Reassessment of Dobutamine, Dopamine, and Milrinone in the Management of Acute Heart Failure Syndromes Melike Bayram, MD,a Leonardo De Luca, MD,b M. Barry Massie, MD,c and Mihai Gheorghiade, MDd,* The appropriate role of intravenous inodilator therapy (inotropic agents with vaso- dilator properties) in the management of acute heart failure syndromes (AHFS) has longbeenasubjectofcontroversy,mainlybecauseofthelackofprospective,placebo- controlledtrialsandalackofalternativetherapies.Theuseofintravenousinodilator infusions,however,remainscommon,buthighlyvariable.Asnewoptionsemergefor the treatment of AHFS, the available information should be reviewed to determine which approaches are supported by evidence, which are used empirically without evidence, and which should be considered inappropriate. For these purposes, we reviewed data available from randomized controlled trials on short-term, intermit- tent,andlong-termuseofintravenousinodilatoragents(dobutamine,dopamine,and milrinone) in AHFS. Randomized controlled trials failed to show benefits with current medications and suggested that acute, intermittent, or continuous use of inodilator infusions may increase morbidity and mortality in patients with AHFS. Their use should be restricted to patients who are hypotensive as a result of low cardiac output despite a high left ventricular filling pressure. © 2005 Elsevier Inc. All rights reserved. (Am J Cardiol 2005;96[suppl]:47G–58G) Acute heart failure syndromes (AHFS) resulting in hospi- thatmayadverselyaffectpostdischargemorbidityandmor- talization represent a major public health problem because tality. of the high numbers of patients (1 million in the United Randomized controlled trials failed to show a benefit States),postdischargemortalityandreadmissionrates(10% with the acute,4 intermittent,5 or continuous6 use of inodi- and25%at60days,respectively),andsignificantassociated lators in patients with heart failure (HF). Despite these costs ($27.9 billion per year).1 Most patients with AHFS negative results, dobutamine, dopamine, and milrinone are presenttotheemergencyroomwitharelativelyhighblood often given to improve cardiac performance and to relieve pressureandsystemiccongestionwithoutsignsofsystemic congestive symptoms of AHFS, even in patients with nor- hypoperfusion (normal cardiac output). In addition, based malbloodpressureandrelativelypreservedcardiacoutput. on the Acute Decompensated Heart Failure National Reg- istry(ADHERE),almost50%ofthepatientsadmittedwith AHFS had a relatively preserved systolic function (PSF).2 Use of Inodilator Therapy in Acute Heart Failure These patients had a higher incidence of hypertension, left Syndromes Registries ventricularhypertrophy,anddiabetesmellitusthanpatients admitted with AHFS and systolic dysfunction.3 The ADHERE database was designed to study prospec- HowwemanageAHFSisimportantbecauseselectionof tively the outcomes, characteristics, and management of therapeutic agents, which are used for only days or hours, AHFS. In this registry, which currently comprises may influence long-term mortality and morbidity. The ini- (cid:1)150,000 patients, (cid:2)3% presented with a systolic blood tial therapy for patients with AHFS should improve symp- pressureof(cid:2)90mmHgandapproximately50%presented tomsandhemodynamicswithoutcausingmyocardialinjury with relative PSF.3 Approximately 14% of the patients in ADHERE were treated with (cid:1)1 acute infusions of inodila- tor agents (dobutamine 6%, dopamine 6%, and milrinone aDepartmentofMedicineResidencyTrainingProgram,Universityof 3%) in the hospital.7 Furthermore, among home discharges Michigan,AnnArbor,Michigan,USA;bDepartmentofCardiovascularand ofpatientswithapriorhistoryofHFduringthisperiod,1% Respiratory Sciences, La Sapienza University, Rome, Italy; cSection of weredischargedonchronicdobutamine,and1%onchronic Cardiology,SanFranciscoVeteransAffairsMedicalCenterandSchoolof Medicine,UniversityofCalifornia,SanFrancisco,SanFrancisco,Califor- milrinone infusion therapy.2 nia, USA; and dNorthwestern University Feinberg School of Medicine, Importantly, 15% of patients receiving inodilators had Chicago,Illinois,USA. PSF.8Theinodilator-treatedpatientswithPSFhadahigher *Addressforreprints:MihaiGheorghiade,MD,DivisionofCardiol- mortality rate (19%) than all other inodilator-treated pa- ogy,NorthwesternUniversityFeinbergSchoolofMedicine,Galter10-240, tients (14%).8 Patients with PSF who were treated with 201EastHuronStreet,Chicago,Illinois60611. E-mailaddress:[email protected]. inodilators also had a higher mortality rate than patients 0002-9149/05/$–seefrontmatter©2005ElsevierInc.Allrightsreserved. www.AJConline.org doi:10.1016/j.amjcard.2005.07.021 48G TheAmericanJournalofCardiology(www.AJConline.org) Vol96(6A) September19,2005 withPSFwhowerenottreatedwithinodilators(19%vs2%, gest that (cid:1)50% of patients with chronic HF and coronary respectively).8 Among the inodilator-treated patients, those artery disease (CAD) have hibernating myocardium, an with PSF also had a longer hospital stay compared with all adaptive response to a sustained reduction in coronary va- other inodilator-treated patients (mean, 12.9 vs 9.6 days).8 sodilator reserve in which the level of tissue perfusion is Although these results may be confounded by unmeasured sufficienttomaintaincellularviabilitybutnotsufficientfor differences in the patients and treatment settings in which normalcontractilefunction.15,16Thisprecariousbalancebe- inodilatortreatmentswereused,theydoraisethepossibility tween perfusion and tissue viability, however, is not sus- that these agents may be harmful, especially when used in tainedindefinitelyandwillprogresstomyocardialnecrosis patients who are not appropriate for this therapy. unlessthebloodflowincreases.15,17–26Areasofhibernating Recently, in a retrospective observational analysis of myocardium or contractile reserve may be adversely af- ADHERE, Abraham and coworkers9 compared in-hospital fected by inodilator agents. In fact, inodilators may cause mortality in a subset of 65,180 patients, 15,230 of whom worsening of ischemia by increasing myocardial oxygen were receiving either intravenous vasodilator therapy (ni- demand through increased contractility and induction of troglycerin or nesiritide) or inodilator therapy (dobutamine tachycardia. Schulz et al24 found that experimentally in- or milrinone). Short-term vasodilator therapy was associ- creasing the contractility of hibernating myocardium by ated with significantly lower in-hospital mortality than was using relatively low doses of an inodilator, such as dobut- positive inodilator therapy in patients hospitalized with amine, for short periods can lead to myocardial necrosis. AHFS. Unadjusted in-hospital mortality varied widely, Regardless of whether the myocytes are hibernating be- rangingfrom4.1%fortheentirecohorttoasmuchas14% cause of CAD or are alive but not contracting for other for patients who received inodilators.9,10 reasons, as is the case in idiopathic cardiomyopathy, stim- The Organized Program to Initiate Life-Saving Treat- ulation of these cells with an inodilator may result in cell ment in Hospitalized Patients with Heart Failure (OPTI- death through necrosis or apoptosis, thereby further reduc- MIZE-HF) study has been designed to improve medical ing contractility, creating a vicious cycle. For this reason, care and education of hospitalized patients with HF.11 patients treated with inodilators may improve clinically in Amongtheapproximately50,000patientswithHFenrolled the short term but may become more dependent on the use to date, 4% received dobutamine, 4% received dopamine, of inodilators. Thus, despite the apparent clinical improve- and 1% received milrinone during hospitalization.12 ment, there may be progression of HF in these patients. In a recent OPTIMIZE-HF subanalysis investigating the relationbetweenadmissionsystolicbloodpressureandout- comes in hospitalized patients with HF, inodilators were Mechanisms of Action and Effects of Inodilators used in 5.5% of patients with and without hypertension (admission systolic blood pressure between 119 and 200 Themostcommonlyusedinodilatoragentsworkthrougha mm Hg), compared with 18.5% of those with relative hy- common pathway of increased intracellular cyclic adeno- potension(admissionsystolicbloodpressure(cid:2)119mmHg) sine monophosphate (cAMP) and calcium concentrations. (M. Gheorghiade et al, unpublished data, 2005). These include (cid:2)-adrenergic agonists, endogenous cat- echolamines, and phosphodiesterase inhibitors. In Myocardial Viability Dobutamine—(cid:1)-adrenergic agonists:Dobutamine is a racemic mixture that stimulates (cid:2)- and (cid:2)-receptors. The 1 2 HF often results in myocyte hypertrophy and/or myocyte negative enantiomer is also an agonist for (cid:2)-receptors, 1 apoptosisornecrosis.However,inHF,asignificantnumber whereasthepositiveenantiomerisaveryweakpartialagonist. of patients with both ischemic and nonischemic cardiomy- Through its action on (cid:2)-receptors, dobutamine activates a 1 opathy and reduced systolic function have viable but non- guanine nucleotide regulatory cascade (via G proteins). This contractile myocardium. This condition can occur for a leads to increased adenylate cyclase activity and increased varietyofreasons,includingexcessiveandcontinuousneu- conversionofadenosinetriphosphate(ATP)totheintracellular rohormonal stimulation, hemodynamic abnormalities, and second messenger cAMP. Intracellular cAMP causes release chronic ischemia. The decrease in cardiac contractility that of calcium from the sarcoplasmic reticulum. The calcium is occurs in HF has been hypothesized to be an important used by contractile proteins and results in increased stroke compensatory mechanism that decreases energy use by the volume.27Inthevasculature,the(cid:3)-adrenergicagonisteffectof failing myocardium and thereby improves long-term sur- the negative enantiomer appears to be counteracted by the vival of cardiac myocytes.13 It has been suggested that partialagonismofthepositiveenantiomerandthevasodilatory although augmentation of contractility by various drugs action caused by (cid:2)-receptor stimulation. This usually results 2 producesatemporaryimprovementincardiacperformance, in a modest decrease in systemic vascular resistances and itmaydosoattheexpenseofincreasingmyocardialenergy venousfillingpressures.27 consumption and accelerating myocardial cell death.14 The rate of infusion doses of dobutamine needed to Recentstudiesusingpositronemissiontomographysug- increasecardiacoutputusuallyrangesfrom2.5to15(cid:4)g/kg Bayrametal/ReassessmentofDobutamine,Dopamine,andMilrinoneintheManagementofAHFS 49G permin.Onsetofactioniswithin1to2minutes,butitmay plained tachycardia or arrhythmia in a patient receiving take as long as 10 minutes to see the peak effect of a “low-dose” dopamine should make a clinician suspect an particularinfusionrate.Theplasmahalf-lifeofdobutamine inaccurate estimation of lean body weight resulting in an is 2 minutes. In studies with infusion periods (cid:1)24 to 72 inappropriately high dopamine infusion rate.27 The effects hours, cardiac output was noted to return toward baseline of dopamine on cardiac function and energy metabolism values in some study subjects, raising the concern of phar- have been compared with those of bucladesine.34 In this macologic tolerance with prolonged infusion. setting, dopamine enhanced anaerobic metabolism at both The overall effect of dobutamine on blood pressure is doses,withaconcomitantdecreaseinsystolicpressureand variable, depending on the relative effects on the vascular coronary flow. tone and cardiac output achieved. Heart rate is often de- Milrinone—phosphodiesterase inhibitors:Phosphodi- creasedbecauseofreflexwithdrawalofsympathetictonein esteraseistheenzymethatbreaksdownintracellularcAMP response to improved cardiovascular function. However, to its inactive metabolite (5=AMP). Milrinone is a bipyri- this is not always the case. The major side effects of do- dine derivative that selectively inhibits the phosphodiester- butamine include tachycardia, especially in patients with ase III enzyme, leading to increased intracellular cAMP.27 atrial fibrillation, and atrial and ventricular arrhythmias. Thisresultsinincreasedintracellularcalciumconcentration Patients taking a (cid:2)-blocker may have an attenuated initial andmyocardialcontractilityaswellasaccelerationofmyo- response to dobutamine until the (cid:2)-blocker has been cardial relaxation. Increased cAMP peripherally produces metabolized. vasodilationinboththearterialandvenouscirculation.The It has been hypothesized that the increased energy de- end result is decreased systemic and pulmonary vascular mands of the failing myocardium lead to a state of relative resistances,decreasedleftandrightventricularfillingpres- energy depletion through an initial compensatory phase of sures, and increased cardiac output. increased oxygen extraction.28,29 This paradigm suggests Treatmentwithmilrinonemaybeinitiatedwithaloading that further inodilator stimulation would impose further doseof50(cid:4)g/kgperminfollowedbyacontinuousinfusion energy demands and ultimately accelerate myocardial cell of between 0.25 and 1.0 (cid:4)g/kg per min or as an infusion death. Several investigators have attempted to demonstrate without the loading dose. Most patients have improvement this using a variety of methods to investigate myocardial inhemodynamicfunctionin5to15minutesafterinitiation oxygen consumption and a variety of in vitro and in vivo of therapy. The elimination half-life is 30 to 60 minutes models.Studiesinanimalmodelswithleftventriculardys- when tested in healthy individuals, but it is doubled in function demonstrated that dobutamine infusion is associ- patients with severe HF.27 ated with an increase in myocardial oxygen consumption A major side effect of milrinone is hypotension, and with a shift in myocardial metabolism, evidenced by an milrinoneisoftenadministeredwithoutaloadingdoseinan increasedpreferenceforglycolyticsubstrates.30,31Studiesin attempt to minimize the decrease in blood pressure. Other patients with ischemic or nonischemic dilated cardiomyop- side effects include increased atrial and ventricular ectopy athy also suggested that dobutamine increases myocardial (eg, nonsustained ventricular tachycardia). The metabolic oxygen consumption and the work-metabolic index.32,33 costofmilrinoneinpatientswithcongestiveHFisunclear, particularly when compared with other inodilator agents.35 Dopamine—endogenous catecholamines:Dopamine White et al36 determined the immediate effects of milri- isanendogenoussubstancewithdose-dependenteffects.At doses of (cid:5)2 (cid:4)g/kg per min, based on estimated lean body noneonexerciseperformancein14patientswithNewYork HeartAssociation(NYHA)classIIItoIVcongestiveHF,in weight, dopamine causes vasodilation by direct stimulation a randomized, double-blind, placebo-controlled study. of dopamine postsynaptic type 1 and presynaptic type 2 Compared with placebo, intravenous milrinone caused a receptors in the splanchnic and renal arterial beds.27 Dopa- higherpeakoxygenuptakeandoxygenuptakeattheanaer- minealsohasdirecteffectsonrenaltubularepithelialcells, obicthresholdwithaconcomitantdecreaseinbloodlactate resulting in increased natriuresis. Intermediateinfusionratesof2to5(cid:4)g/kgpermincause concentrations at matched submaximal exercise intensities. directstimulationof(cid:2)-adrenergicreceptorsintheheartand induce norepinephrine release from vascular sympathetic neurons. This results in increased heart rate and cardiac Trials: Intravenous Inodilator Therapy output. Infusion rates of 5 to 15 (cid:4)g/kg per min generally stimulate (cid:2)- and (cid:3)-adrenergic receptors, leading to an in- There are several different regimens of intravenous inodi- creased heart rate and peripheral vasoconstriction. lator therapy that have been used to treat patients with A major side effect of dopamine is tachycardia, which congestive HF. These agents are used for short-term inpa- tends to be much more pronounced with dopamine than tient therapy to treat AHFS. In this setting, patients are dobutamine.27 Another concern when using dopamine is usually infused over several hours to a few days in combi- correct dosing. Dopamine dose is based on lean body nationwithdiuretics.Acutetreatmentisdiscontinuedwhen weight, which can be difficult to estimate. A new or unex- patients are clinically stable. However, some patients de- 50G TheAmericanJournalofCardiology(www.AJConline.org) Vol96(6A) September19,2005 Table1 Mortalityat1monthand6monthsintheCalciumSensitizerorInotropeorNonein Low-OutputHeartFailureStudy(CASINO) EndPoint Dobutamine Placebo Levosimendan (n(cid:3)100) (n(cid:3)99) (n(cid:3)100) 1-momortality 14.0% 8.1% 6.0%* 6-momortality 42.0%† 28.3% 18.0%‡ *p(cid:3)0.04vsdobutamine. †p(cid:3)0.02vsplacebo. ‡p(cid:3)0.0001vsdobutamineand0.03vsplacebo. Adapted from Program and abstracts of the European Society of Cardiology, Heart FailureUpdate200440andEurJHeartFail.41 compensate when intravenous inodilator infusions are compared with placebo. The CASINO trial suggests that stopped, and they cannot be weaned off or switched to an short-term treatment with dobutamins is associated with oral agent. In such cases, patients may need to be on con- increased postdischarge mortality. tinuous intravenous infusions. This is usually done on an TheongoingSurvivalofPatientswithAcuteHeartFail- outpatient basis. It has also been proposed to use intermit- ure in Need of Intravenous Inotropic Support (SURVIVE) tent inodilator treatment to prevent rehospitalization. This trial will further analyze the effects of levosimendan com- infusionscheduleinvolvesintermittentintravenoustherapy, pared with those of dobutamine on mortality during 180 usually given as a 4- to 6-hour pulse infusion for several days after the start of treatment.42 days per week or as a single 24- to 72-hour infusion once Milrinone:Milrinone was approved for short-term in- weekly. travenous use in the late 1980s. Amrinone, the parent drug ofmilrinone,however,hashadlimitedusebecauseithasa 10% rate of thrombocytopenia caused by reversible bone Short-Term Use of Inodilator Treatment marrow suppression. As mentioned before, oral milrinone Dopamine and dobutamine:There are no randomized, as a continuous treatment has been shown to increase mor- controlledtrialsstudyingtheeffectsofshort-termdopamine tality.43 Its intravenous use in the acute setting has been infusion. Liang and associates37 studied the effects of con- studiedinafewrandomizedcontrolledtrials.Thelargestof tinuous infusion of dobutamine for 72 hours in 15 patients thesetrialsistheOutcomesofProspectiveTrialofIntrave- withNYHAclassIIItoIVHFwithafollow-upperiodof4 nous Milrinone for Exacerbations of Chronic Heart Failure weeks. No deaths were observed in this 4-week period. (OPTIME-CHF).4,44Mostofthecontrolledtrials,including Maximalexercisetimeandleftventricularejectionfraction OPTIME-CHF, evaluated the effects of short-term use of (LVEF) increased significantly in the dobutamine group. milrinone (Table 2).4,44–47 NYHA functional class improved in 6 of 8 patients in the The OPTIME-CHF investigators44 randomized 949 pa- treatment group compared with 2 of 7 control patients. tients(meanage,65years)admittedwithanexacerbationof Recentrandomizedtrialshavecomparedtheeffectsofa systolic HF with NYHA class III to IV HF and an LVEF short-term intravenous infusion of dobutamine with levosi- (cid:2)0.40(meanLVEF,0.23)tostudytheeffectofshort-term mendan, a new calcium sensitizer and ATP-dependent po- milrinoneinfusion(48to72hours)ontheprimaryoutcome: tassiumchannelopener(seealsothearticlebyMebazaaand cumulative days of hospitalization within 60 days of ran- colleagues38 in this supplement). The Levosimendan Infu- domization (the period with the highest risk of rehospital- sion Versus Dobutamine (LIDO) study demonstrated the ization48). They also studied the effects on secondary out- acutehemodynamicbenefitsoflevosimendan(loadingdose of 24 (cid:4)g/kg followed by an infusion of 0.1 (cid:4)g/kg per min comes,includingadverseeventsandmortality.Patientswho for 24 hours) compared with dobutamine (started with a werejudgedtoneedinodilatortherapywereexcludedfrom continuous infusion of 5 (cid:4)g/kg per min) in patients with the study (eg, for shock or severe hypotension) as well as severe low-output HF.39 In addition, levosimendan was as- those who had myocardial ischemia in the last 3 months, sociated with a significantly lower all-cause mortality and atrial fibrillation with poor rate control ((cid:1)110 beats per readmission rate at 180 days. minute), or sustained ventricular tachycardia or ventricular In the Calcium Sensitizer or Inotrope or None in Low- fibrillation. The study concluded that there were no signif- Output Heart Failure Study (CASINO), dobutamine was icantdifferencesbetweenthetreatmentandplacebogroups associated with lower 6-month survival compared with le- for the number of days hospitalized within the 60-day pe- vosimendanorplaceboinpatientswithdecompensatedlow- riod, the number of rehospitalizations, the length of initial output HF (Table 1).40,41 Moreover, this trial demonstrated stay, in-hospital mortality, or 60-day mortality (Table 3). a survival benefit associated with levosimendan treatment Clinical status measured by an HF score was also similar Bayrametal/ReassessmentofDobutamine,Dopamine,andMilrinoneintheManagementofAHFS 51G Table2 Short-term(acute)infusions:milrinoneversusplacebotrials Trial Milrinone Comparison Patient Number Follow- Outcome Population up Andersonetal 50(cid:4)g/kg Placebo NYHAclass 31 1hr Milrinonecausedsignificantincreasesin 198746,199145 loadingdose III–IVwith CI(41%)andSV(32%)and followedby CI(cid:2)2.5 decreasesinPCWP(25%),SVR infusionwith L/min/m2or (24%),andMAP(5%)at1hrof 0.5(cid:4)g/kg/min PCWP infusion. (cid:4)1hr (cid:1)15mmHg Seinoetal,199647 50(cid:4)g/kg Placebo Patientswith 52 1hr 37%decreaseinPAOP,39%decrease loadingdose acuteheart inRAP,31%increaseinCI,and21% followedby failurewith increaseinSVat15mincompared continuous PCWP withdecreasedCIat60minandno infusionwith (cid:1)18mmHg othersignificantchangesinplacebo 0.5(cid:4)g/kg/min group.Subjectivesymptomsalso for6hr improvedcomparedwithno improvementinplacebo.16%rateof ventriculararrhythmiasinmilrinone group. Cuffeetal,200244 48–72-hr Salineplacebo NYHAclass 951 2mo Nosignificantdifferenceinnumberof infusionwith III–IV;mean dayshospitalized,in-hospital 0.5(cid:4)g/kg/min LVEF(cid:3)0.23 mortality,60-daymortality,or compositeincidenceofdeathor re-admissions. Felkeretal,20034 48–72-hr Salineplacebo NYHAclass 951 2mo Milrinone-treatedpatientswithischemic infusionwith III–IV;mean heartdiseasetendedtohaveworse 0.5(cid:4)g/kg/min LVEF(cid:3)0.23 outcomesforthecompositeofdeath andrehospitalizations. CI (cid:3) cardiac index; LVEF (cid:3) left ventricular ejection fraction; MAP (cid:3) mean arterial pressure; NYHA (cid:3) New York Heart Association; PAOP (cid:3) pulmonaryarteryopenpressure;PCWP(cid:3)pulmonarycapillarywedgepressure;RAP(cid:3)rightatrialpressure;SV(cid:3)strokevolume;SVR(cid:3)systemicvascular resistance. Table3 ResultsfromtheOutcomesofProspectiveTrialofIntravenousMilrinoneforExacerbationsofChronicHeartFailure(OPTIME-CHF)4 Outcome Placebo Milrinone pValue (n(cid:3)472) (n(cid:3)477) Cardiovascularhospitalizationwithin60days,meandays 12.5(cid:5)14 12.3(cid:5)14 0.71 Deathwithin60days 8.9% 10.3% 0.41 Deathorreadmissionwithin60days 35.3% 35.0% 0.92 Treatmentfailuresduringtheinfusionperiod 9.2% 20.6% (cid:2)0.001 Newatrialfibrillationorflutterduringindexhospitalization 1.5% 4.6% 0.004 Sustainedhypotensionduringindexhospitalization* 3.2% 10.7% (cid:2)0.001 *Definedasasystolicbloodpressure(cid:2)80mmHgfor(cid:1)30minutes,requiringintervention. AdaptedfromJAMA.44 between the 2 groups, although patients treated with milri- termintravenousmilrinonetreatmentindecompensatedpa- none subjectively reported feeling better at 30 days com- tients with HF.4 A total of 485 patients had ischemic HF pared with the placebo group. The 2 groups, however, (defined as prior history of bypass grafting, percutaneous differed in the treatment failures caused by adverse events coronary intervention, or myocardial infarction [MI]) com- within 48 hours. There were more incidents of sustained pared with 464 patients in the nonischemic group. In each hypotension, atrial fibrillation, atrial flutter, ventricular group,approximately50%ofthepatientswerefoundtobe tachycardia, and ventricular fibrillation in the treatment randomizedinitiallytomilrinone.Thestudyconcludedthat group.Theresultsfromthisstudydonotsupporttheuseof theresponsetomilrinonewasdifferentintheischemicand short-term milrinone infusion in decompensated patients nonischemic groups. Patients with nonischemic HF bene- who do not present with hypotension resulting from a low fited from short-term use of milrinone. The composite of cardiac output. deathorrehospitalizationat60dayswassignificantlylower The OPTIME-CHF investigators retrospectively evalu- in the treatment group compared with placebo (28% vs ated the outcomes of the study to assess the interaction 35%, p (cid:3) 0.01), as well as the in-hospital mortality rate between HF etiology (ischemic vs nonischemic) and short- (2.6% for milrinone compared with 3.1% for placebo, p (cid:3) 52G TheAmericanJournalofCardiology(www.AJConline.org) Vol96(6A) September19,2005 Figure1.Kaplan-Meiersurvivalcurvesforin-hospitalsurvivalto60daysbyheartfailureetiologyandtreatmentassignmentinaposthocanalysisofthe OutcomesofProspectiveTrialofIntravenousMilrinoneforExacerbationsofChronicHeartFailure(OPTIME-CHF).(AdaptedfromJAmCollCardiol.4) 0.04). Mortality at 60 days was similar between the treat- require inodilator treatment as judged by their physicians. mentandplacebogroups.Thetotalnumberofhospitaldays Nonetheless, data from the trial indicated that patients in tendedtobelowerinthemilrinone-treatedgroupcompared this trial had severe HF, with event rates up to 35% within withtheplacebogroup(10.9daysvs12.6days,p(cid:3)0.055). 60 days after discharge.44 Regarding the reanalysis of the Incontrast,theischemicgroupwasadverselyaffectedby OPTIME-CHF study outcomes for ischemic versus non- short-termintravenousmilrinonetreatment.4Themilrinone ischemicetiologyofHF,itshouldberememberedthatthis treatment group trended toward prolonged hospitalizations is a retrospective study and can only be used to derive a and increased mortality. Days hospitalized at 60 days was hypothesis, not a conclusion.4,44 13.6 for treated patients versus 12.4 days for placebo pa- Numerous studies compared milrinone with dobutamine tients (p (cid:3) 0.055). The composite of death or rehospital- asanalternativetoreplacedobutamineintheacutesetting. izationat60dayswassignificantlygreaterinthemilrinone A list of the randomized, controlled trials comparing the 2 group (42% compared with 36% for placebo, p (cid:3) 0.01). agents is shown in Table 4.49–52 All of these trials studied In-hospital mortality was also significantly higher in the short-term infusion of dobutamine and milrinone, whereas treatment group (Figure 1), whereas 60-day mortality rates in the study by Aranda and coworkers,53 the infusion was were similar. continued until patients received cardiac transplant. The Anderson,45 Anderson and colleagues,46 and Seino and follow-up periods were brief and mostly ended with com- associates47 also studied the effects of short-term use of pletion of the infusion. Thus, no data were available com- intravenous milrinone. However, they analyzed data only paring long-term effects on morbidity or mortality. It is for the 1-hour period after infusion and did not analyze difficult to reach a common conclusion from these trials long-termmortalityorworseningHF.Theyfoundthatmil- because the patient population in each trial varied broadly: rinoneprovidedsymptomaticreliefcomparedwithplacebo. trials studied stable patients with HF,49,50 patients post- However, there was also a tendency toward increased ven- MI,51 patients after cardiac surgery,52 and patients waiting triculararrhythmiasassociatedwiththeuseofmilrinonein for cardiac transplantation.53 Overall, in these trials both both studies. Transient occurrence of ventricular arrhyth- milrinoneanddobutamineseemedtobereasonableoptions mias was observed in 16% and 12.2% of the milrinone- to be used in the acute setting. Biddle and colleagues49 treated patients in the placebo-controlled, double-blind foundthatsupraventriculararrhythmiasandsinustachycar- studybySeinoandassociates47andinthemulticenterstudy dia occurred more frequently in the dobutamine group. In by Anderson45 and Anderson and colleagues.46 So far, OP- thisstudy,nonsustainedventriculartachycardiaoccurredin TIME-CHF investigators provided the largest randomized 2 patients in each group and resolved spontaneously. Also, controlled trial and raised questions about the beneficial themilrinonegrouphad1patientwithventriculartachycar- effects of short-term infusion of milrinone in decompen- dia requiring cardioversion and 1 patient with ventricular sated patients with HF, especially in the presence of an fibrillation. Ventricular arrhythmias tended to occur in pa- ischemicetiology.However,itisimportantthatthepatients tientsreceivinglargerbolusesofmilrinone.However,given in OPTIME-CHF were not critically ill in that they did not the small number of patients studied in these trials, larger Bayrametal/ReassessmentofDobutamine,Dopamine,andMilrinoneintheManagementofAHFS 53G Table4 Short-term(acute)infusions:milrinonevsdobutaminetrials Trial Milrinone Dobutamine Patient N Follow-up Outcome Population Biddleetal 50or75(cid:4)g/kg Incrementaldoses NYHAclass 79 48hr Nodifferenceinhemodynamiceffectsbetween (1987)49 bolusthen of2.5–15(cid:4)g/ III–IV groups:SVincreased,HRincreased,SVR Openlabel 0.5–1(cid:4)g/kg/ kg/min(cid:4)48hr (stablefor decreased,andPCWPdecreasedsimilarlyin mininfusion (cid:1)2wk bothgroups. (cid:4)48hr before study) Eichhornetal 50(cid:4)g/kgbolus 2.5–15(cid:4)g/kg/min NYHAclass 14 During 24%increaseinCIfrombaselineinbothgroups; (1987)50 then0.5(cid:4)g/ (doseadjusted III–IV hemodynamic increaseinRVsystolicperformance. kg/min toachieveequal and SignificantRVafterloadandPAESPreduction increasesin radionuclide onlyinmilrinonegroup. CO) recordings Karlsbergetal 50(cid:4)g/kgbolus 24-hrinfusionof Within12hr 33 24hr CriteriafordecreaseinMPCWPweremetby (1996)51 then24-hr 2.5–15(cid:4)g/kg/ to5days 94%ofthemilrinone-treatedpatientsand57% Openlabel infusionof min(titratedup afteracute ofthedobutamine-treatedpatients(p(cid:3)0.03). 0.25–0.75 until(cid:1)30% MI MaximalreductioninMPCWPwasgreaterfor (cid:4)g/kg/min increaseinCI themilrinone(53.2%vs31%,p(cid:3)0.01).Both (titratedup or(cid:1)25% improvedglobalEF. similarto decreasein dobutamine) MPCWP) Fenecketal 50(cid:4)g/kgbolus 10–20(cid:4)g/kg/min Patientswith 120 4hr DobutaminegrouphadgreaterincreasesinCI, (2001)52 then0.5(cid:4)g/ infusion(cid:4)4hr lowCO MAP,andLVstrokeworkindex.Milrinone Openlabel kg/min after grouphadgreaterdecreasesinMPCWP. infusion(cid:4) cardiac Dobutaminegrouphadhigherincidencesof 4hr surgery hypertensionandatrialfibrillation;milrinone grouphadhigherincidenceofsinus bradycardia. CI(cid:3)cardiacindex;CO(cid:3)cardiacoutput;EF(cid:3)ejectionfraction;HR(cid:3)heartrate;LV(cid:3)leftventricle;MAP(cid:3)meanarterialpressure;MI(cid:3)myocardial infarction;MPCWP(cid:3)meanpulmonarycapillarywedgepressure;NYHA(cid:3)NewYorkHeartAssociation;PAESP(cid:3)pulmonaryarteryend-systolicpressure; PCWP(cid:3)pulmonarycapillarywedgepressure;RV(cid:3)rightventricular;SV(cid:3)strokevolume;SVR(cid:3)systemicvascularresistance. randomized controlled trials are needed to conclude which Intermittent Use of Inodilator Treatment drug is better in which group of patients. No randomized, controlled studies have been designed to Concomitant use of milrinone and (cid:1)-blockers:The study the effects of using intermittent infusions of dopa- mine.Arandomized,controlledtrial(theRandomizedOut- increase in mortality associated with inodilator therapy patient Milrinone Evaluation [ROME] trial) studying the hasbeenattributedtoaproarrhythmiceffectandtodirect effects of intermittent outpatient infusions of milrinone has myocyte toxicity with acceleration of disease progres- been terminated after enrollment of approximately 100 pa- sion.54,55This toxicity may be related to cAMP-mediated calcium overload.56,57 (cid:2)-Blockers have been shown to tients, and no data on the results are available yet.67 All of the randomized, controlled trials retrieved in our search attenuate these changes at a molecular and cellular analyzed intermittent infusions of dobutamine (Ta- level.58,59 For these and other reasons, these agents may ble 5).68–73 be ideal in attenuating the undesirable side effects of inodilators.60 Phosphodiesterase inhibitors, such as mil- Dobutamine:We identified 6 randomized, controlled rinone, would be expected to retain their positive inotro- trials that analyzed the effects of intermittent infusions of pic and vasodilator effects in the presence of a (cid:2)-blocker dobutamine.68–73 A review of the outcomes supports a ten- because their site of action is beyond the (cid:2)-adrenergic dency for symptomatic improvement68,69,71 and increased receptor.61 Several studies demonstrated that phosphodi- exercisetolerance68–72withdobutaminecomparedwithpla- esterase inhibitors, in contrast to dobutamine and dopa- cebo. The Dobutamina nell’Insufficienza Cardiaca Estrema mine, have continued positive inotropic effects in pa- (DICE)trial,however,foundnoimprovementinfunctional tients with advanced HF receiving chronic (cid:2)-blocker status.72Therewasanonsignificanttrendtowarddecreased therapy.62,63 Thus, the addition of a (cid:2)-blocker to a phos- hospitalizations in the DICE trial,72 whereas Elis and asso- phodiesterase inhibitor would be expected to attenuate ciates73 found no difference in the number of hospitaliza- the negative inotropic side effects of the former and the tions between groups at 6 months. Other prospective trials long-term adverse effects of the latter.64–66 did not provide data on the number of hospitalizations. 54G TheAmericanJournalofCardiology(www.AJConline.org) Vol96(6A) September19,2005 Mortality data were provided in 5 of the prospective stud- who really need the continuous infusions would not be ies.68–70,72,73 Adamopoulos and coworkers71 reported no enrolled in placebo-controlled, randomized trials. Indeed, deathsineithergroup.Mortalitywasincreasedinthetreat- there are no data from randomized, controlled trials study- mentgroupsinthetrialbyDiesandcolleagues,69whichwas ing the effects of continuous administration of intravenous stopped because of increased mortality in the dobutamine inodilator drugs prospectively compared with placebo ef- group. In the dobutamine group, death was more common fects. Reports in the literature indicate that the use of con- amongpatientswith(cid:1)4episodesofventriculartachycardia tinuous inodilator treatment has a significant impact on per day at baseline, although dobutamine did not seem to qualityoflifeandisassociatedwithanincreasedmortality increase the frequency of arrhythmias. The study by Elis rate. In the past, several large-scale trials were designed to and associates73 and the DICE trial72 did not find a signif- studytheeffectsoflong-termoralinodilatoruseinHFand icant difference in mortality between the dobutamine and showed increased mortality with these agents.43,74–76 The placebo groups (3 of 19 in the placebo group vs 5 of 19 in Prospective Randomized Milrinone Survival Evaluation the dobutamine group). However, in the DICE trial, 2 pa- (PROMISE) analyzed 1,088 patients with severe chronic tientsinthedobutaminegroupunderwentcardiactransplan- HF (NYHA class III or IV). Compared with placebo, mil- tation and 1 patient discontinued the protocol because of rinone increased hospitalizations, mortality from all causes severeventriculararrhythmias.Inthistrial,dobutaminewas by 28%, and cardiovascular mortality by 34%.43 This in- not associated with an increased number of ventricular ar- creaseinmortalitywasparticularlyevidentinpatientswith rhythmias. No adverse effects on mortality were observed verysevereHForclassIVHF.Thisfindingarguesagainst by Leier and coworkers68 or Erlemeier and colleagues70 (1 the common belief that these agents are most useful for deathin10patientsintheplacebogroupvs1deathin10in patients with the most advanced stage of HF. the dobutamine group). A meta-analysis by Thackray and Other agents that have been studied are pimobendan, a colleagues5 included 6 trials37,69,70,72,73 and calculated an phosphodiesterase inhibitor with calcium-sensitizing prop- oddsratioof1.5(95%confidenceinterval,0.51to3.92)for erties74;ibopamine,anoraldopaminergicagonistwithrenal all-causemortalityinthedobutaminegroupcomparedwiththe and peripheral vasodilatory effects75; and vesnarinone, a controlgroup.Itischallengingtoderiveconclusionsbasedon phosphodiesterase inhibitor with effects on sodium ion theresultsofthesecontrolledtrialsforseveralreasons:(1)the channels.76 All 3 agents increased mortality when used in smallnumbersofpatientsenrolledineachofthesetrialsonly patients with advanced HF. Vesnarinone appeared to im- allowdetectionoflargedifferencesbetweenthetreatmentand provethequalityoflifeattheexpenseofincreasingtherisk controlgroups;(2)theinfusionpatternsofdobutaminevaried of death.76 widelybetweendifferenttrials(eg,theaveragerateofinfusion In contrast to oral inodilator agents, no large-scale trials byDiesandcolleagues69washigh[8.1(cid:4)g/kgpermin],which have been designed to study the effects of long-term intra- may have played a role in the increased mortality associated venous inodilator therapy. There are no randomized con- withdobutamine);(3)patientpopulationsstudiedinthesetrials trolledtrialslookingattheeffectsofcontinuousinfusionsof werenotalwayscomparable(Liangandassociates37excluded dopamine.Forintravenoususeofmilrinone,Arandaetal53 patientswithischemicheartdisease,whereasElisandassoci- studied 36 patients awaiting cardiac transplantation who ates,73 Erlemeier and colleagues,70 and the DICE trial72 en- wererandomizedtoreceiveeithermilrinoneordobutamine, rolledpatientswithCADorischemicHF);and(4)follow-up andfollowedthemuntildeath,transplantation,orplacement durationwasvariedbetweentrials.However,untilmorecon- ofmechanicalcardiacsupport.Nodifferencebetweenthe2 clusive trials are conducted analyzing the safety of using do- groupswasobservedinrightheartdynamics,death,orneed butamineinHF,thisinodilatoragentshouldbeavoidedwhen- for other inodilator/vasodilator treatment or for mechanical everasaferoptionisavailable. cardiac support.53 Similar to other inodilator agents, there are no data from prospective, randomized controlled trials Continuous Inodilator Treatment on chronic intravenous infusion of dobutamine. A retro- spective analysis of the Flolan International Randomized Many patients with advanced HF are hospitalized because SurvivalTrial(FIRST)istheonlysourceofdatalookingat ofexacerbatedofcongestivesymptoms.Theuseofoptimal chronicinfusionofthisagent.6Cautionmustbeexercisedin HFtherapydoesnotsufficeforsymptomaticreliefinsome interpreting the results of this post hoc analysis because a ofthesepatients,andintravenousinodilatortherapyiscom- higher proportion of the dobutamine patients had NYHA monly used. Of patients who are started on intravenous class IV HF. inodilators for refractory HF symptoms, some cannot be successfullyweanedoffafterbeingstabilizedclinicallyand Dobutamine:In FIRST, 471 patients with NYHA class become dependent on inodilator therapy. In this setting, III to IV HF were enrolled initially to study the effects of continuousinodilatorinfusionsareusedeitherasabridgeto conventionaltherapywithandwithoutintravenousepopro- cardiac transplantation or for palliative purposes. At this stenol. The results of the study showed a trend toward stage,patientshavenootheroption,regardlessoftheeffect increased mortality rate in the epoprostenol group.77 The of continuous inodilator infusions on survival. Thus, those data from this trial were later analyzed to compare the Bayrametal/ReassessmentofDobutamine,Dopamine,andMilrinoneintheManagementofAHFS 55G Table5 Intermittentinfusions:dobutamineversusplacebotrials Trial Dobutamine Control Patient Number Follow-up Outcome Population (NYHAclass) Leieretal IVinfusionfor4hr Matched III–IV 26 24wk NosignificantchangeinCIorrestingLVEF. (1982)68 weekly(cid:4) control Improvedfunctionalclassification(p(cid:2) 24wk group 0.05);increasedexercisetolerance(p(cid:2) 0.05).2of15diedindobutaminegroupvs 1of11incontrolgroup. Diesetal IVinfusionfor48 Placebo III–IV, 60 8wk Increasedtreadmilltimes;improvedsymptom (1986)69 hr/wk(cid:4)24wk EF0.20(cid:5)0.11 scores.Increasedmortalityintreatment group(44%vs17%inplacebogroup). Erlemeieretal 8(cid:4)24-hrinfusions 5% IV 20 3daysafterlast Increasedexercisedurationontreadmilltest; (1992)70 overa4-wk dextrose infusion decreasedbodyweight.1deathintreatment periodwithat solution group(1/10)and1death(1/10)incontrol least3daysin group. between Adamopoulos IVinfusion4days/ Usual MostlyIII,EF 20 6wkafter Increasedexercisetoleranceat3and6wk; etal(1995)71 wk(cid:4)3wkto activity 0.23(cid:5)0.03 intervention increasedchronotropicresponsivenessto raiseHRto70%– only exercise;improvedsymptoms;increased 80%maximum (cid:2)-receptordensity.Noclinicallysignificant for30min/day arrhythmiasandnodeathsreported. Olivaetal Infusionfor48hr/ Optimal III–IV,EF 38 8wkforCI;6 Didnotimprovefunctionalstatus;non- (1999)72 wk(cid:4)6mo standard (cid:2)0.30 moforother significanttendencytowarddecreased treatment outcomes hospitalizations.Nonsignificanttrendto improveexercisetolerance.Noincreasein ventriculararrhythmias.Didnot significantlyincreasemortality. Elisetal 24-hrinfusionevery Placebo III–IV,EF0.30 19 Untildeathor Nodifferenceinnumberofhospitalizations (1998)73 2wk(cid:4)6wk (ischemia- Dec.1996 betweengroupsat6mo.Nosignificant thenevery3wk inducedHF) (survival differencebetweensurvivalcurvesat32 (cid:4)6mo analysisat32 mo(p(cid:3)0.7) mo) CI(cid:3)cardiacindex;EF(cid:3)ejectionfraction;HF(cid:3)heartfailure;HR(cid:3)heartrate;IV(cid:3)intravenous;LVEF(cid:3)leftventricularejectionfraction;NYHA (cid:3)NewYorkHeartAssociation. outcomes in 2 patient groups: patients who were receiving nousdobutaminetreatment,nottoshort-termorintermittent intravenous continuous dobutamine at the time of random- intravenous treatment. ization for the initial study versus patients who were not receiving dobutamine at the time of randomization.6 There were 391 patients in the no-dobutamine group and 80 pa- Indications for Inodilators in Current Guidelines tients in the dobutamine group. The median age, ratio of men to women, and etiology of HF were similar in the 2 The current guidelines on chronic HF from the American groups. However, more patients in the dobutamine group CollegeofCardiologyandtheAmericanHeartAssociation had NYHA class IV HF. The median dose of dobutamine accept the use of continuous intravenous inodilator infu- administeredwas9(cid:4)g/kgpermin(5to12(cid:4)g/kgpermin) sions for stage D patients (those with HF refractory to and the median duration of treatment was 14 days (7 to 52 therapy) as a palliative treatment or as a bridge to cardiac days).Thisstudyconcludedthatthedobutaminegrouphad transplantation,onlyafterallalternativeattemptstoachieve a higher occurrence of first events and a higher mortality stabilityhavefailed(classIIbrecommendation:usefulness/ rate compared with the no-dobutamine group. Caution is efficacy is less well established by evidence/opinion).78 warranted when interpreting these results, given the limita- These guidelines do not approve of using intermittent or tions of a retrospective study. It is not possible to identify continuous intravenous inodilator therapy in stage C pa- what proportion of the increased mortality was attributable tients(thosewithsevereHFwhoappeartorespondtoother to dobutamine versus the baseline characteristics of the therapies; long-term intermittent infusions of a positive in- dobutamine group. However, the investigators concluded odilator drug in these patients is considered a class III that even when the baseline differences were adjusted for, recommendation [conditions for which there is evidence thetreatmentgrouphada2-foldincreaseinmortalityrate.6 and/or general agreement that a procedure/therapy is not The results of this study apply only to continuous intrave- useful/effective and in some cases may be harmful]), or in 56G TheAmericanJournalofCardiology(www.AJConline.org) Vol96(6A) September19,2005 stage D patients who can be successfully weaned from 6. O’ConnorCM,GattisWA,UretskyBF,AdamsKFJr,McNultySE, inodilator therapy (routine intermittent infusions in these GrossmanSH,McKennaWJ,ZannadF,SwedbergK,GheorghiadeM, CaliffRM.Continuousintravenousdobutamineisassociatedwithan patients are considered a class III recommendation). Con- increasedriskofdeathinpatientswithadvancedheartfailure:insights versely,theEuropeanSocietyofCardiologyguidelinessug- fromtheFlolanInternationalRandomizedSurvivalTrial(FIRST).Am gest the use of inodilator agents in the presence of periph- HeartJ1999;138:78–86. eral hypoperfusion (hypotension, decreased renal function) 7. FonarowGC,YancyCW,HeywoodJT,fortheADHEREScientific with or without congestion or pulmonary edema refractory Advisory Committee, Study Group, and Investigators. Adherence to to diuretics and vasodilators at optimal doses (class IIa heartfailurequality-of-careindicatorsinUShospitals:analysisofthe ADHEREregistry.ArchInternMed2005;165:1469–1477 recommendation: weight of evidence/opinion is in favor 8. AdamsKFJr,DeMarcoT,BerkowitzR,ChandS.Inotropeuseand of usefulness/efficacy).79 negativeoutcomesintreatmentofacuteheartfailureinpatientswith preserved systolic function: data from the ADHERE database [ab- stract].Circulation2003;108:IV-695. 9. 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