Neuromuscular blocking agents in large animals

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Neuromuscular blocking agents(NMBA) used in animals and humans for muscle relaxation.This presentation is all about NMBA used in large animals viz. cattle and horse. Although use of NMBA alone is very limited, but this ppt can help in knowing NMBA along with doses,their mechanism of action, non neuromuscular effects and reversal of muscle relaxation. thank you Dr. Amandeep GADVASU

Transcript

Neuromuscular Blocking Agents

Submitted by – Amandeep

Department Of Veterinary Medicine

L2013V40M

INTRODUCTION

• Agents that interfere with transmission of

nerve impulse from somatic nerve ending to

skeletal muscle fibres

• Profound muscle relaxation & even paralysis

of skeletal muscles

Muscle Relaxants

Peripheral acting muscle

relaxant

Centrally acting muscle relaxant

Peripheral Acting Muscle Relaxant

Neuromuscular blocking agents

Directly acting drugs

Why?

• Inhalant anesthetics(IA) are complete anesthetics

• Fulfill triad-unconsciousness, analgesia & muscle

relaxation- of anesthesia

• Light planes- good loss of consciousness

• Deeper planes- analgesia & M. relaxation

• Cardiovascular compromise

Balanced Anesthesia

• Low concentration of IA to provide unconsciousness

• Analgesic to inhibit nociceptive processing

• NMBA to relax skeletal muscle

Physiology

At Microscopic Level

• Protruded circular area- binding site for Ach

• Pit- extracellular opening for ion channel

• Ach binds to one R• R composed of alpha,

beta, gamma & delta• 2 molecules of Ach bind

to 2 alpha subunits• Protein rotates into new

conformation

Other Mechanisms

• Densensitized state

• Channel blockade

Uses of NMBA

• Adequate surgical muscle relaxation without compromising

recovery

Absolute relaxation, eg : intra-ocular procedures, microsurgery

Specific muscle relaxation, eg : laparotomy , Caesarean

section, some orthopaedic surgery (reduction of dislocations),

diaphragm surgery

Uses of NMBA

• Reduction of anaesthetic dose

• Preservation of cardiopulmonary function

• Reduced operating times in 'high risk' patients

• Where positive pressure ventilation (PPV) required

• Where spinal reflexes need to be suppressed, eg: ear canal

surgery

Non – Depolarizing Depolarizing

• Act by competitively

blocking the binding of ACh

to its receptors / directly

block the ionotropic activity

of the ACh receptors

• Bind to Ach receptors but no

activation occurs

• Act by depolarizing the

plasma membrane of the

skeletal muscle fibre similar

to Ach

• Bind to Ach receptors

causing activation

Muscle paralysis

Neuromuscular Blocking Agents

• Non depolarising-

1. Long acting e.g tubocurarine

2. Intermediate acting e.g vecuronium, atracurium

3. Short acting e.g mivacurium

• Depolarising eg suxamethonium & decamethonium

Dose rates

• Pancuronium –

• In cattle - 0.04mg/kg, slow I/V(initial dose),

followed by increments of 0.008mg/kg

• In horse – 0.06mg/kg, , slow I/V(initial dose),

followed by increments of 0.001mg/kg

Dose rates

Doxacurium- usually not used

Atracurium –

Horse@ 0.15mg/kg, slow I/V(initial dose), then

increments of 0.06 mg/kg

Vecuronium- Horses@ 0.1 mg/kg slow I/V initial dose,

then increment of 0.02mg/kg

Mivacurium- it does not need reversal

Drug ( Depolarizing NMB)

Horse(mg/kg)

Cattle(mg/kg)

Succinyl choline(Scoline ®)

0.12-0.15 0.01-0.02

Non Neuromuscular effect

• Cardiovascular effect

• Histamine release

• Placental transfer

• CNS effects

• Protein binding

Non Neuromuscular Effect Of Succinylcholine

• Hyperkalemia

• Intraocular pressure

• Intragastric pressure

• Intracranial pressure

• Muscle soreness

Reversal Of NM Blockade 

Achieved by establishing high concentration of acetylcholine at the

binding site

Atropine (0.04 mg/kg S/C)

Glycopyrrolate (0.01 mg/kg I/M) administered intravenously atleast

one minute prior to the administration of reversal agent to block the

muscarinic effects of acetylcholine

Reversal Of NM Blockade

• Neostigmine 0.1 mg/kg I.V

• Edrophonium 1.0 mg/kg I.V

Cholinesterase Reversal

Cholinesterase reversal by increasing ACh and

displacing NMBA from receptors

Sugammadex MOA

• Modified cyclodextrin

• Cavity created by ring

is lipophilic, exterior is

hydrophilic

• Encapsulate lipophilic

drugs yet remain soluble

in water

Sugammadex MOA

• Resultant sugammadex bound NMBA (inclusion

complex) is then excreted by the kidneys

• Renal clearance of the NMBA has been found to be

enhanced by sugammadex encapsulation

Thanks

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