SlideShare a Scribd company logo

Neuromuscular physiology

Download as PPTX, PDF
D
DrVishal Kandhway

Physiology of drugs acting at neuromuscular juction i/v/o anesthesia

Health & Medicine
1 of 36
Neuromuscular Physiology Presented by: Dr. Vishal kr. Kandhway Jawaharlal Nehru Medical College, Sawangi, Wardha
• A neuromuscular junction (NMJ) is the synapse or junction of the axon terminal of a motorneuron with the motor end plate, responsible for initiation of action potentials across the muscle's surface, ultimately causing the muscle to contract.
• Morphology: • The neuromuscular junction is specialized on the nerve side and on the muscle side to transmit and receive chemical messages. • Each motor neuron runs without interruption from the ventral horn of the spinal cord or medulla to the neuromuscular junction as a large, myelinated axon. • As it approaches the muscle, it branches repeatedly to contact many muscle cells and gather them into a functional group known as a motor unit .
Neuromuscular Junction (NMJ)
• The nerve is separated from the surface of the muscle by a gap of approximately 20 nm, called the junctional or synaptic cleft. • The nerve and muscle are held in tight alignment by protein filaments called basal lamina that span the cleft between the nerve and end plate. • The muscle surface is heavily corrugated, with deep invaginations of the junctional cleft—the primary and secondary clefts.
The Neuromuscular junction consists of A) Axon Terminal: contains around 300,000 vesicles which contain the neurotransmitter acetylcholine (Ach). B) Synaptic Cleft : 20 – 30 nm ( nanometer ) space between the axon terminal & the muscle cell membrane. It contains the enzyme cholinesterase which can destroy Ach . C) Synaptic Gutter ( Synaptic Trough) It is the muscle cell membrane which is in contact with the nerve terminal . It has many folds called Subneural Clefts , which greatly increase the surface area , allowing for accomodation of large numbers of Ach receptors . Ach receptors are located here .
• Formation of Neurotransmitter at Motor Nerve Endings:- • The axon of the motor nerve carries electrical signals from the spinal cord to muscles and has all of the biochemical apparatus needed to transform the electrical signal into a chemical one. • All the ion channels, enzymes, other proteins, macromolecules, and membrane components needed by the nerve ending to synthesize, store, and release acetylcholine and other trophic factors are made in the cell body and transmitted to the nerve ending by axonal transport.
• Ach formed is stored in cytoplasm until it is transported into vesicles for the release.
• How is Ach released…..
Ach release Ca entry into the nerve Opening of Ca channels P channels L Channels (slow) Na influx Depolarisation Nerve Action Potential
Muscle Contraction Transmission of AP along sarcolemma to open Tubular Ca Channels Generation of Action Potential depolarisation Opening of Na channels Ach binds to the post junctional receptors
• 1.Upon the arrival of an action potential at the presynaptic neuron terminal, voltage-dependent calcium channels open and Ca2+ ions flow from the extracellular fluids into the presynaptic neuron's cytosol • 2.This influx of Ca2+ causes neurotransmitter-containing vesicles to dock and fuse to the presynaptic neuron's cell membrane. Fusion of the vesicular membrane with the presynaptic cell membrane results in the emptying of the vesicle's contents (acetylcholine) into the synaptic cleft, a process known as exocytosis. • 3.Acetylcholine diffuses into the synaptic cleft and binds to the nicotinic acetylcholine receptors bound to the motor end plate. • 4.These receptors are ligand-gated ion channels, and when they bind acetylcholine, they open, allowing sodium ions to flow in and potassium ions to flow out of the muscle's cytosol.
• 5.Because of the differences in electrochemical gradients across the plasma membrane, more sodium moves in than potassium out, producing a local depolarization of the motor end plate known as an end-plate potential (EPP). • 6.This depolarization spreads across the surface of the muscle fiber into transverse tubules, eliciting the release of calcium from the sarcoplasmic reticulum, thus initiating muscle contraction. • 7.The action of acetylcholine is terminated when the enzyme acetylcholinesterase degrades part of the neurotransmitter (producing choline and an acetate group) and the rest of it diffuses away. • 8. The choline produced by the action of acetylcholinesterase is recycled — it is transported, through reuptake, back into the presynaptic terminal, where it is used to synthesize new acetylcholine molecules.
Acetylcholine (1)  Ach is synthesized locally in the cytoplasm of the nerve terminal , from active acetate (acetylcoenzyme A) and choline.  Then it is rapidly absorbed into the synaptic vesicles and stored there.  The synaptic vesicles themselves are made by the Golgi Apparatus in the nerve soma ( cell-body).  Then they are carried by Axoplasmic Transport to the nerve terminal , which contains around 300,000 vesicles .  Each vesicle is then filled with around 10,000 Ach molecules .
Acetylcholine (2) • When a nerve impulse reaches the nerve terminal , • it opens calcium channels  calcium diffuses from the ECF int the axon terminal  Ca++ releases Ach from vesicles by a process of EXOCYTOSIS • One nerve impulse can release 125 Ach vesicles. • The quantity of Ach released by one nerve impulse is more than enough to produce one End- Plate Potential .
 Ach combines with its receptors in the subneural clefts. This opens sodium channels  & sodium diffuses into the muscle causing a local,non- propagated potential called the “ End-Plate Potential (EPP)”, whose value is 50 – 75 mV.  This EPP triggers a muscle AP which spreads down inside the muscle to make it cntract .
• Fate of Ach….
• After ACh acts on the receptors , it is hydrolyzed by the enzyme Acetylcholinesterase (cholinesterase ) into Acetate & Choline . The Choline is actively reabsorbed into the nerve terminal to be used again to form ACh. This whole process of Ach release, action & destruction takes about 5-10 ms .
Anaesthetic Implication of Ca channels • Higher than normal concentrations of cations (e.g., magnesium, cadmium, manganese) can also block entry of calcium through P channels and decrease neuromuscular transmission. • This is the mechanism for muscle weakness in the mother and fetus when magnesium sulfate is administered to treat preeclampsia. • P channels are not affected by CCB”s– verapamil, diltiazem, and nifedipine. (These drugs have profound effects on the slower L channels present in CVS.) • As a result, the L-type calcium channel blockers have no significant effect at therapeutic doses on the normal release of Ach
Post-junctional Acetylcholine Receptors • 3 types: • 1) a junctional or mature receptor, • 2) an extrajunctional or immature (fetal) receptor • 3) neuronal α7 receptor (recently described)
• Mature receptor - α, β, δ, and ε • Fetal (immature/extrajunctional)- α, β, δ, and γ; there are two subunits of α and one of each of the others. • Neuronal α7 AChR consists of five α7-subunits
Drug Effects on Postjunctional Receptors • Nondepolarizing Muscle Relaxants • All NDMRs impair or block neurotransmission by competitively preventing the binding of acetylcholine to its receptor. • The final outcome (i.e., block or transmission) depends on the relative concentrations of the chemicals and their comparative affinities for the receptor.
• Reversal • Normally, acetylcholinesterase destroys acetylcholine and removes it from competition for a receptor. • Inhibitor of acetylcholinesterase such as neostigmine blocks it acetylcholine conc rises. • High concentration shifts the competition between acetylcholine and NDMR in favor of the former, thereby improving the chance of two acetylcholine molecules binding to a receptor. • This causes reversal of NDMR effect.
• Actions of Depolarizing Muscle Relaxants • have a biphasic action on muscle—an initial contraction, followed by relaxation lasting minutes to hours. • Not susceptible to hydrolysis by acetylcholinesterasethe depolarizing relaxants are not eliminated from the junctional cleft until after they are eliminated from plasma. • The time required to clear the drug from the body is the principal determinant of how long the drug effect lasts. • Because relaxant molecules are not cleared from the cleft quicklyreact repeatedly with receptors repeatedly depolarizing the end plate and opening channels.(basis of hyperkalemia)
Anaesthetic Implication of DMR”s • Ocular muscles express both mature and fetal receptors. • Accommodation (when synapse area is inexcitable through nerve) does not occur, and these muscles can undergo a sustained contracture in the presence of succinylcholine. • The tension thus developed forces the eye against the orbit  increased IOP by depolarizing relaxants.
Nonclassic and Noncompetitive Actions of Neuromuscular Drugs • Several drugs can interfere with the receptor, directly or through its lipid environment, and change transmission. • These drugs react with the neuromuscular receptor to change its function and impair transmission but do not act through the acetylcholine binding site. • These reactions cause drug-induced changes in the dynamics of the receptor, and instead of opening and closing sharply, the modified channels are sluggish. • These effects on channels cause corresponding changes in the flow of ions and distortions of the end-plate potential. • For example, procaine, ketamine, inhaled anesthetics, or other drugs that dissolve in the membrane lipid may change the opening or closing characteristics of the channel.
• If the channel is prevented from opening, transmission is weakened. • If, however, the channel is prevented from or slowed in closing, transmission may be enhanced. • Basis is two clinically important reactions: receptor desensitization and channel blockade.
Desensitization Block • Some receptors that bind to agonists do not undergo the conformational change to open the channel. • Receptors in these states are called desensitized (i.e., they are not sensitive to the channel-opening actions of agonists).
Anaesthetic Implication • The drugs acting by this route can decrease neuromuscular transmission. • They can cause an apparent increase in the capacity of nondepolarizing agents to block transmission.
Drugs Causing Desensitization of Nicotinic Cholinergic Receptors • Volatile anesthetics : Halothane ,Sevoflurane ,Isoflurane. • Antibiotics : Polymyxin B. • Barbiturates: Thiopental, Pentobarbital. • Agonists: Acetylcholine, Succinylcholine. • Local anesthetics: Dibucaine ,Lidocaine,Prilocaine. • Phenothiazines:Chlorpromazine,Trifluoperazine,Prochlorperaz ine.
Channel Block • Block channels at Ach receptors. • The normal flow of ions through the receptor is impaired, thereby resulting in prevention of depolarization of the end plate and a weaker or blocked neuromuscular transmission. • Anaesthetic Implication: • Channel block is believed to play a role in cocaine, quinidine, piperocaine, tricyclic antidepressant, naltrexone, naloxone induced alterations in neuromuscular function.
Extrajunctional, or fetal form of AChR • is expressed when there is decreased activity in muscle, as seen in the fetus before innervation or • after chemically or physically induced immobilization; • after lower or upper motor neuron injury, burns, or sepsis; or • after other events that cause increased muscle protein catabolism, including sepsis or generalized inflammation.
Anaesthetic Implication • Depolarizing or agonist drugs such as succinylcholine and acetylcholine depolarize immature receptors more easily, • thereby resulting in cation fluxes; doses one tenth to one hundredth of those needed for mature receptors can effect depolarization.
Anaesthetic Implication • most serious side effect with the use of succinylcholine in the presence of upregulated AChRs in one or more muscles is hyperkalemia. • (immature) receptor channels stay open for a longer timethe amount of potassium that moves from muscle to blood can be considerable. The resulting hyperkalemia can cause dangerous disturbances in cardiac rhythm, including ventricular fibrillation.
Acquired cholinesterase deficiency Conditions: • Liver failure • Renal insufficiency • Burn injury • Pregnancy (high estrogen levels) Inhibitory drugs: • Anti cholinesterases • Pancuronium • Metoclopramide • Insecticides • Drugs for Glaucoma, myasthenia • Chemotherapeutic agents
Thank you

Recommended

Physiology of the Neuromuscular Junction
Physiology of the Neuromuscular JunctionPhysiology of the Neuromuscular Junction
Physiology of the Neuromuscular JunctionAshwin Haridas
 
NEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONNEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONDr Nilesh Kate
 
neuromuscular junction physiology
neuromuscular junction physiologyneuromuscular junction physiology
neuromuscular junction physiologyGowri Shankar
 
Neuromuscular Junction (NMJ).pptx
Neuromuscular Junction (NMJ).pptxNeuromuscular Junction (NMJ).pptx
Neuromuscular Junction (NMJ).pptxPandian M
 
The neuromuscular physiology
The neuromuscular physiologyThe neuromuscular physiology
The neuromuscular physiologySourav Mondal
 
AUTONOMIC NERVOUS SYSTEM
AUTONOMIC NERVOUS SYSTEMAUTONOMIC NERVOUS SYSTEM
AUTONOMIC NERVOUS SYSTEMSado Anatomist
 
Bp regulation
Bp regulationBp regulation
Bp regulationDrChintansinh Parmar
 
Smooth Muscles
Smooth MusclesSmooth Muscles
Smooth MusclesPradeep Singh Narwat
 

Recommended

Physiology of the Neuromuscular Junction
Physiology of the Neuromuscular JunctionPhysiology of the Neuromuscular Junction
Physiology of the Neuromuscular JunctionAshwin Haridas
 
NEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONNEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONDr Nilesh Kate
 
neuromuscular junction physiology
neuromuscular junction physiologyneuromuscular junction physiology
neuromuscular junction physiologyGowri Shankar
 
Neuromuscular Junction (NMJ).pptx
Neuromuscular Junction (NMJ).pptxNeuromuscular Junction (NMJ).pptx
Neuromuscular Junction (NMJ).pptxPandian M
 
The neuromuscular physiology
The neuromuscular physiologyThe neuromuscular physiology
The neuromuscular physiologySourav Mondal
 
AUTONOMIC NERVOUS SYSTEM
AUTONOMIC NERVOUS SYSTEMAUTONOMIC NERVOUS SYSTEM
AUTONOMIC NERVOUS SYSTEMSado Anatomist
 
Bp regulation
Bp regulationBp regulation
Bp regulationDrChintansinh Parmar
 
Smooth Muscles
Smooth MusclesSmooth Muscles
Smooth MusclesPradeep Singh Narwat
 
Arterial blood pressure
Arterial blood pressureArterial blood pressure
Arterial blood pressureJamilah AlQahtani
 
Brachial plexus
Brachial plexusBrachial plexus
Brachial plexusNepalese army institute of health sciences
 
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUTDETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUTakash chauhan
 
Hypoxia
HypoxiaHypoxia
HypoxiaDrChintansinh Parmar
 
Compliance of lung
Compliance of lungCompliance of lung
Compliance of lungDr Nilesh Kate
 
Neuromuscular junction
Neuromuscular junctionNeuromuscular junction
Neuromuscular junctionMohamed Mahroof
 
Lungs compliance
Lungs complianceLungs compliance
Lungs compliancemariaidrees3
 
3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGY3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGYDr Nilesh Kate
 
Regulation of blood pressure
Regulation of blood pressureRegulation of blood pressure
Regulation of blood pressureAli Mansoor
 
Regulation of respiration
Regulation of respirationRegulation of respiration
Regulation of respirationLawrence James
 
Oxygen dissociation curve
Oxygen dissociation curveOxygen dissociation curve
Oxygen dissociation curveDIVYA JAIN
 
Properties of nerve fibre
Properties of nerve fibreProperties of nerve fibre
Properties of nerve fibreYogesh Ramasamy
 
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...Maryam Fida
 
cardiac output
cardiac output cardiac output
cardiac outputAthulya Lakshmanan
 
Neuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacologyNeuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacologyPradeep Singh Narwat
 
Cardiovascular physiology
Cardiovascular physiologyCardiovascular physiology
Cardiovascular physiologyJonathan Downham
 
Cerebral circulation
Cerebral circulationCerebral circulation
Cerebral circulationDr Nilesh Kate
 
Action potential
Action potentialAction potential
Action potentialAyub Abdi
 
Coronary circulation
Coronary circulationCoronary circulation
Coronary circulationAnwar Siddiqui
 
Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects Aqsa Mushtaq
 
Neuromuscular junction and its physiology
Neuromuscular junction and its physiologyNeuromuscular junction and its physiology
Neuromuscular junction and its physiologyDr.Prachee Sachan
 
Anatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junctionAnatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junctiongaganbrar18
 

More Related Content

What's hot

DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUTDETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUTakash chauhan
 
3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGY3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGYDr Nilesh Kate
 
Regulation of blood pressure
Regulation of blood pressureRegulation of blood pressure
Regulation of blood pressureAli Mansoor
 
Regulation of respiration
Regulation of respirationRegulation of respiration
Regulation of respirationLawrence James
 
Oxygen dissociation curve
Oxygen dissociation curveOxygen dissociation curve
Oxygen dissociation curveDIVYA JAIN
 
Properties of nerve fibre
Properties of nerve fibreProperties of nerve fibre
Properties of nerve fibreYogesh Ramasamy
 
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...Maryam Fida
 
Neuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacologyNeuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacologyPradeep Singh Narwat
 
Action potential
Action potentialAction potential
Action potentialAyub Abdi
 
Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects Aqsa Mushtaq
 

What's hot (20)

Arterial blood pressure
Arterial blood pressureArterial blood pressure
Arterial blood pressure
 
Brachial plexus
Brachial plexusBrachial plexus
Brachial plexus
 
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUTDETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
DETERMINANTS AND FACTORS AFFECTING CARDIAC OUTPUT
 
Hypoxia
HypoxiaHypoxia
Hypoxia
 
Compliance of lung
Compliance of lungCompliance of lung
Compliance of lung
 
Neuromuscular junction
Neuromuscular junctionNeuromuscular junction
Neuromuscular junction
 
Lungs compliance
Lungs complianceLungs compliance
Lungs compliance
 
3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGY3.9 SMOOTH MUSCLE PHYSIOLOGY
3.9 SMOOTH MUSCLE PHYSIOLOGY
 
Regulation of blood pressure
Regulation of blood pressureRegulation of blood pressure
Regulation of blood pressure
 
Regulation of respiration
Regulation of respirationRegulation of respiration
Regulation of respiration
 
Oxygen dissociation curve
Oxygen dissociation curveOxygen dissociation curve
Oxygen dissociation curve
 
Properties of nerve fibre
Properties of nerve fibreProperties of nerve fibre
Properties of nerve fibre
 
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
Surfactant & compliance, LAW OF LAPLACE, Work of Breathing (the guyton and ha...
 
cardiac output
cardiac output cardiac output
cardiac output
 
Neuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacologyNeuromuscular transmission and its pharmacology
Neuromuscular transmission and its pharmacology
 
Cardiovascular physiology
Cardiovascular physiologyCardiovascular physiology
Cardiovascular physiology
 
Cerebral circulation
Cerebral circulationCerebral circulation
Cerebral circulation
 
Action potential
Action potentialAction potential
Action potential
 
Coronary circulation
Coronary circulationCoronary circulation
Coronary circulation
 
Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects Hypoxia :types , causes,and its effects
Hypoxia :types , causes,and its effects
 

Viewers also liked

Neuromuscular junction and its physiology
Neuromuscular junction and its physiologyNeuromuscular junction and its physiology
Neuromuscular junction and its physiologyDr.Prachee Sachan
 
Anatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junctionAnatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junctiongaganbrar18
 
Anatomy & physiology of neuromuscular junction & monitoring
Anatomy & physiology of neuromuscular junction & monitoringAnatomy & physiology of neuromuscular junction & monitoring
Anatomy & physiology of neuromuscular junction & monitoringhavalprit
 
The neuromuscular junction disorders including myasthenia gravis
The neuromuscular junction disorders including myasthenia gravisThe neuromuscular junction disorders including myasthenia gravis
The neuromuscular junction disorders including myasthenia gravisSudhakar Marella
 
Neuromuscular junction
Neuromuscular junctionNeuromuscular junction
Neuromuscular junctionsheentarsis
 
Neuromuscular Transmission
Neuromuscular TransmissionNeuromuscular Transmission
Neuromuscular Transmissionmanuupanta
 
Neuro muscular blockers
Neuro muscular blockersNeuro muscular blockers
Neuro muscular blockersraj kumar
 

Viewers also liked (9)

Neuromuscular junction and its physiology
Neuromuscular junction and its physiologyNeuromuscular junction and its physiology
Neuromuscular junction and its physiology
 
Anatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junctionAnatomy and physiology of neuromuscular junction
Anatomy and physiology of neuromuscular junction
 
Anatomy & physiology of neuromuscular junction & monitoring
Anatomy & physiology of neuromuscular junction & monitoringAnatomy & physiology of neuromuscular junction & monitoring
Anatomy & physiology of neuromuscular junction & monitoring
 
The neuromuscular junction disorders including myasthenia gravis
The neuromuscular junction disorders including myasthenia gravisThe neuromuscular junction disorders including myasthenia gravis
The neuromuscular junction disorders including myasthenia gravis
 
Neuromuscular junction
Neuromuscular junctionNeuromuscular junction
Neuromuscular junction
 
Neuromuscular Transmission
Neuromuscular TransmissionNeuromuscular Transmission
Neuromuscular Transmission
 
Neuromuscular junction
Neuromuscular junctionNeuromuscular junction
Neuromuscular junction
 
Neuromuscular Diseases
Neuromuscular DiseasesNeuromuscular Diseases
Neuromuscular Diseases
 
Neuro muscular blockers
Neuro muscular blockersNeuro muscular blockers
Neuro muscular blockers
 

Similar to Neuromuscular physiology

Neuromuscular junction anatomy & physiology
Neuromuscular junction anatomy & physiologyNeuromuscular junction anatomy & physiology
Neuromuscular junction anatomy & physiologychet07
 
Attachments 2012 03_7
Attachments 2012 03_7Attachments 2012 03_7
Attachments 2012 03_7Muhammad Saim
 
acetylcholine (1).pdf
acetylcholine (1).pdfacetylcholine (1).pdf
acetylcholine (1).pdfjokpiel
 
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdf
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdfanatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdf
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdfDrHardikDudhatra
 
Neuronal Synaptic Transmission.pptx
Neuronal Synaptic Transmission.pptxNeuronal Synaptic Transmission.pptx
Neuronal Synaptic Transmission.pptxSaaduSalisu
 
Neuromuscular junction and synapses by DR.IRUM
Neuromuscular junction and synapses by DR.IRUMNeuromuscular junction and synapses by DR.IRUM
Neuromuscular junction and synapses by DR.IRUMSMS_2015
 
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.ppt
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.pptNEUROMUSCULAR JUNCTION AND MONITORING- pratibha.ppt
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.pptDrNaveen Mv
 
Lec 4. neuromuscular junction
Lec 4. neuromuscular junctionLec 4. neuromuscular junction
Lec 4. neuromuscular junctionAyub Abdi
 
Neuromuscular blocking agents & reversal in anesthesia
Neuromuscular blocking agents & reversal in anesthesiaNeuromuscular blocking agents & reversal in anesthesia
Neuromuscular blocking agents & reversal in anesthesiamushtaq ahmad Malik
 
5. Neuromuscular transmission .pdf
5. Neuromuscular transmission .pdf5. Neuromuscular transmission .pdf
5. Neuromuscular transmission .pdfBensufatiPizzo
 
Neuromuscular blocking agents
Neuromuscular blocking agentsNeuromuscular blocking agents
Neuromuscular blocking agentsDrJagadish Jena
 
Neuro Muscular Junction.pptx
Neuro Muscular Junction.pptxNeuro Muscular Junction.pptx
Neuro Muscular Junction.pptxAragawHamza2
 
Neuromuscular junction and Neuromuscular transmission
Neuromuscular junction and Neuromuscular transmissionNeuromuscular junction and Neuromuscular transmission
Neuromuscular junction and Neuromuscular transmissionDeekshya Devkota
 
NEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONNEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONAmudhaLakshmi1
 
Neuromuscular anatomy physiology
Neuromuscular anatomy physiologyNeuromuscular anatomy physiology
Neuromuscular anatomy physiologytulsimd
 

Similar to Neuromuscular physiology (20)

Neuromuscular physiology
Neuromuscular physiologyNeuromuscular physiology
Neuromuscular physiology
 
Neuromuscular junction anatomy & physiology
Neuromuscular junction anatomy & physiologyNeuromuscular junction anatomy & physiology
Neuromuscular junction anatomy & physiology
 
Attachments 2012 03_7
Attachments 2012 03_7Attachments 2012 03_7
Attachments 2012 03_7
 
acetylcholine (1).pdf
acetylcholine (1).pdfacetylcholine (1).pdf
acetylcholine (1).pdf
 
Lec 1 stu
Lec 1 stuLec 1 stu
Lec 1 stu
 
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdf
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdfanatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdf
anatomyphysiologyofneuromuscularjunctionmonitoring-110201023707-phpapp02 2.pdf
 
Neuronal Synaptic Transmission.pptx
Neuronal Synaptic Transmission.pptxNeuronal Synaptic Transmission.pptx
Neuronal Synaptic Transmission.pptx
 
Neuromuscular junction and synapses by DR.IRUM
Neuromuscular junction and synapses by DR.IRUMNeuromuscular junction and synapses by DR.IRUM
Neuromuscular junction and synapses by DR.IRUM
 
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.ppt
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.pptNEUROMUSCULAR JUNCTION AND MONITORING- pratibha.ppt
NEUROMUSCULAR JUNCTION AND MONITORING- pratibha.ppt
 
Lec 4. neuromuscular junction
Lec 4. neuromuscular junctionLec 4. neuromuscular junction
Lec 4. neuromuscular junction
 
Neuromuscular blocking agents & reversal in anesthesia
Neuromuscular blocking agents & reversal in anesthesiaNeuromuscular blocking agents & reversal in anesthesia
Neuromuscular blocking agents & reversal in anesthesia
 
5. Neuromuscular transmission .pdf
5. Neuromuscular transmission .pdf5. Neuromuscular transmission .pdf
5. Neuromuscular transmission .pdf
 
Neuromuscular blocking agents
Neuromuscular blocking agentsNeuromuscular blocking agents
Neuromuscular blocking agents
 
Anatomy of nmj
Anatomy of nmjAnatomy of nmj
Anatomy of nmj
 
Anatomy of nmj
Anatomy of nmjAnatomy of nmj
Anatomy of nmj
 
Neuro Muscular Junction.pptx
Neuro Muscular Junction.pptxNeuro Muscular Junction.pptx
Neuro Muscular Junction.pptx
 
Neuromuscular junction and Neuromuscular transmission
Neuromuscular junction and Neuromuscular transmissionNeuromuscular junction and Neuromuscular transmission
Neuromuscular junction and Neuromuscular transmission
 
Synapse
SynapseSynapse
Synapse
 
NEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTIONNEUROMUSCULAR JUNCTION
NEUROMUSCULAR JUNCTION
 
Neuromuscular anatomy physiology
Neuromuscular anatomy physiologyNeuromuscular anatomy physiology
Neuromuscular anatomy physiology
 

More from DrVishal Kandhway

Effects of anesthesia on mother and baby
Effects of anesthesia on mother and babyEffects of anesthesia on mother and baby
Effects of anesthesia on mother and babyDrVishal Kandhway
 

More from DrVishal Kandhway (7)

Brain death
Brain deathBrain death
Brain death
 
Insulin and antidiabetics
Insulin and antidiabeticsInsulin and antidiabetics
Insulin and antidiabetics
 
TURP
TURPTURP
TURP
 
Effects of anesthesia on mother and baby
Effects of anesthesia on mother and babyEffects of anesthesia on mother and baby
Effects of anesthesia on mother and baby
 
Iv cannula technique
Iv cannula techniqueIv cannula technique
Iv cannula technique
 
Ketamine
KetamineKetamine
Ketamine
 
Anticholinergic drugs
Anticholinergic drugsAnticholinergic drugs
Anticholinergic drugs
 

Recently uploaded

Pharmaceutical Marketting: Unit-5, Pricing
Pharmaceutical Marketting: Unit-5, PricingPharmaceutical Marketting: Unit-5, Pricing
Pharmaceutical Marketting: Unit-5, PricingArunagarwal328757
 
97111 47426 Call Girls In Delhi MUNIRKAA
97111 47426 Call Girls In Delhi MUNIRKAA97111 47426 Call Girls In Delhi MUNIRKAA
97111 47426 Call Girls In Delhi MUNIRKAAjennyeacort
 
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...Badalona Serveis Assistencials
 
epilepsy and status epilepticus for undergraduate.pptx
epilepsy and status epilepticus for undergraduate.pptxepilepsy and status epilepticus for undergraduate.pptx
epilepsy and status epilepticus for undergraduate.pptxMohamed Rizk Khodair
 
POST NATAL EXERCISES AND ITS IMPACT.pptx
POST NATAL EXERCISES AND ITS IMPACT.pptxPOST NATAL EXERCISES AND ITS IMPACT.pptx
POST NATAL EXERCISES AND ITS IMPACT.pptxvirengeeta
 
See the 2,456 pharmacies on the National E-Pharmacy Platform
See the 2,456 pharmacies on the National E-Pharmacy PlatformSee the 2,456 pharmacies on the National E-Pharmacy Platform
See the 2,456 pharmacies on the National E-Pharmacy PlatformKweku Zurek
 
Measurement of Radiation and Dosimetric Procedure.pptx
Measurement of Radiation and Dosimetric Procedure.pptxMeasurement of Radiation and Dosimetric Procedure.pptx
Measurement of Radiation and Dosimetric Procedure.pptxDr. Dheeraj Kumar
 
world health day presentation ppt download
world health day presentation ppt downloadworld health day presentation ppt download
world health day presentation ppt downloadAnkitKumar311566
 
Basic principles involved in the traditional systems of medicine PDF.pdf
Basic principles involved in the traditional systems of medicine PDF.pdfBasic principles involved in the traditional systems of medicine PDF.pdf
Basic principles involved in the traditional systems of medicine PDF.pdfDivya Kanojiya
 
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptx
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptxPERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptx
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptxdrashraf369
 
Presentation on Parasympathetic Nervous System
Presentation on Parasympathetic Nervous SystemPresentation on Parasympathetic Nervous System
Presentation on Parasympathetic Nervous SystemPrerana Jadhav
 
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara Rajendran
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara RajendranMusic Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara Rajendran
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara RajendranTara Rajendran
 
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic Analysis
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic AnalysisVarSeq 2.6.0: Advancing Pharmacogenomics and Genomic Analysis
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic AnalysisGolden Helix
 
Case Report Peripartum Cardiomyopathy.pptx
Case Report Peripartum Cardiomyopathy.pptxCase Report Peripartum Cardiomyopathy.pptx
Case Report Peripartum Cardiomyopathy.pptxNiranjan Chavan
 
SWD (Short wave diathermy)- Physiotherapy.ppt
SWD (Short wave diathermy)- Physiotherapy.pptSWD (Short wave diathermy)- Physiotherapy.ppt
SWD (Short wave diathermy)- Physiotherapy.pptMumux Mirani
 
Glomerular Filtration and determinants of glomerular filtration .pptx
Glomerular Filtration and determinants of glomerular filtration .pptxGlomerular Filtration and determinants of glomerular filtration .pptx
Glomerular Filtration and determinants of glomerular filtration .pptxDr.Nusrat Tariq
 
History and Development of Pharmacovigilence.pdf
History and Development of Pharmacovigilence.pdfHistory and Development of Pharmacovigilence.pdf
History and Development of Pharmacovigilence.pdfSasikiranMarri
 
Radiation Dosimetry Parameters and Isodose Curves.pptx
Radiation Dosimetry Parameters and Isodose Curves.pptxRadiation Dosimetry Parameters and Isodose Curves.pptx
Radiation Dosimetry Parameters and Isodose Curves.pptxDr. Dheeraj Kumar
 
PULMONARY EDEMA AND ITS MANAGEMENT.pdf
PULMONARY EDEMA AND ITS MANAGEMENT.pdfPULMONARY EDEMA AND ITS MANAGEMENT.pdf
PULMONARY EDEMA AND ITS MANAGEMENT.pdfDolisha Warbi
 

Recently uploaded (20)

Pharmaceutical Marketting: Unit-5, Pricing
Pharmaceutical Marketting: Unit-5, PricingPharmaceutical Marketting: Unit-5, Pricing
Pharmaceutical Marketting: Unit-5, Pricing
 
97111 47426 Call Girls In Delhi MUNIRKAA
97111 47426 Call Girls In Delhi MUNIRKAA97111 47426 Call Girls In Delhi MUNIRKAA
97111 47426 Call Girls In Delhi MUNIRKAA
 
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...
Presentació "Real-Life VR Integration for Mild Cognitive Impairment Rehabilit...
 
epilepsy and status epilepticus for undergraduate.pptx
epilepsy and status epilepticus for undergraduate.pptxepilepsy and status epilepticus for undergraduate.pptx
epilepsy and status epilepticus for undergraduate.pptx
 
POST NATAL EXERCISES AND ITS IMPACT.pptx
POST NATAL EXERCISES AND ITS IMPACT.pptxPOST NATAL EXERCISES AND ITS IMPACT.pptx
POST NATAL EXERCISES AND ITS IMPACT.pptx
 
See the 2,456 pharmacies on the National E-Pharmacy Platform
See the 2,456 pharmacies on the National E-Pharmacy PlatformSee the 2,456 pharmacies on the National E-Pharmacy Platform
See the 2,456 pharmacies on the National E-Pharmacy Platform
 
Measurement of Radiation and Dosimetric Procedure.pptx
Measurement of Radiation and Dosimetric Procedure.pptxMeasurement of Radiation and Dosimetric Procedure.pptx
Measurement of Radiation and Dosimetric Procedure.pptx
 
Epilepsy
EpilepsyEpilepsy
Epilepsy
 
world health day presentation ppt download
world health day presentation ppt downloadworld health day presentation ppt download
world health day presentation ppt download
 
Basic principles involved in the traditional systems of medicine PDF.pdf
Basic principles involved in the traditional systems of medicine PDF.pdfBasic principles involved in the traditional systems of medicine PDF.pdf
Basic principles involved in the traditional systems of medicine PDF.pdf
 
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptx
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptxPERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptx
PERFECT BUT PAINFUL TKR -ROLE OF SYNOVECTOMY.pptx
 
Presentation on Parasympathetic Nervous System
Presentation on Parasympathetic Nervous SystemPresentation on Parasympathetic Nervous System
Presentation on Parasympathetic Nervous System
 
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara Rajendran
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara RajendranMusic Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara Rajendran
Music Therapy's Impact in Palliative Care| IAPCON2024| Dr. Tara Rajendran
 
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic Analysis
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic AnalysisVarSeq 2.6.0: Advancing Pharmacogenomics and Genomic Analysis
VarSeq 2.6.0: Advancing Pharmacogenomics and Genomic Analysis
 
Case Report Peripartum Cardiomyopathy.pptx
Case Report Peripartum Cardiomyopathy.pptxCase Report Peripartum Cardiomyopathy.pptx
Case Report Peripartum Cardiomyopathy.pptx
 
SWD (Short wave diathermy)- Physiotherapy.ppt
SWD (Short wave diathermy)- Physiotherapy.pptSWD (Short wave diathermy)- Physiotherapy.ppt
SWD (Short wave diathermy)- Physiotherapy.ppt
 
Glomerular Filtration and determinants of glomerular filtration .pptx
Glomerular Filtration and determinants of glomerular filtration .pptxGlomerular Filtration and determinants of glomerular filtration .pptx
Glomerular Filtration and determinants of glomerular filtration .pptx
 
History and Development of Pharmacovigilence.pdf
History and Development of Pharmacovigilence.pdfHistory and Development of Pharmacovigilence.pdf
History and Development of Pharmacovigilence.pdf
 
Radiation Dosimetry Parameters and Isodose Curves.pptx
Radiation Dosimetry Parameters and Isodose Curves.pptxRadiation Dosimetry Parameters and Isodose Curves.pptx
Radiation Dosimetry Parameters and Isodose Curves.pptx
 
PULMONARY EDEMA AND ITS MANAGEMENT.pdf
PULMONARY EDEMA AND ITS MANAGEMENT.pdfPULMONARY EDEMA AND ITS MANAGEMENT.pdf
PULMONARY EDEMA AND ITS MANAGEMENT.pdf
 

Neuromuscular physiology

  • 1. Neuromuscular Physiology Presented by: Dr. Vishal kr. Kandhway Jawaharlal Nehru Medical College, Sawangi, Wardha
  • 2. • A neuromuscular junction (NMJ) is the synapse or junction of the axon terminal of a motorneuron with the motor end plate, responsible for initiation of action potentials across the muscle's surface, ultimately causing the muscle to contract.
  • 3. • Morphology: • The neuromuscular junction is specialized on the nerve side and on the muscle side to transmit and receive chemical messages. • Each motor neuron runs without interruption from the ventral horn of the spinal cord or medulla to the neuromuscular junction as a large, myelinated axon. • As it approaches the muscle, it branches repeatedly to contact many muscle cells and gather them into a functional group known as a motor unit .
  • 5. • The nerve is separated from the surface of the muscle by a gap of approximately 20 nm, called the junctional or synaptic cleft. • The nerve and muscle are held in tight alignment by protein filaments called basal lamina that span the cleft between the nerve and end plate. • The muscle surface is heavily corrugated, with deep invaginations of the junctional cleft—the primary and secondary clefts.
  • 6. The Neuromuscular junction consists of A) Axon Terminal: contains around 300,000 vesicles which contain the neurotransmitter acetylcholine (Ach). B) Synaptic Cleft : 20 – 30 nm ( nanometer ) space between the axon terminal & the muscle cell membrane. It contains the enzyme cholinesterase which can destroy Ach . C) Synaptic Gutter ( Synaptic Trough) It is the muscle cell membrane which is in contact with the nerve terminal . It has many folds called Subneural Clefts , which greatly increase the surface area , allowing for accomodation of large numbers of Ach receptors . Ach receptors are located here .
  • 7. • Formation of Neurotransmitter at Motor Nerve Endings:- • The axon of the motor nerve carries electrical signals from the spinal cord to muscles and has all of the biochemical apparatus needed to transform the electrical signal into a chemical one. • All the ion channels, enzymes, other proteins, macromolecules, and membrane components needed by the nerve ending to synthesize, store, and release acetylcholine and other trophic factors are made in the cell body and transmitted to the nerve ending by axonal transport.
  • 8. • Ach formed is stored in cytoplasm until it is transported into vesicles for the release.
  • 9. • How is Ach released…..
  • 10. Ach release Ca entry into the nerve Opening of Ca channels P channels L Channels (slow) Na influx Depolarisation Nerve Action Potential
  • 11. Muscle Contraction Transmission of AP along sarcolemma to open Tubular Ca Channels Generation of Action Potential depolarisation Opening of Na channels Ach binds to the post junctional receptors
  • 12. • 1.Upon the arrival of an action potential at the presynaptic neuron terminal, voltage-dependent calcium channels open and Ca2+ ions flow from the extracellular fluids into the presynaptic neuron's cytosol • 2.This influx of Ca2+ causes neurotransmitter-containing vesicles to dock and fuse to the presynaptic neuron's cell membrane. Fusion of the vesicular membrane with the presynaptic cell membrane results in the emptying of the vesicle's contents (acetylcholine) into the synaptic cleft, a process known as exocytosis. • 3.Acetylcholine diffuses into the synaptic cleft and binds to the nicotinic acetylcholine receptors bound to the motor end plate. • 4.These receptors are ligand-gated ion channels, and when they bind acetylcholine, they open, allowing sodium ions to flow in and potassium ions to flow out of the muscle's cytosol.
  • 13. • 5.Because of the differences in electrochemical gradients across the plasma membrane, more sodium moves in than potassium out, producing a local depolarization of the motor end plate known as an end-plate potential (EPP). • 6.This depolarization spreads across the surface of the muscle fiber into transverse tubules, eliciting the release of calcium from the sarcoplasmic reticulum, thus initiating muscle contraction. • 7.The action of acetylcholine is terminated when the enzyme acetylcholinesterase degrades part of the neurotransmitter (producing choline and an acetate group) and the rest of it diffuses away. • 8. The choline produced by the action of acetylcholinesterase is recycled — it is transported, through reuptake, back into the presynaptic terminal, where it is used to synthesize new acetylcholine molecules.
  • 14. Acetylcholine (1)  Ach is synthesized locally in the cytoplasm of the nerve terminal , from active acetate (acetylcoenzyme A) and choline.  Then it is rapidly absorbed into the synaptic vesicles and stored there.  The synaptic vesicles themselves are made by the Golgi Apparatus in the nerve soma ( cell-body).  Then they are carried by Axoplasmic Transport to the nerve terminal , which contains around 300,000 vesicles .  Each vesicle is then filled with around 10,000 Ach molecules .
  • 15. Acetylcholine (2) • When a nerve impulse reaches the nerve terminal , • it opens calcium channels  calcium diffuses from the ECF int the axon terminal  Ca++ releases Ach from vesicles by a process of EXOCYTOSIS • One nerve impulse can release 125 Ach vesicles. • The quantity of Ach released by one nerve impulse is more than enough to produce one End- Plate Potential .
  • 16.  Ach combines with its receptors in the subneural clefts. This opens sodium channels  & sodium diffuses into the muscle causing a local,non- propagated potential called the “ End-Plate Potential (EPP)”, whose value is 50 – 75 mV.  This EPP triggers a muscle AP which spreads down inside the muscle to make it cntract .
  • 17. • Fate of Ach….
  • 18. • After ACh acts on the receptors , it is hydrolyzed by the enzyme Acetylcholinesterase (cholinesterase ) into Acetate & Choline . The Choline is actively reabsorbed into the nerve terminal to be used again to form ACh. This whole process of Ach release, action & destruction takes about 5-10 ms .
  • 19. Anaesthetic Implication of Ca channels • Higher than normal concentrations of cations (e.g., magnesium, cadmium, manganese) can also block entry of calcium through P channels and decrease neuromuscular transmission. • This is the mechanism for muscle weakness in the mother and fetus when magnesium sulfate is administered to treat preeclampsia. • P channels are not affected by CCB”s– verapamil, diltiazem, and nifedipine. (These drugs have profound effects on the slower L channels present in CVS.) • As a result, the L-type calcium channel blockers have no significant effect at therapeutic doses on the normal release of Ach
  • 20. Post-junctional Acetylcholine Receptors • 3 types: • 1) a junctional or mature receptor, • 2) an extrajunctional or immature (fetal) receptor • 3) neuronal α7 receptor (recently described)
  • 21. • Mature receptor - α, β, δ, and ε • Fetal (immature/extrajunctional)- α, β, δ, and γ; there are two subunits of α and one of each of the others. • Neuronal α7 AChR consists of five α7-subunits
  • 22. Drug Effects on Postjunctional Receptors • Nondepolarizing Muscle Relaxants • All NDMRs impair or block neurotransmission by competitively preventing the binding of acetylcholine to its receptor. • The final outcome (i.e., block or transmission) depends on the relative concentrations of the chemicals and their comparative affinities for the receptor.
  • 23. • Reversal • Normally, acetylcholinesterase destroys acetylcholine and removes it from competition for a receptor. • Inhibitor of acetylcholinesterase such as neostigmine blocks it acetylcholine conc rises. • High concentration shifts the competition between acetylcholine and NDMR in favor of the former, thereby improving the chance of two acetylcholine molecules binding to a receptor. • This causes reversal of NDMR effect.
  • 24. • Actions of Depolarizing Muscle Relaxants • have a biphasic action on muscle—an initial contraction, followed by relaxation lasting minutes to hours. • Not susceptible to hydrolysis by acetylcholinesterasethe depolarizing relaxants are not eliminated from the junctional cleft until after they are eliminated from plasma. • The time required to clear the drug from the body is the principal determinant of how long the drug effect lasts. • Because relaxant molecules are not cleared from the cleft quicklyreact repeatedly with receptors repeatedly depolarizing the end plate and opening channels.(basis of hyperkalemia)
  • 25. Anaesthetic Implication of DMR”s • Ocular muscles express both mature and fetal receptors. • Accommodation (when synapse area is inexcitable through nerve) does not occur, and these muscles can undergo a sustained contracture in the presence of succinylcholine. • The tension thus developed forces the eye against the orbit  increased IOP by depolarizing relaxants.
  • 26. Nonclassic and Noncompetitive Actions of Neuromuscular Drugs • Several drugs can interfere with the receptor, directly or through its lipid environment, and change transmission. • These drugs react with the neuromuscular receptor to change its function and impair transmission but do not act through the acetylcholine binding site. • These reactions cause drug-induced changes in the dynamics of the receptor, and instead of opening and closing sharply, the modified channels are sluggish. • These effects on channels cause corresponding changes in the flow of ions and distortions of the end-plate potential. • For example, procaine, ketamine, inhaled anesthetics, or other drugs that dissolve in the membrane lipid may change the opening or closing characteristics of the channel.
  • 27. • If the channel is prevented from opening, transmission is weakened. • If, however, the channel is prevented from or slowed in closing, transmission may be enhanced. • Basis is two clinically important reactions: receptor desensitization and channel blockade.
  • 28. Desensitization Block • Some receptors that bind to agonists do not undergo the conformational change to open the channel. • Receptors in these states are called desensitized (i.e., they are not sensitive to the channel-opening actions of agonists).
  • 29. Anaesthetic Implication • The drugs acting by this route can decrease neuromuscular transmission. • They can cause an apparent increase in the capacity of nondepolarizing agents to block transmission.
  • 30. Drugs Causing Desensitization of Nicotinic Cholinergic Receptors • Volatile anesthetics : Halothane ,Sevoflurane ,Isoflurane. • Antibiotics : Polymyxin B. • Barbiturates: Thiopental, Pentobarbital. • Agonists: Acetylcholine, Succinylcholine. • Local anesthetics: Dibucaine ,Lidocaine,Prilocaine. • Phenothiazines:Chlorpromazine,Trifluoperazine,Prochlorperaz ine.
  • 31. Channel Block • Block channels at Ach receptors. • The normal flow of ions through the receptor is impaired, thereby resulting in prevention of depolarization of the end plate and a weaker or blocked neuromuscular transmission. • Anaesthetic Implication: • Channel block is believed to play a role in cocaine, quinidine, piperocaine, tricyclic antidepressant, naltrexone, naloxone induced alterations in neuromuscular function.
  • 32. Extrajunctional, or fetal form of AChR • is expressed when there is decreased activity in muscle, as seen in the fetus before innervation or • after chemically or physically induced immobilization; • after lower or upper motor neuron injury, burns, or sepsis; or • after other events that cause increased muscle protein catabolism, including sepsis or generalized inflammation.
  • 33. Anaesthetic Implication • Depolarizing or agonist drugs such as succinylcholine and acetylcholine depolarize immature receptors more easily, • thereby resulting in cation fluxes; doses one tenth to one hundredth of those needed for mature receptors can effect depolarization.
  • 34. Anaesthetic Implication • most serious side effect with the use of succinylcholine in the presence of upregulated AChRs in one or more muscles is hyperkalemia. • (immature) receptor channels stay open for a longer timethe amount of potassium that moves from muscle to blood can be considerable. The resulting hyperkalemia can cause dangerous disturbances in cardiac rhythm, including ventricular fibrillation.
  • 35. Acquired cholinesterase deficiency Conditions: • Liver failure • Renal insufficiency • Burn injury • Pregnancy (high estrogen levels) Inhibitory drugs: • Anti cholinesterases • Pancuronium • Metoclopramide • Insecticides • Drugs for Glaucoma, myasthenia • Chemotherapeutic agents