Milrinone

Milrinone
Clinical data
AHFS/Drugs.com	Monograph
MedlinePlus	a601020
Routes of; administration	IV only
ATC code	C01CE02 (WHO) ;
Legal status
Legal status	In general: ℞ (Prescription only);
Pharmacokinetic data
Bioavailability	100% (as IV bolus, infusion)
Protein binding	70 to 80%
Metabolism	Hepatic (12%)
Elimination half-life	2.3 hours (mean, in CHF)
Excretion	Urine (85% as unchanged drug) within 24 hours
Identifiers
	IUPAC name 2-Methyl-6-oxo-1,6-dihydro-3,4'-bipyridine-5-carbonitrile;
CAS Number	78415-72-2 ;
PubChem CID	4197;
IUPHAR/BPS	5225;
DrugBank	DB00235 ;
ChemSpider	4052 ;
UNII	JU9YAX04C7;
KEGG	D00417 ;
ChEBI	CHEBI:50693 ;
ChEMBL	ChEMBL189 ;
CompTox Dashboard (EPA)	DTXSID5023324 ;
ECHA InfoCard	100.071.709
Chemical and physical data
Formula	C12H9N3O
Molar mass	211.224 g·mol−1
3D model (JSmol)	Interactive image;
Density	1.344 g/cm3
Melting point	315 °C (599 °F)
	SMILES c1cnccc1-c2c(C)[nH]c(=O)c(C#N)c2;
	InChI InChI=1S/C12H9N3O/c1-8-11(9-2-4-14-5-3-9)6-10(7-13)12(16)15-8/h2-6H,1H3,(H,15,16) ; Key:PZRHRDRVRGEVNW-UHFFFAOYSA-N ;

Milrinone, commonly known and marketed under the brand name Primacor, is a pulmonary vasodilator^[1] used in patients who have heart failure. It is a phosphodiesterase 3 inhibitor that works to increase the heart's contractility and decrease pulmonary vascular resistance. Milrinone also works to vasodilate which helps alleviate increased pressures (afterload) on the heart, thus improving its pumping action. While it has been used in people with heart failure for many years, studies suggest that milrinone may exhibit some negative side effects that have caused some debate about its use clinically.^[2]^[3]

Overall, milrinone supports ventricular functioning of the heart by decreasing the degradation of cyclic adenosine monophosphate (cAMP) and thus increasing phosphorylation levels of many components in the heart that contribute to contractility and heart rate. Milrinone is used as a drug that causes positive ionotrophy and it will lead to an increased force of contraction. Milrinone use following cardiac surgery has been under some debate because of the potential increase risk of postoperative atrial arrhythmias.^[4] However, in the short term milrinone has been deemed beneficial to those experiencing heart failure and an effective therapy to maintain heart function following cardiac surgeries. There is no evidence of any long term beneficial effects on survival.^[5] In critically ill patients with evidence of cardiac dysfunction there is limited good quality evidence to recommend its use.^[6]

Milrinone is administered IV only and eliminated unchanged in the urine. Dose adjustment is required for patients with renal impairment.^{[citation needed]}

Contractility in the heart[]

People experiencing some forms of heart failure have a significant decrease in the contractile ability of muscle cells in the heart (cardiomyocytes). This impaired contractility occurs through a number of mechanisms. Some of the main problems associated with decreased contractility in those with heart failure are issues arising from imbalances in the concentration of calcium. Calcium permits myosin and actin to interact which allows initiation of contraction within the cardiomyocytes. In those with heart failure there may be a decreased amount of calcium within the cardiomyocytes reducing the available calcium to initiate contraction. When contractility is decreased the amount of blood being pumped out of the heart into circulation is decreased as well. This reduction in cardiac output can cause many systemic implications such as fatigue, syncope and other issues associated with decreased blood flow to peripheral tissues.

Mechanism of action[]

cAMP causes increased activation of protein kinase A (PKA). PKA is an enzyme that phosphorylates many elements of the contractile machinery within the heart cell. In the short term this leads to an increased force of contraction. Phosphodiesterases are enzymes responsible for the breakdown of cAMP. Therefore, when phosphodiesterases lower the level of cAMP in the cell they also lower the active fraction of PKA within the cell and reduce the force of contraction.

Milrinone is a phosphodiesterase-3 inhibitor. This drug inhibits the action of phosphodiesterase-3 and thus prevents degradation of cAMP. With increased cAMP levels there is an increase in the activation of PKA. This PKA will phosphorylate many components of the cardiomyocyte such as calcium channels and components of the myofilaments. Phosphorylation of calcium channels permits an increase in calcium influx into the cell. This increase in calcium influx results in increased contractility. PKA also phosphorylates potassium channels promoting their action. Potassium channels are responsible for repolarization of the cardiomyocytes therefore increasing the rate at which cells can depolarize and generate contraction. PKA also phosphorylates components on myofilaments allowing actin and myosin to interact more easily and thus increasing contractility and the inotropic state of the heart. Milrinone allows stimulation of cardiac function independently of β-adrenergic receptors which appear to be down-regulated in those with heart failure.

Clinical use[]

Milrinone is a commonly used therapy for severe pulmonary arterial hypertension (PAH),^[7] often in combination with other medications such as sildenafil.^[8] Targeting PDE3 with optimal doses and timing, milrinone prevents allergic inflammation in HDM-driven models of allergic airway inflammation.^[9]

Adverse effects[]

Common adverse effects include ventricular arrhythmias (including ventricular ectopy and ), supraventricular arrhythmias, hypotension, and headache.^[10]

References[]

^ Baxter, Frederick J.; Whippey, Amanda (2020). "Amniotic Fluid Embolism Treated with Inhaled Milrinone: A Case Report". A&A Practice. 14 (13): e01342. doi:10.1213/XAA.0000000000001342. PMID 33185413. S2CID 226851766.
^ Packer M (December 1990). "Calcium channel blockers in chronic heart failure. The risks of "physiologically rational" therapy". Circulation. 82 (6): 2254–7. doi:10.1161/01.cir.82.6.2254. PMID 2242549. S2CID 11255642.
^ Packer M, Carver JR, Rodeheffer RJ, Ivanhoe RJ, DiBianco R, Zeldis SM, et al. (November 1991). "Effect of oral milrinone on mortality in severe chronic heart failure. The PROMISE Study Research Group". The New England Journal of Medicine. 325 (21): 1468–75. doi:10.1056/NEJM199111213252103. PMID 1944425.
^ Fleming GA, Murray KT, Yu C, Byrne JG, Greelish JP, Petracek MR, et al. (October 2008). "Milrinone use is associated with postoperative atrial fibrillation after cardiac surgery". Circulation. 118 (16): 1619–25. doi:10.1161/CIRCULATIONAHA.108.790162. PMC 2770257. PMID 18824641.
^ British National Formulary. 66 ed. London: BMJ Group and Pharmaceutical Press; Sept 2013
^ Koster G, Bekema HJ, Wetterslev J, Gluud C, Keus F, van der Horst IC (September 2016). "Milrinone for cardiac dysfunction in critically ill adult patients: a systematic review of randomised clinical trials with meta-analysis and trial sequential analysis". Intensive Care Medicine. 42 (9): 1322–35. doi:10.1007/s00134-016-4449-6. PMC 4992029. PMID 27448246.
^ McNamara PJ, Shivananda SP, Sahni M, Freeman D, Taddio A (January 2013). "Pharmacology of milrinone in neonates with persistent pulmonary hypertension of the newborn and suboptimal response to inhaled nitric oxide". Pediatric Critical Care Medicine. 14 (1): 74–84. doi:10.1097/PCC.0b013e31824ea2cd. PMID 23132395. S2CID 7696208.
^ Hui-li G (June 2011). "The management of acute pulmonary arterial hypertension". Cardiovascular Therapeutics. 29 (3): 153–75. doi:10.1111/j.1755-5922.2009.00095.x. PMID 20560976.
^ Beute J, Lukkes M, Koekoek EP, Nastiti H, Ganesh K, de Bruijn MJ, et al. (2018). "A pathophysiological role of PDE3 in allergic airway inflammation". JCI Insight. 3 (2). doi:10.1172/jci.insight.94888. PMC 5821178. PMID 29367458.
^ "Milrinone Lactate Monograph". drugs.com.

External links[]

Mechanism of action

[1] Baxter, Frederick J.; Whippey, Amanda (2020). "Amniotic Fluid Embolism Treated with Inhaled Milrinone: A Case Report". A&A Practice. 14 (13): e01342. doi:10.1213/XAA.0000000000001342. PMID 33185413. S2CID 226851766.

[2] Packer M (December 1990). "Calcium channel blockers in chronic heart failure. The risks of "physiologically rational" therapy". Circulation. 82 (6): 2254–7. doi:10.1161/01.cir.82.6.2254. PMID 2242549. S2CID 11255642.

[3] Packer M, Carver JR, Rodeheffer RJ, Ivanhoe RJ, DiBianco R, Zeldis SM, et al. (November 1991). "Effect of oral milrinone on mortality in severe chronic heart failure. The PROMISE Study Research Group". The New England Journal of Medicine. 325 (21): 1468–75. doi:10.1056/NEJM199111213252103. PMID 1944425.

[4] Fleming GA, Murray KT, Yu C, Byrne JG, Greelish JP, Petracek MR, et al. (October 2008). "Milrinone use is associated with postoperative atrial fibrillation after cardiac surgery". Circulation. 118 (16): 1619–25. doi:10.1161/CIRCULATIONAHA.108.790162. PMC 2770257. PMID 18824641.

[5] British National Formulary. 66 ed. London: BMJ Group and Pharmaceutical Press; Sept 2013

[6] Koster G, Bekema HJ, Wetterslev J, Gluud C, Keus F, van der Horst IC (September 2016). "Milrinone for cardiac dysfunction in critically ill adult patients: a systematic review of randomised clinical trials with meta-analysis and trial sequential analysis". Intensive Care Medicine. 42 (9): 1322–35. doi:10.1007/s00134-016-4449-6. PMC 4992029. PMID 27448246.

[7] McNamara PJ, Shivananda SP, Sahni M, Freeman D, Taddio A (January 2013). "Pharmacology of milrinone in neonates with persistent pulmonary hypertension of the newborn and suboptimal response to inhaled nitric oxide". Pediatric Critical Care Medicine. 14 (1): 74–84. doi:10.1097/PCC.0b013e31824ea2cd. PMID 23132395. S2CID 7696208.

[8] Hui-li G (June 2011). "The management of acute pulmonary arterial hypertension". Cardiovascular Therapeutics. 29 (3): 153–75. doi:10.1111/j.1755-5922.2009.00095.x. PMID 20560976.

[9] Beute J, Lukkes M, Koekoek EP, Nastiti H, Ganesh K, de Bruijn MJ, et al. (2018). "A pathophysiological role of PDE3 in allergic airway inflammation". JCI Insight. 3 (2). doi:10.1172/jci.insight.94888. PMC 5821178. PMID 29367458.

[10] "Milrinone Lactate Monograph". drugs.com.

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v t Phosphodiesterase inhibitors
PDE1	MMPX SCH-51866 Vinpocetine
PDE2	BAY 60-7550 EHNA Oxindole
PDE3	Adibendan Amrinone (inamrinone) Anagrelide Bucladesine Cilostamide Cilostazol Enoximone KMUP-1 Milrinone Olprinone Pimobendan Quazinone RPL-554 Siguazodan Trequinsin Vesnarinone Zardaverine
PDE4	Apremilast Arofylline Atizoram CC-1088 Cilomilast Crisaborole Drotaverine Etazolate Filaminast Glaucine HT-0712 ICI-63197 Irsogladine Luteolin Mesembrenone Mesembrine Piclamilast Roflumilast Rolipram RPL-554 YM-976 Zardaverine
PDE5	Acetildenafil Aildenafil Avanafil Benzamidenafil Icariin Homosildenafil Lodenafil Mirodenafil MY-5445 Nitrosoprodenafil SCH-51866 Sildenafil Sulfoaildenafil T-0156 Tadalafil Udenafil Vardenafil
PDE7	BRL-50481
PDE9	BAY 73-6691 Paraxanthine
PDE10	Mardepodect Papaverine Tofisopam
PDE11
Non-selective	Aminophylline Caffeine Choline theophyllinate CPX Dipyridamole Doxofylline Enprofylline Ibudilast IBMX Luteolin Pentoxifylline Propentofylline Theobromine Theophylline Zaprinast
Unsorted	Diazepam Diprophylline DPCPX Furafylline Lisofylline Moxaverine Pentifylline Proxyphylline Quercetin Trapidil
See also: Receptor/signaling modulators