinically relevant.[1][4]

Vernakalant does not inhibit the enzymes CYP3A4, CYP1A2, CYP2C9, CYP2C19, CYP2E1, nor the transporter protein P-gp.[1]

Chemistry edit

The molecule has three asymmetric carbon atoms, allowing for 23 = 8 stereomers. The trans stereomers are known to be pharmacologically active, but only the RRR-form is contained in the marketed formulation. The SRR-form (with the hydroxyl group in S configuration) is a minor metabolite that is formed in the human body, mainly in poor metabolizers.[4]

The infusion contains vernakalant hydrochloride, which is highly water-soluble.[4]

History edit

Vernakalant was initially developed by Cardiome Pharma, and the intravenous formulation was bought for further development by Merck in April 2009.[5] In September 2012, Merck terminated its agreements with Cardiome and has consequently returned all rights of the drug back to Cardiome, which as of 2018 is known as Correvio Pharma.[citation needed]

In December 2007, the Cardiovascular and Renal Drugs Advisory Committee of the US Food and Drug Administration (FDA) voted to recommend the approval of vernakalant,[6] but in August 2008, the FDA judged that additional information was necessary for approval.[5] In the European Union, the medication was approved under the brand name Brinavess in September 2010.[7]

An oral formulation underwent phase II clinical trials between 2005 and 2008.[8][9]

In December 2019, the resubmitted New Drug Application for vernakalant was discussed by the Cardiovascular and Renal Drugs Advisory Committee.[10] The Advisory Committee voted not to recommend the approval.[11]

References edit

  1. ^ a b c d e f g h "Brinavess: EPAR – Product information" (PDF). European Medicines Agency. 19 December 2019.
  2. ^ "Heart health". Health Canada. 9 May 2018. Retrieved 13 April 2024.
  3. ^ a b Finnin M (July 2010). "Vernakalant: A novel agent for the termination of atrial fibrillation". American Journal of Health-System Pharmacy. 67 (14): 1157–64. doi:10.2146/ajhp080501. PMID 20592320.
  4. ^ a b c "Brinavess: EPAR – Public assessment report" (PDF). European Medicines Agency. 25 June 2010.
  5. ^ a b "Merck and Cardiome Pharma Sign License Agreement for Vernakalant, an Investigational Drug for Treatment of Atrial Fibrillation". FierceBiotech. 9 April 2009. Retrieved 12 October 2010.
  6. ^ "FDA Advisory Committee Recommends Approval of Kynapid for Acute Atrial Fibrillation". Drugs.com. Retrieved 15 March 2008.
  7. ^ (Press release). Merck & Co., Inc. 1 September 2010. Archived from the original on 28 September 2010. Retrieved 28 September 2010.
  8. ^ Clinical trial number NCT00267930 for "Study of RSD1235-SR for the Prevention of Atrial Fibrillation/Atrial Flutter Recurrence" at ClinicalTrials.gov
  9. ^ Clinical trial number NCT00526136 for "Vernakalant (Oral) Prevention of Atrial Fibrillation Recurrence Post-Conversion Study" at ClinicalTrials.gov
  10. ^ "December 10, 2019 Meeting of the Cardiovascular and Renal Drugs Advisory Committee Meeting Announcement". FDA. Retrieved 9 December 2019.
  11. ^ "FDA Panel Shoots Down Afib Cardioversion Drug Over Safety". MedPage Today. Retrieved 11 December 2019.

January 01, 1970
vernakalant, sold, under, brand, name, brinavess, class, antiarrhythmic, drug, acute, conversion, atrial, fibrillation, kind, irregular, heartbeat, form, intravenous, infusion, been, approved, european, union, united, kingdom, since, 2010, food, drug, administ. Vernakalant sold under the brand name Brinavess is a class III antiarrhythmic drug for the acute conversion of atrial fibrillation a kind of irregular heartbeat in form of an intravenous infusion It has been approved for use in the European Union and the United Kingdom since 2010 The US Food and Drug Administration denied approval in 2008 and 2019 VernakalantClinical dataTrade namesBrinavessOther namesRSD1235Routes ofadministrationIntravenous 1 ATC codeC01BG11 WHO Legal statusLegal statusCA only 2 EU Rx only In general Prescription only Pharmacokinetic dataProtein bindinglowMetabolismCYP2D6 glucuronidationElimination half life3 5 5 hoursIdentifiersIUPAC name 3R 1 1R 2R 2 2 3 4 dimethoxyphenyl ethoxy cyclohexyl pyrrolidin 3 olCAS Number794466 70 9 Y https commonchemistry cas org detail cas rn 748810 28 8 amp title 748810 28 8 HCl 748810 28 8 HCl PubChem CID9930049DrugBankDB06217 YChemSpider8105680 NUNII9G468C8B13KEGGD06665CompTox Dashboard EPA DTXSID60229659ECHA InfoCard100 121 790Chemical and physical dataFormulaC 20H 31N O 4Molar mass349 471 g mol 13D model JSmol Interactive imageSMILES O c1ccc cc1OC CCO C H 3CCCC C H 3N2CC C H O C2 CInChI InChI 1S C20H31NO4 c1 23 19 8 7 15 13 20 19 24 2 10 12 25 18 6 4 3 5 17 18 21 11 9 16 22 14 21 h7 8 13 16 18 22H 3 6 9 12 14H2 1 2H3 t16 17 18 m1 s1 NKey VBHQKCBVWWUUKN KZNAEPCWSA N N N Y what is this verify Contents 1 Medical uses 2 Contraindications 3 Side effects 4 Overdose 5 Interactions 6 Pharmacology 6 1 Mechanism of action 6 2 Pharmacokinetics and pharmacogenomics 7 Chemistry 8 History 9 ReferencesMedical uses editThe drug is used for the treatment of atrial fibrillation lasting up to three days in adults after heart surgery or lasting up to seven days in other adults as an intravenous infusion 1 Contraindications editVernakalant is contraindicated in a number of heart conditions severe aortic stenosis low blood pressure systolic pressure under 100 mmHg heart failure NYHA class III IV prolonged QT time severe bradycardia slow heart rate sinus node dysfunction second or third degree atrioventricular block acute coronary syndrome including heart attack Vernakalant and other intravenous rhythm control drugs class I and class III antiarrhythmics must not be given within four hours of each other 1 Side effects editThe most common adverse effects in studies were dysgeusia taste disturbance in 18 of patients sneezing 13 and paraesthesia abnormal skin sensations 7 they were transient and rarely led to an abortion of the treatment Potentially serious side effects included low blood pressure and conversion of the heart rhythm to atrial flutter instead of a normal sinus rhythm flutter mostly responded to a second dose of vernakalant 1 Overdose editThere is a single case report of a person receiving an infusion of the full vernakalant dose in half the recommended time resulting in tachycardia fast heartbeat without lasting adverse effects 1 Interactions editDrugs that inhibit the liver enzyme CYP2D6 might theoretically increase vernakalant concentrations in the body as the latter is metabolized by this enzyme but this has been found to be of no clinical significance While the drug itself is a moderate CYP2D6 inhibitor it is not expected to have a relevant impact on other pharmaceuticals that are broken down by this enzyme because it only remains in the body for a short time Vernakalant probably interacts with other antiarrhythmic drugs although no formal studies have been done 1 Pharmacology editMechanism of action edit Like other class III antiarrhythmics vernakalant blocks atrial potassium channels thereby prolonging repolarization It differs from typical class III agents by blocking a certain type of potassium channel the cardiac transient outward potassium current with increased potency as the heart rate increases This means that it is more effective at high heart rates while other class III agents tend to lose effectiveness under these circumstances It also slightly blocks the hERG potassium channel leading to a prolonged QT interval This may theoretically increase the risk of ventricular tachycardia though this does not seem to be clinically relevant 3 The drug also blocks atrial sodium channels 3 Pharmacokinetics and pharmacogenomics edit After infusion the substance is rapidly distributed in the body In the blood serum 53 56 are circulating freely and are not bound to plasma proteins In people with normal CYP2D6 function the main route of degradation is by O demethylation via this enzyme In 2D6 poor metabolizers vernakalant is mainly inactivated by glucuronidation and excreted by the kidney Elimination half life is three hours in 2D6 extensive normal metabolizers and 5 5 hours in poor metabolizers The differences between poor and extensive metabolizers regarding peak concentrations AUC and half life are not clinically relevant 1 4 Vernakalant does not inhibit the enzymes CYP3A4 CYP1A2 CYP2C9 CYP2C19 CYP2E1 nor the transporter protein P gp 1 Chemistry editThe molecule has three asymmetric carbon atoms allowing for 23 8 stereomers The trans stereomers are known to be pharmacologically active but only the RRR form is contained in the marketed formulation The SRR form with the hydroxyl group in S configuration is a minor metabolite that is formed in the human body mainly in poor metabolizers 4 The infusion contains vernakalant hydrochloride which is highly water soluble 4 History editVernakalant was initially developed by Cardiome Pharma and the intravenous formulation was bought for further development by Merck in April 2009 5 In September 2012 Merck terminated its agreements with Cardiome and has consequently returned all rights of the drug back to Cardiome which as of 2018 is known as Correvio Pharma citation needed In December 2007 the Cardiovascular and Renal Drugs Advisory Committee of the US Food and Drug Administration FDA voted to recommend the approval of vernakalant 6 but in August 2008 the FDA judged that additional information was necessary for approval 5 In the European Union the medication was approved under the brand name Brinavess in September 2010 7 An oral formulation underwent phase II clinical trials between 2005 and 2008 8 9 In December 2019 the resubmitted New Drug Application for vernakalant was discussed by the Cardiovascular and Renal Drugs Advisory Committee 10 The Advisory Committee voted not to recommend the approval 11 References edit a b c d e f g h Brinavess EPAR Product information PDF European Medicines Agency 19 December 2019 Heart health Health Canada 9 May 2018 Retrieved 13 April 2024 a b Finnin M July 2010 Vernakalant A novel agent for the termination of atrial fibrillation American Journal of Health System Pharmacy 67 14 1157 64 doi 10 2146 ajhp080501 PMID 20592320 a b c Brinavess EPAR Public assessment report PDF European Medicines Agency 25 June 2010 a b Merck and Cardiome Pharma Sign License Agreement for Vernakalant an Investigational Drug for Treatment of Atrial Fibrillation FierceBiotech 9 April 2009 Retrieved 12 October 2010 FDA Advisory Committee Recommends Approval of Kynapid for Acute Atrial Fibrillation Drugs com Retrieved 15 March 2008 Brinavess vernakalant for Infusion Approved in the European Union for Rapid Conversion of Recent Onset Atrial Fibrillation Press release Merck amp Co Inc 1 September 2010 Archived from the original on 28 September 2010 Retrieved 28 September 2010 Clinical trial number NCT00267930 for Study of RSD1235 SR for the Prevention of Atrial Fibrillation Atrial Flutter Recurrence at ClinicalTrials gov Clinical trial number NCT00526136 for Vernakalant Oral Prevention of Atrial Fibrillation Recurrence Post Conversion Study at ClinicalTrials gov December 10 2019 Meeting of the Cardiovascular and Renal Drugs Advisory Committee Meeting Announcement FDA Retrieved 9 December 2019 FDA Panel Shoots Down Afib Cardioversion Drug Over Safety MedPage Today Retrieved 11 December 2019 Retrieved from https en wikipedia org w index php title Vernakalant amp oldid 1220353686, wikipedia, wiki, book, books, library,

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