SUMMARY OF PRODUCT CHARACTERISTICS 1. NAME OF THE MEDICINAL PRODUCT RocuroniumKabi10mg/mlsolutionforinjection/infusion 2. QUALITATIVE AND QUANTITATIVE COMPOSITION Eachmlofsolutionforinjection/infusioncontains10mgrocuroniumbromide. Eachvialwith2.5mlcontains25mgrocuroniumbromide. Eachvialwith5mlcontains50mgrocuroniumbromide. Eachvialwith10mlcontains100mgrocuroniumbromide. Forafulllistofexcipients,seesection6.1.

3. PHARMACEUTICAL FORM Solutionforinjection/infusion Clear,colourlesstopalebrownishyellowsolution pHofthesolution:3.8to4.2 Osmolarity:271–312mOsmol/kg. 4. CLINICAL PARTICULARS 4.1 Therapeutic indications Rocuronium bromide is indicated as an adjunct to general anaesthesia to facilitate tracheal intubation during routine and rapid sequence induction, to provide skeletal muscle relaxation, during . It is also indicated as an adjunct in the intensive care unit (ICU) (e.g..to facilitate intubation), for short termuse. Seealsosection4.2and5.1. 4.2 Posology and method of administration Aswithotherneuromuscularblockingagents,thedosageofrocuroniumbromide should be individualised in each patient. The method of anaesthesia and the expecteddurationofsurgery,themethodofsedationandtheexpectedduration ofmechanicalventilation,thepossibleinteractionwithothermedicinalproducts that are administered concomitantly and the condition of the patient should be taken into account when determining the dose. The use of an appropriate neuromuscular monitoring technique is recommended for the evaluation of the neuromuscularblockandrecovery. Inhalational anaesthetics potentiate the neuromuscular blocking effects of rocuronium bromide. This potentiation becomes clinically relevant during the courseofanaesthesiawhenacertaintissueconcentrationofthevolatileagents isreached.Consequently,adjustmentsshouldbemadebyadministeringsmaller maintenancedosesatlessfrequentintervalsorbyusinglowerinfusionratesof

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rocuronium bromide during long lasting procedures (longer than 1 hour) under inhalationalanaesthesia. Inadultpatientsthefollowingdosagerecommendationsmayserveasageneral guidance for tracheal intubation and muscle relaxation for short to long lasting surgicalproceduresandforuseintheintensivecareunit. Thismedicinalproductisforsingleuseonly.

Surgical Procedures Trachealintubation The standard intubating dose during routine anaesthesia is 0.6 mg rocuronium bromide per kg body weight, which results in adequate intubation conditions within60secondsin nearlyallpatients.Adoseof1.0mgrocuroniumbromide perkgbodyweightisrecommendedforfacilitatingtrachealintubationconditions duringrapidsequenceinductionofanaesthesia,afterwhichadequateintubation conditionsarealsoestablishedwithin60secondsinnearlyallpatients.Ifadose of 0.6 mg rocuronium bromide per kg body weight is used for rapid sequence inductionofanaesthesia,itisrecommendedtointubatethepatient90seconds afteradministrationofrocuroniumbromide. Maintenancedosage The recommended maintenance dose is 0.15 mg rocuronium bromide per kg bodyweight.Incaseoflongterminhalationalanaesthesiaitshouldbereduced to0.0750.1mgofrocuroniumbromideperkgbodyweight. Themaintenancedosesshouldbestbegivenwhentwitchheighthasrecovered to 25 % of control twitch height, or when 2 to 3 responses to trainoffour stimulation(TOF)arepresent. Continuousinfusion Ifrocuroniumbromideisadministeredbycontinuousinfusion,itisrecommended togivealoadingdoseof0.6mgrocuroniumbromideperkgbodyweightand, when the neuromuscular block starts to recover, to start administration by infusion.Theinfusionrateshouldbeadjustedtomaintaintwitchresponseat10 % of control twitch height or to maintain 1 to 2 responses to trainoffour stimulation. Inadultsunder intravenousanaesthesia, theinfusionraterequiredto maintain the neuromuscular block at this level ranges from 0.3 0.6 mg/kg/h. Under inhalationalanaesthesiatheinfusionraterangesfrom0.30.4mg/kg/h. Continuousmonitoringoftheneuromuscularblockisessentialsinceinfusionrate requirementsvaryfrompatienttopatientandwiththeanaestheticmethodused. Dosageinpregnantpatients InpatientsundergoingCaesareansection,itisrecommendedtoonlyuseadose of0.6mgrocuroniumbromideperkgbodyweight,sincea1.0mg/kgdosehas notbeeninvestigatedinthispatientgroup. Reversalofneuromuscularblockinducedbyneuromuscularblockingagentsmay beinhibitedorunsatisfactoryinpatientsreceivingmagnesiumsaltsfortoxemia of pregnancy because magnesium salts enhance neuromuscular blockade. Therefore,inthesepatientsthedosageofrocuroniumshouldbereducedandbe titratedtotwitchresponse.

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Dosageinpaediatricpatients For infants (28 days23 months) children (211 years) and adolescents (1217 years) the recommended intubation dose during routine anaesthesia and maintenance dose are similar to those in adults. For continuous infusion in pediatrics, the infusion rates, with exception of children, are the same as for adults.Forchildrenhigherinfusionratesmightbenecessary. For children the same initial infusion rates as for adults are recommended and this should be adjusted to maintain twitch response at 10% of control twitch height or to maintain 1 or 2 responses to trainoffour stimulation during the procedure. Theexperiencewithrocuroniumbromideinrapidsequenceinductioninpediatric patients is limited. Rocuronium bromide is therefore not recommended for facilitation tracheal intubation conditions during rapid sequence induction in pediatricpatients. There are no data to support recommendations for the use of rocuronium bromideinnewborninfants(01month). Dosageingeriatricpatientsandpatientswithhepaticand/orbiliarytractdisease and/orrenalfailure The standard intubation dose for geriatric patients and patients with hepatic and/orbiliarytractdiseaseand/orrenalfailureduringroutineanaesthesiais0.6 mg rocuronium bromide per kg body weight. A dose of 0.6 mg per kg body weight should be considered for rapid sequence induction of anaesthesia in patients in which a prolonged duration ofaction is expected however adequate conditions for intubation may not be established for 90 seconds after administration of rocuronium bromide. Regardless of the anaesthetic technique used,therecommendedmaintenancedoseforthesepatientsis0.0750.1mg rocuroniumbromideperkgbodyweight,andtherecommendedinfusionrateis 0.30.4mg/kg/h(seealsoContinuousinfusion). Dosageinoverweightandobesepatients When used in overweight or obese patients (defined as patients with a body weight of 30% or more above ideal body weight) doses should be reduced takingintoaccountabodymass.

Intensive care procedures Trachealintubation Fortrachealintubation,thesamedosesshouldbeusedasdescribedaboveunder surgicalprocedures. Administration

Rocuronium bromide is administered intravenously (i.v.) either as a bolus injection or as a continuous infusion (for further information see also section 6.6). 4.3 Contraindications Rocuronium bromide is contraindicated in patients with hypersensitivity to rocuroniumbromideortothebromideionortoanyoftheexcipients.

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4.4 Special warnings and precautions for use Rocuronium bromide should be administered only by an experienced staff familiar with the use of neuromuscular blocking agents. Adequate facilities and staffforendotrachealintubationandartificialventilationhavetobeavailablefor immediateuse. Since rocuronium bromide causes paralysis of the respiratory muscles, ventilatorysupportismandatoryforpatientstreatedwiththis activesubstance until adequate spontaneous respiration is restored. As with all neuromuscular blocking agents, it is important to anticipate intubation difficulties, particularly whenusedaspartofarapidsequenceinductiontechnique. As with other neuromuscular blocking agents, residual curarization has been reported for Rocuronium. In order to prevent complications resulting from residual curarization, it is recommended to extubate only after the patient has recovered sufficiently from neuromuscular block. Other factors which could causeresidualcurarizationafterextubationinthepostoperativephase(suchas druginteractionsorpatientcondition)shouldalsobeconsidered.Ifnotusedas part of standard clinical practice, the use of a reversal agent should be considered,especiallyinthosecaseswhereresidualcurarizationismorelikelyto occur. Itisessentialtoensurethatthepatientisbreathingspontaneously,deeplyand regularlybeforeleavingthetheatreafteranaesthesia. Anaphylactic reactions (see above) can occur after the administration of neuromuscular blocking agents. Precautions for treating such reactions should always be taken. Particularly in the case of previous anaphylactic reactions to neuromuscularblockingagents,specialprecautionsshouldbetakensinceallergic crossreactivitytoneuromuscularblockingagentshasbeenreported. Dose levels higher than 0.9 mg rocuronium bromide per kg body weight may increasetheheartrate;thiseffectcouldcounteractthebradycardiaproducedby otheranaestheticagentsorbyvagalstimulation. In general, following long term use of muscle relaxants in the ICU, prolonged paralysis and/or skeletal muscle weakness has been noted. In order to help precludepossibleprolongationofneuromuscularblockageand/oroverdose,itis stronglyrecommendedthatneuromusculartransmissionismonitoredthroughout the use of muscle relaxants. In addition, patients should receive adequate analgesiaandsedation.Furthermore,musclerelaxantsshouldbetitratedtothe effectintheindividualpatient.Thisshouldbedonebyorunderthesupervision of experienced clinicians who are familiar with the effects and with appropriate neuromuscularmonitoringtechniques. Because rocuronium bromide is always used with other agents and because of thepossibilityoftheoccurrenceofmalignanthyperthermiaduringanaesthesia, evenintheabsenceofknowntriggeringagents,cliniciansshouldbefamiliarwith theearlysigns,confirmatorydiagnosisandtreatmentofmalignanthyperthermia prior to the start of any anaesthesia. In animal studies it was shown that rocuroniumbromideisnotatriggeringfactorformalignanthyperthermia. Myopathy has been reported after longterm concurrent use of non depolarisatingneuromuscularblockersandconticosteroids.Thecoadministration periodshouldbereducedtobeasshortaspossible(seesection4.5). Rocuronium should only be administered after full recovery from the neuromuscularblockadecausedbysuxamethonium.

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The following conditions may influence the and/or pharmacodynamicsofrocuroniumbromide: Hepaticand/orbiliarytractdiseaseandrenalfailure Rocuroniumbromideisexcretedinurineandbile.Therefore,itshouldbeused withcautioninpatientswithclinicallysignificanthepaticand/orbiliarydiseases and/orrenalfailure.Inthesepatientgroupsprolongationoftheeffecthasbeen observedwithdosesof0.6mgrocuroniumbromideperkgbodyweight. Prolongedcirculationtime Conditions associated with prolonged circulation time such as cardiovascular diseases,oldageandanoedematousstateresultinginanincreasedvolumeof distribution,maycontributetoasloweronsetoftheeffect. Neuromusculardisease Like other neuromuscular blocking agents, rocuronium bromide should be used with extreme caution in patients with a neuromuscular disease or after poliomyelitis since the response to neuromuscular blocking agents may be considerably altered in these cases. The magnitude and direction of this alteration may vary widely. In patients with myasthenia gravis or with the myasthenic(EatonLambert)syndrome,smalldosesofrocuroniumbromidemay have profound effects and rocuronium bromide should be titrated to the response. Hypothermia In surgery under hypothermic conditions, the neuromuscular blocking effect of rocuroniumbromideisincreasedandthedurationprolonged. Obesity Like other neuromuscular blocking agents, rocuronium bromide may exhibit a prolonged duration and a prolonged spontaneous recovery in obese patients, whentheadministereddosesarecalculatedonactualbodyweight.Burns Patients with burns are known to develop resistance to nondepolarizing neuromuscular blocking agents. It is recommended that the dose is titrated to theresponse. Conditionswhichmayincreasetheeffectsofrocuroniumbromide Hypokalaemia (e.g. after severe vomiting, diarrhoea or diuretic therapy), hypermagnesaemia, hypocalcaemia (after massive transfusions), hypoproteinaemia,dehydration,acidosis,hypercapniaandcachexia. Severeelectrolytedisturbances,alteredbloodpHordehydrationshouldtherefore becorrectedwhenpossible. Thismedicinalproductcontainslessthan1mmolsodium(23mg)perdose,i.e. essentially‘sodiumfree‘.

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4.5 Interaction with other medicinal products and other forms of interaction The following medicinal products have been shown to influence the magnitude and/ordurationoftheeffectofnondepolarizingneuromuscularblockingagents: Increasedeffect  Halogenatedvolatileanaesthetics  High doses of: thiopental, methohexital, , fentanyl, gammahydroxybutyrate,andpropofol  Othernondepolarizingneuromuscularblockingagents.  Prioradministrationofsuxamethonium(seesection4.4) .  LongtermconcomitantuseofcorticosteroidsandRocuroniumintheICUmay result in prolonged duration of neuromuscular block or myopathy (see sections4.4and4.8). Othermedicinalproducts  Antibiotics:aminoglycosides,lincosamides(e.g.lincomycinandclindamycin), polypeptide antibiotics, acylaminopenicillin antibiotics, tetracyclines, high dosesofmetronidazole.  diuretics, thiamine, MAO inhibiting agents, quinidine and its isomer , protamine, adrenergic blocking agents, magnesium salts, calcium channel blocking agents and lithium salts and local anaesthetics (lidocaine i.v., bupivacaineepidural). Decreasedeffect  ,edrophonium,pyridostigmine,aminopyridinederivatives  Priorchronicadministrationofcorticosteroids,phenytoinorcarbamazepine  Noradrenaline, azathioprine (only transient and limited effect), theophylline, calciumchloride,potassiumchloride  proteaseinhibitors Variableeffect Administation of other nondepolarizing neuromuscular blocking agents in combination with rocuronium bromide may produce attenuation or potentiation of the neuromuscular block, depending on the order of administration and the neuromuscularblockingagentused. Suxamethonium given after the administration of rocuronium bromide may produce potentiation or attenuation of the neuromuscular blocking effect of rocuroniumbromide.

Effectofrocuroniumonotherdrugs Combinedusewithlidocainecouldresultinamoreinstanteffectoflidocaine. Recurarization has been reported after postoperative administration of: aminoglycoside, lincosamide, polypeptide and acylaminopenicillin antibiotics, quinidine,quinineandmagnesiomsalts(seesection4.4).

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4.6 Pregnancy and lactation Pregnancy There are very limited data on the use of rocuronium bromide during human pregnancy.Animalstudiesdonotindicatedirectorindirectharmfuleffectswith respect to reproductive toxicity. Rocuronium bromide should only be given to pregnant women when strictly necessary and the attending physician decides that the benefits outweigh the risks. Use of rocuronium bromide during caesareansectionatdosesof0.6mg/kgbodyweightdoesnoteffecttheApgar score,thefoetalmuscletoneorthecardiorespiratoryadaptation. From umbilical cord blood sampling it is apparent that only limited placental transferofrocuroniumbromideoccurs,whichdoesnotleadtotheobservationof clinicaladversereactionsinthenewborninfant. Note: doses of 1.0 mg/kg have been investigated during rapid sequence inductionofanaesthesia,butnotinCaesareansectionpatients. Lactation There are no human data on the use of rocuronium bromide during lactation. Othermedicinalproductsofthisclassshowlittleintobreastmilkand low resorption by the suckling child. Animal studies have shown excretion of rocuroniumbromideininsignificantamountsinbreastmilk. A decision on whether to continue/discontinue breastfeeding should be made taking into account the benefit of breastfeeding and the potential risk to the child. 4.7 Effects on ability to drive and use machines Rocuronium bromide has a major influence on the ability to drive and use machines . Itisnotrecommendedtousepotentiallydangerousmachineryorto drive a car during the first 24 hours after the full recovery from the neuromuscularblockingactionofrocuroniumbromide. 4.8 Undesirable effects Thefrequencyofundesirableeffectsisclassifiedintothefollowingcategories: Very ≥1/10 common Common ≥1/100to<1/10 Uncommon ≥1/1,000to<1/100 Rare ≥1/10,000to<1/1,000 Very rare <1/10,000 Not known cannotbeestimatedfromtheavailabledata

The most common undesirable effects are pain/reaction around injection site, changesinvitalfunctionsandprolongedneuromuscularblock.

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Immune system disorders Veryrare • Anaphylacticreactione.g.anaphylacticshock • Anaphylactoidreaction* • Hypersensitivity Nervous system disorders Veryrare • Paralysis Cardiac disorders Veryrare • Tachycardia Vascular disorders Veryrare • Hypotension • Circulatorycollapseandshock Respiratory, thoracic, and mediastinal disorders Veryrare • Bronchospasm Notknown • Apnoea • Respiratoryfailure

Skin and subcutaneous tissue disorders Veryrare • Rash,erythematousrash • Angioedema • Urticaria • Itching • Exanthema Musculoskeletal disorders Notknown • skeletalmuscleweakness • steroidmyopathy*(seesection4.4) General disorders and administration site conditions Verycommon • Injectionsitepain/reaction* Investigations Veryrare • Increasedhistaminelevel* Injury, poisoning and procedural complication Veryrare • Prolongedneuromuscularblock*

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*Additional information on adverse reactions: Anaphylactic reaction Severe anaphylactic reactions to neuromuscular blocking agents have been reported to be fatal in some cases. Due to the possible severity of these reactions, one should always assume that they may occur and take the necessaryprecautions. Local injection site reactions During rapid sequence induction of anaesthesia, pain on injection has been reported,especiallywhenthepatienthasnotyetcompletelylostconsciousness andparticularlywhenpropofolisusedastheinductionagent.Inclinicalstudies, pain on injection has been noted in 16% of the patients who underwent rapid sequence induction of anaesthesia with propofol and in less than 0.5% of the patients who underwent rapid sequence induction of anaesthesia with fentanyl andthiopental. Increased histamine level Since neuromuscular blocking agents are known to be capable of inducing histaminereleasebothlocallyandsystemically,thepossibleoccurrenceofitching anderythematousreactionatthesiteofinjectionand/orgeneralisedhistaminoid (anaphylactoid)reactionssuchasbronchospasmandcardiovascularchangese.g. hypotension and tachycardia should always be taken into consideration when administering these drugs. Rash, exanthema, urticaria, bronchospasm and hypotension have been reported very rarely in patients given rocuronium bromide. Inclinicalstudiesonlyaslightincreaseinmeanplasmahistaminelevelhasbeen observed following rapid bolus administration of 0.3 0.9 mg rocuronium bromideperkgbodyweight. Prolonged neuromuscular block The most frequent adverse reaction to nondepolarizing blocking agents as a classconsistsofanextensionoftheagent’spharmacologicalactionbeyondthe timeperiodneeded. Thismayvaryfrom skeletalmuscleweaknesstoprofound and prolonged skeletal muscle paralysis resulting in respiratory insufficiency or apnoea. 4.9 Overdose Intheeventofoverdoseandprolongedneuromuscularblock,thepatientshould continuetoreceiveventilatorysupportandsedation.Uponstartofspontaneous recovery an acetylcholinesterase inhibitor (e.g. neostigmine, edrophonium, pyridostigmine)shouldbeadministeredinadequatedoses.Whenadministration of an acetylcholinesterase inhibiting agent fails to reverse the neuromuscular effects of rocuronium bromide, artificial ventilation must be continued until spontaneousbreathingisrestored.Repeateddosagesofanacetylcholinesterase inhibitorcanbedangerous. In animal studies, severe depression of cardiovascular function, ultimately leadingtocardiaccollapse,didnotoccuruntilacumulativedoseof750xED 90 (135mgperkgbodyweight)wasadministered.

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5. PHARMACOLOGICAL PROPERTIES 5.1 Pharmacodynamic properties Pharmacotherapeuticgroup:musclerelaxants,peripherallyactingagents,other quaternaryammoniumcompounds. ATCcode:M03AC09 Pharmacodynamics Rocuronium bromide is an intermediate acting, nondepolarizing neuromuscular blocking agent with a fast onset, possessing all of the characteristic pharmacological actions of this class of medicinal products (curariform). It acts by competing for nicotinic cholinoceptors at the motor endplate. This action is antagonisedbyacetylcholinesteraseinhibitorssuchasneostigmine,edrophonium andpyridostigmine.

TheED 90 (doserequiredtoproduce90%depressionofthetwitchresponseof the thumb to stimulation of the ulnar nerve) during balanced anaesthesia is approximately0.3mgperkgbodyweight. Routinepractice Within 60 seconds after intravenous administration of adose of 0.6 mg rocuroniumbromideperkgbodyweight(2xED 90 underbalancedanaesthesia), adequateintubationconditionscanbeachievedinnearlyallpatients.In80%of thesepatientsintubationconditionsareratedexcellent.Within2minutesgeneral muscleparalysisadequateforanytypeofprocedureisestablished.Theclinical duration (the duration until spontaneous recovery to 25% of control twitch height) with this dose is 30 40 minutes. The total duration (time until spontaneousrecoveryto90%ofcontroltwitchheight)is50minutes.Themean time of spontaneous recovery of twitch response from 25 to 75 % (recovery index)afterabolusdoseof0.6mgrocuroniumbromideperkgbodyweightis14 minutes. Withlowerdosagesof0.30.45mgrocuroniumbromideperkgbodyweight(1

1½x2xED 90 ),theonsetoftheeffectisslowerandthedurationofactionis shorter(1326min).Afteradministrationof0.45mgrocuroniumbromideper kgbodyweight,acceptableintubationconditionsarereachedafter90seconds. Emergencyintubation During rapid sequence induction of anaesthesia under propofol or fentanyl/thiopental anaesthesia, adequate intubation conditions are achieved within 60 seconds in 93 % and 96% of the patients respectively, after administrationofadoseof1.0mgrocuroniumbromideperkgbodyweight.Of these,70%areratedexcellent.Theclinicaldurationwiththisdoseapproaches1 hour,atwhichtimetheneuromuscularblockcanbesafelyreversed Afteradministrationofadoseof0.6mgrocuroniumbromideperkgbodyweight, adequateintubationconditionsareachievedwithin60secondsin81%and75% of the patients during a rapid sequence induction technique with propofol or fentanyl/thiopental,respectively. Doses higher than 1.0 mg rocuronium bromide per kg body weight will not improve the intubation conditions appreciably; the duration of the effect, however,willbeprolonged.Doseshigherthan4xED 90 havenotbeenstudied.

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Intensivecare TheuseofrocuroniumintheIntensiveCareUnitwasstudiedintwoopenlabel trials. A total of 95 adult patients were treated with an initial dose of 0.6 mg rocuroniumbromideperkgbodyweight,followedbyacontinuousinfusionof0.2 0.5 mg/kg/h during the first hour of administration as soon as twitch height recoversto10%oruponreappearanceof1to2twitchestotrainoffour(TOF) stimulation.Thedosageswereindividuallytitrated.Inthefollowinghours,doses weredecreasedunderregularmonitoringoftheTOFstimulation.Administration foratimepe.riodofupto7dayshasbeeninvestigated. Adequateneuromuscularblockadewasachieved,butahighvariabilityinhourly infusion rates between patients and a prolonged recovery from neuromuscular blockadewasobserved. Thetimetorecoverofthetrainoffourratioto0.7isnotsignificantlycorrelated to the total duration of rocuronium infusion. After a continuous infusion for 20 hours or more the median (range) time between return of T2 to train of four stimulationandrecoveryofthetrainoffourratioto0.7variedbetween0,8and 12,5hours inpatientswithoutmultipleorganfailureand 1.2–25.5hours in patientswithmultipleorganfailure. Specialpopulations The mean time to effect after 0.6 mg/kg is shorter in infants and children compared to adults. The duration of effect is shorter in children compared to adults. Thedurationoftheeffectofmaintenancedosesof0.15mgrocuroniumbromide perkgbodyweight mightbesomewhatlongerunderand anaesthesia in geriatric patients and in patients with hepatic or renal disease (approximately 20 minutes) than in patients without impairment of excretory organ functions under intravenous anaesthesia (approximately 13 minutes). No cumulation of effect (progressive increase in duration of action) with repetitive maintenancedosesattherecommendedlevelhasbeenobserved. Cardiovascularsurgery In patients scheduled for cardiovascular surgery the most common cardiovascularchangesduringtheonsetofmaximumblockageafterreceivinga doseof 0.6 0.9 mg rocuronium bromide per kg body weight are a slight and clinically insignificant increase in heart rate up to 9% and an increase in mean arterialbloodpressureupto16%fromthecontrolvalues. Antagonists Administration of acetylcholinesterase inhibitors, such as neostigmine, pyridostigmineoredrophonium,antagonisestheactionofrocuroniumbromide.

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5.2 Pharmacokinetic properties After intravenous administration of a single bolus dose of rocuronium bromide, thetimecourseoftheplasmaconcentrationrunsinthreeexponentialphases.In normaladults,themean(95%Cl) eliminationhalflifeis73(6680)minutes,the (apparent) volume of distribution at steady state conditions is 203 (193214) ml/kgandtheplasmaclearanceis3.7(3.53.9)ml/kg/min. Theplasmaclearanceingeriatricpatientsandinpatientswithrenaldysfunction isslightlyreducedcomparedtoyoungerpatientswithnormalrenalfunction.In patientswithhepaticdiseases,themeaneliminationhalflifeisprolongedby30 minutesandthemeanplasmaclearanceisreducedby1ml/kg/min .(Seealso section4.2). Theapparentvolumeofdistributionininfants(3–12months)ishighercompared toolderchildren(1–8years)andadults.Inchildrenaged38years,clearanceis higher and the elimination halflife is approximately 20 minutes shorter comparedtoadultsandchildren<3years. When administered as acontinuous infusion to facilitate mechanical ventilation for a time period of 20 hours or more, the mean elimination halflife and the mean (apparent) volume of distribution at steady state are increased. Ahigh variabilitybetweenpatientswasfoundincontrolledclinicalstudies,relatedtothe nature and extent of (multiple) organ failure and individual patient characteristics.Inpatientswithmultipleorganfailureamean(±SD)elimination halflife of 21.5 (±3.3) hours, an (apparent) volume of distribution at steady state of 1.5 (±0.8) l/kg and a plasma clearance of 2.1(±0.8)ml/kg/min were found. Rocuroniumbromideisexcretedinurineandbile.Excretioninurineapproaches 40%within 1224hours.Afterinjectionofaradiolabeleddoseofrocuronium bromide, excretion of the radiolabel is on average 47% in urine and 43% in faecesafter9days.Approximately50%isrecoveredasrocuroniumbromide.No metabolitesaredetectedintheplasma. 5.3 Preclinical safety data Preclinical data reveal no special hazard for humans based on conventional studies of safety pharmacology, repeated dose toxicity, toxicity to reproduction andgenotoxicity. Carcinogenicitystudieshavenotbeenperformedwithrocuroniumbromide. 6. PHARMACEUTICAL PARTICULARS 6.1 List of excipients Waterforinjections Aceticacid,glacial(forpHadjustment) Sodiumchloride Sodiumacetatetrihydrate

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6.2 Incompatibilities Physical incompatibility has been documented for rocuronium bromide when added to solutions containing the following active substances: amphotericin, amoxicillin, azathioprine, cefazolin, cloxacillin, dexamethasone, , enoximone, erythromycin, famotidine, furosemide, hydrocortisone sodium succinate, insulin, intralipid, methohexital, methylprednisolone, prednisolone sodiumsuccinate,thiopental,trimethoprimandvancomycin. Thismedicinalproductmustnotbemixedwithothermedicinalproductsexcept thosementionedinsection6.6. 6.3 Shelf life Unopenedvial 3years Openedvial Theproductshouldbeusedimmediatelyafteropeningthevial. Afterdilution Chemical and physical inuse stability of a 5.0 mg/ml and 0.1 mg/ml solution (diluted with sodium chloride 9 mg/ml (0.9%) and glucose 50 mg/ml (5%) solutionforinfusion)hasbeendemonstratedfor24hoursatroomtemperature exposedtoroomlightinglass,PEandPVC. Fromthemicrobiologicalpointofview,theproductshouldbeusedimmediately. Ifnotusedimmediately,inusestoragetimesandconditionspriortousearethe responsibilityoftheuserandwouldnormallynotbelongerthan24hoursat2to 8°C, unless dilution has taken place in controlled and validated aseptic conditions. 6.4 Special precautions for storage Storeinarefrigerator(2°C8°C). Storageoutoftherefrigerator: RocuroniumKabimayalsobestoredoutsideoftherefrigeratoratatemperature ofupto30°Cforamaximumof12weeks,afterwhichitshouldbediscarded. Theproductshouldnotbeplacedbackintotherefrigerator,onceithasbeen keptoutside.Thestorageperiodmustnotexceedtheshelflife . Forstorageconditionsofthedilutedmedicinalproduct,seesection6.3. 6.5 Nature and contents of container Colourless glass vials (type I) with chlorobutyl rubber stopper and aluminium cap.Contentofthevials:2.5ml,5mlor10ml. Packagesizes: Packagingof5and10vialseachcontaining2.5ml. Packagingof5and10vialseachcontaining5ml.

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Packagingof5and10vialseachcontaining10ml. Notallpacksizesmaybemarketed.

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6.6 Pecial precautions for disposal and other handling Anyunusedsolutionsshouldbediscarded. The solution is to be visually inspected prior to use. Only clear solutions practicallyfreefromparticlesshouldbeused. Rocuronium Kabi has shown to be compatible with: sodium chloride 9 mg/ml (0.9%)andglucose50mg/ml(5%)solutionforinfusion. If rocuronium bromide is administered via the same infusion line with othermedicinal products, it is important that the infusion line is adequately flushed (e.g. with sodium chloride 9 mg/ml (0.9%) solution for infusion) betweenadministrationofrocuroniumbromideandmedicinalproductsforwhich incompatibility with rocuronium bromide has been demonstrated or for which compatibilitywithrocuroniumbromidehasnotbeenestablished. Anyunusedproductorwastematerialshouldbedisposedofinaccordancewith localrequirements.

7. MARKETING AUTHORISATION HOLDER [Tobecompletednationally.] 8. MARKETING AUTHORISATION NUMBER(S) [Tobecompletednationally.] 9. DATE OF FIRST AUTHORISATION/RENEWAL OF THE AUTHORISATION <{DD/MM/YYYY}><{DDmonthYYYY}> [Tobecompletednationally.] 10. DATE OF REVISION OF THE TEXT May2011 Date of SmPC: May 2011

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