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CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDE

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Title: CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDE Author: Dept of Anesthesiology Last modified by: Administrator Created Date: 7/23/2001 1:17:25 PM – PowerPoint PPT presentation

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Title: CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDE


1
CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDE
  • Jerrold H. Levy, MD
  • Professor of Anesthesiology
  • Emory University School of Medicine
  • Division of Cardiothoracic Anesthesiology and
    Critical Care
  • Emory Healthcare
  • Atlanta, Georgia

2
HISTORICAL PERSPECTIVES OF NEUROMUSCULAR BLOCKING
AGENTS
3
INTRODUCTION OF NEW DRUGS
  • 1494 - 1942 Curare
  • 1947 - 1951 Succinylcholine chloride, Gallamine,
    Metocurine, Decamethonium
  • 1960s Alcuronium
  • 1970s Pancuronium bromide, Fazadinium
  • 1980s Vecuronium bromide, Atracurium besylate
  • 1990 Pipecuronium bromide
  • 1991 Doxacurium chloride
  • 1992 Mivacurium chloride
  • 1994 Rocuronium bromide
  • 1999 Rapacuronium bromide

4
STRUCTURAL CLASSES OF NONDEPOL.ARIZING RELAXANTS
  • Steroids Rocuronium bromide, Vecuronium
    bromide, Pancuronium bromide, Pipecuronium
    bromide
  • Naturally occurring benzylisoquinolones curare,
    metocurine
  • Benzylisoquinoliniums Atracurium besylate,
    Mivacurium chloride, Doxacurium chloride

5
THE IDEAL RELAXANT
  • Nondepolarizing
  • Rapid onset
  • Dose-dependent duration
  • No side-effects
  • Elimination independent of organ function
  • No active or toxic metabolites

6
ONSET OF PARALYSIS IS AFFECTED BY
  • Dose (relative to ED95)
  • Potency (number of molecules)
  • Keo (chemistry/blood flow)
  • Clearance
  • Age

7
PHARMACODYNAMICS OF ROCURONIUM BROMIDE
8
ONSET OF ROCURONIUM BROMIDE
  • Onset rapid to intermediate
  • (dose dependent)

9
TRACHEAL INTUBATION
  • Pre-Medication Meperidine 1 mg/kg
  • Atropine 0.01 mg/kg
  • Induction Propofol to 2.5 mg/kg
  • Alfentanil to 0.25 mg/kg
  • Rocuronium bromide 0.6 mg/kg OR
  • Succinylcholine chloride 1 mg/kg
  • Intubation 60 sec. later

10
ROCURONIUM BROMIDETRACHEAL INTUBATION
  • Median time to ?80 block with 0.6 mg/kg is 60
    seconds (0.4-6.0 minutes)
  • Median onset time with 0.6 mg/kg is 1.8 minutes
    (0.6-13 minutes)

11
ROCURONIUM BROMIDETRACHEAL INTUBATION
  • Median time to ?80 blockade with 0.45 mg/kg is
    78 seconds (0.8-6.2 minutes)
  • Median onset time with 0.45 mg/kg is 3.0 minutes
    (1.3-8.2 minutes)

12
LOW DOSE PHARMACODYNAMICSCLINICAL PARAMETERS
  • Rocuronium bromide
  • Dose .45 mg/kg (n 14)
  • Mean maximum blockade 96 5
  • Mean time to 80 blockade 117 24 seconds
  • Mean time to maximum blockade 214 25 seconds
  • Mean time to completion of intubation 159 25
    seconds

13
ROCURONIUM BROMIDETRACHEAL INTUBATION
  • Median time to ? 80 blockade with 0.9 mg/kg is
    66 seconds (0.3-3.8 minutes)
  • Median onset time with 0.9 mg/kg is 84 seconds
    (0.8-6.2 minutes)
  • Median time to ? 80 blockade with 1.2 mg/kg is
    42 seconds (0.4-1.7 minutes)
  • Median onset time with 1.2 mg/kg is 60 seconds
    (0.6-4.7 minutes)

14
ROCURONIUM BROMIDERAPID SEQUENCE INTUBATION
15
ROCURONIUM BROMIDE RAPID SEQUENCE INTUBATION
  • n 230 (six clinical trials)
  • Premedication midazolam or temazepam
  • Induction thiopental (3-6 mg/kg) fentanyl
    (2-5 mcg/kg)
  • or or
  • propofol (1.5 - 2.5 mg/kg) alfentanil (1 mg)
  • Rocuronium bromide dose 0.6 mg/kg
  • Succinylcholine chloride dose 1-1.5 mg/kg

16
RAPID SEQUENCE INTUBATION
  • Rapid sequence intubation excellent-to-good
    conditions achieved within 60 - 90 seconds of
    administration in most patients
  • Dose Percentage of patients with
    excellent-to-good conditions
  • Rocuronium bromide (n120) 0.6 mg/kg 99 (95
    confidence
  • interval 95-99.9)
  • Succinylcholine chloride (n110) 1.0-1.5
    mg/kg 98 (95 confidence interval
    95-99.8)

17
DURATION OF ACTION OF NEUROMUSCULAR BLOCKING
AGENTS
  • Ultra-Short Succinylcholine chloride
  • Short Mivacurium chloride
  • Intermediate Rocuronium bromide, Vecuronium
    bromide, Atracurium besylate
  • Long Pancuronium bromide, curare,
    metocurine, Pipecuronium bromide,
    Doxacurium chloride

18
LOW DOSE PHARMACODYNAMICS DURATION
  • Rocuronium bromide
  • Dose .45 mg/kg
  • From injection to
  • Recovery of T1 n min
  • 10 of control 12 18 1
  • 25 of control 14 21 1
  • 90 of control 14 36 2
  • Spontaneous
  • Recovery n min
  • T 10-25 12 4 1
  • T 25-75 14 9 1
  • Adapted from Tullock et al Anesthesiology, vol
    75, no. 3A, 1991

19
CARDIOVASCULAR PROFILE OF ROCURONIUM BROMIDE
  • AND OTHER NEUROMUSCULAR BLOCKING AGENTS

20
HISTAMINE RELEASING POTENTIAL
  • Significant Insignificant
  • Tubocurarine Rocuronium bromide
  • Metocurine Vecuronium bromide
  • Atracurium besylate Pancuronium bromide
  • Mivacurium chloride Pipecuronium bromide
  • Succinylcholine chloride Doxacurium chloride

21
Muscle Relaxants
  • Pancuronium
  • Vagolytic increases heart rate, may require beta
    blockade
  • Easy to use
  • Intermediate duration of action
  • Slower onset
  • Not reversed at end of case

22
Muscle Relaxants
  • Vecuronium
  • No effects on HR, BP
  • Requires reconstitution
  • Reliable and controllable duration of action
  • Slower onset
  • Stable hemodynamics/no histamine release

23
Muscle Relaxants
  • Rapacuronium
  • Minimal effects on HR, BP
  • Controllable duration of action
  • Fast onset
  • Stable hemodynamics/minimal histamine release
  • Potential for bronchospasm led to its removal in
    2001

24
Effects of Rocuronium on Heart Rate
Levy et al. Anesth Analg 199478,318-321.
25
Effects of Rocuronium on Mean Arterial Pressure
100
90
80
Mean Arterial Pressure (mmHg)
70
60
50
0.0
1.0
2.0
3.0
4.0
5.0
6.0
Time (minutes)
Levy et al. Anesth Analg 199478,318-321.
26
Effects of Rocuronium on Histamine Release
3.0
2.5
2.0
Plasma Histamine (ng/ml)
1.5
1.0
0.5
0.0
0.0
1.0
2.0
3.0
4.0
5.0
Time (minutes)
Levy et al. Anesth Analg 199478,318-321.
27
ROCURONIUM BROMIDECARDIOVASCULAR PROFILE
  • Favorable cardiovascular profile
  • Histamine release unlikely
  • Mild vagolytic activity

28
PHARMACODYNAMICS OF ROCURONIUM BROMIDE IN
PEDIATRICS
29
ONSET AND DURATIONOF ACTION OF ROCURONIUM BROMIDE
IN INFANTS (3 MOS.-1 YR. DURING
N2O/HALOTHANE ANESTHESIA
30
ONSET AND DURATION OF ACTION OF ROCURONIUM
BROMIDE IN CHILDREN (1-5 YRS.) DURING
N2O/HALOTHANE ANESTHESIA
31
PHARMACODYNAMICS OF ROCURONIUM BROMIDE IN
GERIATRICS
32
ROCURONIUM BROMIDE IN THE ELDERLY (gt65YR.)
33
ROCURONIUM BROMIDE INFLUENCE OF AGESummary
  • Pediatrics (3 mos. - 1 yr)
  • 0.6 mg/kg Rocuronium bromide produces excellent
    to good intubating conditions within 1 minute,
    with 41 minutes of clinical relaxation (median)
  • Rocuronium bromide package insert

34
ROCURONIUM BROMIDE INFLUENCE OF AGESummary
  • Pediatrics (1 yr - 12 yrs)
  • 0.6 mg/kg Rocuronium bromide produces excellent
    to good intubating conditions within 1 minute,
    with 27 minutes of clinical relaxation (median)
  • Rocuronium bromide package insert

35
ROCURONIUM BROMIDE INFLUENCE OF AGESummary
  • Adults (18 - 64 yrs)
  • 0.6 mg/kg Rocuronium bromide produces excellent
    to good intubating conditions within 60 seconds,
    with 31 minutes of clinical relaxation (median)
  • Rocuronium bromide package insert

36
ROCURONIUM BROMIDE INFLUENCE OF AGESummary
  • Geriatric (? 65 yrs)
  • 0.6 mg/kg Rocuronium bromide produces excellent
    to good intubating conditions within 2.3 minutes,
    with 46 minutes of clinical relaxation (median)
  • Rocuronium bromide package insert

37
CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDE IN
RENAL FAILURE
38
Rocuronium bromide (0.6 mg/kg)Effects of Renal
Failure on Onsetof Neuromuscular BlockageUnder
Steady State Isoflurane Anesthesia
  • Normal Renal Function Renal Transplantation
  • (n 10) (n 10)
  • Onset Time (sec) 69 24 63 17
  • Values are mean SD
  • Patients with end-stage renal disease
    undergoing cadaver renal transplantation
  • Adapted from Szenochradsky et al Anesthesiology
    77899-904, 1992

39
CLINICAL PHARMACOLOGY OF ROCURONIUM BROMIDEIN
HEPATIC DISEASE
40
ROCURONIUM BROMIDEEffects of Hepatic Disease
Under Steady State Isoflurane Anesthesia
  • Neuromuscular Effects
  • Onset unchanged
  • Recovery increased
  • Larger or repeat doses may have prolonged effect
  • Rocuronium bromide package insert

41
ROCURONIUM BROMIDEEffects of Hepatic Disease
Under Steady State Isoflurane Anesthesia
  • Pharmacokinetics
  • Clearance unchanged
  • Central and steady state distribution volumes and
    elimination half-life increased
  • Rocuronium bromide package insert

42
THE PHARMACODYNAMICS OF ROCURONIUM BROMIDE IN THE
OBESE
43
  • Obesity defined as ? 30 of Ideal Body Weight
  • Dose can be based on patients actual body weight
  • Rocuronium bromide package insert

44
ROCURONIUM BROMIDE IN CONTINUOUS INFUSION
45
ROCURONIUM BROMIDEContinuous Infusion
  • Recommended Initial Infusion Rate (Adult)
  • 0.01-0.012 mg/kg/min. initiated only after
    spontaneous recovery from an intubating dose
  • Upon reaching the desired level of neuromuscular
    block, the infusion of Rocuronium bromide must be
    individualized for each patient
  • Rocuronium bromide package insert

46
ROCURONIUM BROMIDEContinuous Infusion
  • Recommended Initial Infusion Rate (Pediatric)
  • 0.012 mg/kg/min. initiated only after spontaneous
    recovery from an intubating dose (under
    Halothane)
  • Upon reaching the desired level of neuromuscular
    block, the infusion of Rocuronium bromide must be
    individualized for each patient
  • Rocuronium bromide package insert

47
ROCURONIUM BROMIDE DRUG INTERACTIONS
48
ROCURONIUM BROMIDE DRUG INTERACTIONS
  • Intravenous Anesthetics
  • The use of propofol for Induction and
    maintenance of anesthesia does not alter clinical
    duration of recovery
  • Rocuronium bromide package insert

49
ROCURONIUM BROMIDE DRUG INTERACTIONS
  • Volatile Anesthetics
  • Rocuronium bromide requirements are reduced by
    approximately 10-25 when used with enflurane or
    isoflurane, but little change when used with
    halothane
  • Rocuronium bromide package insert

50
ROCURONIUM BROMIDE DRUG INTERACTIONS
  • Antibiotics
  • Drugs which may enhance the neuromuscular
    blocking action of nondepolarizing agents such as
    Rocuronium bromide include certain antibiotics
    (i.e., aminoglycosides vancomycin
    tetracyclines bacitracin polymyzins collistin
    and sodium colistimethate)
  • Rocuronium bromide package insert

51
ROCURONIUM BROMIDE DRUG INTERACTIONS
  • Anticonvulsants
  • shorter durations of neuromuscular block may
    occur and infusion rates may be higher
  • Rocuronium bromide package insert

52
ROCURONIUM BROMIDECONCLUSIONS
  • Mono-quaternary steroidal drug
  • Structural relative of Vecuronium bromide
  • Rapid to intermediate onset of action.
    Significantly more rapid than Vecuronium bromide
    or Atracurium besylate
  • For use in outpatient or inpatient procedures of
    varying lengths
  • suitable for rapid sequence intubation
  • Favorable cardiovascular profiles
  • Eliminated mainly by liver minimally by the
    kidneys

53
Current ConceptsinNeuromuscular Blockade
7776
54
Neuromuscular Agents Costs of Care
  • Cost of care ? acquisition cost
  • The real, substantial savings accrue from use of
    intermediate- and short-acting drugs because
  • Inexpensive, long-acting drugs are associated
    with prolonged postoperative recovery 1
  • Fast recovery means shorter risk periods of
    residual blockade. This translates into fewer
    postoperative complications, as shown in the Berg
    study2
  • Postoperative complications are very
    expensiveAvoiding these is where the real cost
    savings accrue
  • 1Ballantyne JC, et al. Anesth Analg. 1997 85476
  • 2Berg H, et al. Acta Anaesthesiol Scand.
    1997411095

55
Rationale for Selection of NMBs
  • Cardiovascular stability
  • Nondepolarizing vs depolarizing
  • Organ-independent elimination
  • Clinically significant active or toxic
    metabolites
  • Predictability of duration
  • Cumulative effects
  • Reversibility
  • Time to onset
  • Stability of solution
  • Cost
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