Neuromuscular Physiology and Pharmacology

Question 1

Where do motor neurons to skeletal muscle originate?

Answer 1

anterior (ventral) horn of the spinal cord (DAVE— ventral efferent)

Question 2

The sensory neurons from the skeletal muscle carry action potentials to the spinal cord via the _______ _______.

Answer 2

dorsal horn (DAVE— dorsal afferent)

Question 3

The motor and sensory nerves of the skeletal muscle are ______ nerves.

Answer 3

somatic

Question 4

Explain the role of calcium in the pre-synaptic junction?

Answer 4

when an action potential is generated and reaches the pre-synaptic junction–> stimulates Ca channel to open–> Ca causes vesicles to open–> release AcH into synaptic cleft–> pre-synaptic nicotinic receptor response to AcH–> produce more and release more AcH

Question 5

What is the positive feedback system that is associated with AcH?

Answer 5

the pre-synaptic nicotinic receptor responds to AcH by increasing the synthesis and release of AcH… this is a positive feedback system that prevents depletion of AcH at the NMJ.

Question 6

Explain the events that occur when AcH leaves the pre-synaptic membrane.

Answer 6

AcH diffuses down concentration gradient from pre-synaptic membrane to motor end plate of postsynaptic membrane–> combines with nicotinic receptors of protein channel–> when BOTH alpha subunits of nicotinic receptor channel are occupied by AcH, the channel snaps open= Na and Ca into the cell, K ions diffuse out into extracellular space–> contraction of muscle cell

Question 7

How is the neurotransmitter action impulse at the neuromuscular junction terminated?

Answer 7

acetylcholinesterase, aka true cholinesterase, breaks down acetylcholine into choline and acetate–> as AcH is metabolized, the motor end plate repolarizes and the muscle cell becomes ready for another squirt of AcH from the nerve terminal–> choline is transported back into the nerve terminal where it is used to re-synthesize AcH

Question 8

Acetylcholinesterase breaks acetylcholine down into _____ and ______.

Answer 8

choline (reabsorbed by nerve terminal to re-synthesize AcH) and acetate

Question 9

The release of the neurotransmitter (AcH) from all nerve terminals, including the motor nerve terminals, depends on the entry into the terminal of ______ ions.

Answer 9

calcium ions; calcium comes in, neurotransmitter goes out

Question 10

How does calcium relate to hyporeflexia and hyper-reflexia?

Answer 10

hypocalcemia is associated with a decrease in amount of neurotransmitter released (hyporeflexia), and hypercalcemia is associated with an increase in amount released (hyperreflexia)

Magnesium will be the OPPOSITE of calcium

Question 11

Calcium and magnesium are ______ (agonists or antagonists) at nerve terminals (pre-synaptically).

Answer 11

antagonistic

Question 12

The channel operated by the nicotinic receptor has _____ subunits. _____ AcH molecules are needed to open each nicotinic AcH receptor channel.

Answer 12

5 subunits (2 are identical– 40k); 2 AcH molecules are needed

Question 13

It takes ___ (#) acetylcholine molecules to open the ______-gated channel of the skeletal muscle motor end plate.

Answer 13

2; acetylcholine gated channels

Question 14

Non-depolarizers are _______ (competitive or non-competitive).

Answer 14

competitive inhibitors; when non-depolarizers bind to either AcH binding site on a nicotinic receptor, AcH CANNOT attach to that receptor, so the channel CANNOT open.

Question 15

Succinylcholine binds to the nicotinic receptors and _____ (opens or closes) the channels. ________ is maintained for an extended amount of time because Sux is not metabolized by true acetylcholinesterase.

Answer 15

opens; depolarization

Question 16

What neuromuscular blocking agent mimics acetylcholine at the NMJ?

Answer 16

Succinylcholine; results in opening of the channel and remains open d\t slower metabolism by plasma cholinesterase—> depolarization is prolonged

Question 17

What type of neuromuscular blocking agent produces the following effect: IV administration–> diffuses from vascular department into synaptic cleft of NMJ–> combines with nicotinic receptors of motor end plate–> exerts no direct effect on the channel–> channels stay closed, the post-synaptic membrane remains polarized.

Answer 17

Non-depolarizing NMB’s

Question 18

What NMB agent is associated with the following: action potentials cannot be initiated in skeletal muscle until the cell repolarizes because the Na channels are in the inactivated state.

Answer 18

depolarizing neuromuscular blocker

Question 19

How is succinylcholine metabolized?

Answer 19

by an enzyme in the plasma called plasma cholinesterase… also called pseudocholinesterase and butyrocholinesterase; as circulating Sux is metabolized, a gradient is created for Sux to diffuse from the skeletal muscle motor end plate back into the plasma to be quickly metabolized

Question 20

How is succinylcholine terminated?

Answer 20

by diffusion

Question 21

At the NMJ, does the pre-synaptic action of Sux enhance or antagonize its postsynaptic action?

Answer 21

Sux, by stimulating the presynaptic nicotinic receptor, augments the release of AcH–> since the released AcH opens channels and depolarizes the motor end-plate like Sux, the presynaptic action of Sux enhances its post-synaptic action.

Question 22

What are some of the physiological properties of neuromuscular relaxants?

Answer 22

1- 100% ionized at physiologic pH
2- very highly protein bound
3- do not cross the BBB (ions do not cross lipid bilayers)
4- do not cross the placental barrier (same reason)
5- trapped in renal tubule after filtration because of high degree of ionization (all muscle relaxants can be excreted by the kidney if other routes are unavailable)

Question 23

What is the trade name for succinylcholine?

Answer 23

Anectine (very short)

Question 24

What is the trade name for vecuronium?

Answer 24

Norcuron (intermediate)

Question 25

What is the trade name for rocuronium?

Answer 25

Zemuron (intermediate)

Question 26

What is the trade name for pancuronium?

Answer 26

Pavulon (LONG)

Question 27

What is the trade name for cisatracurium?

Answer 27

Nimbex (intermediate)

Question 28

What is the trade name for mivacurium?

Answer 28

Mivacron (short)

Question 29

What is the trade name for atracurium?

Answer 29

Tracrium (intermediate)

Question 30

_________ is the primary route of elimination for succinylcholine, atracurium, cisatracurium, and mivavurium.

Answer 30

metabolism

Question 31

_________ excretion is the primary route of elimination for vecuronium and rocuronium.

Answer 31

biliary excretion

Question 32

_________ excretion is the primary route of elimination for d-tubocurarine, metocurarine, pancuronium, gallamine, doxacurium, and pipecuronium.

Answer 32

renal excretion

Question 33

What two NMBs are metabolized by plasma cholinesterase?

Answer 33

succinylcholine and mivacurium

Question 34

What two NMBs are metabolized by Hoffman elimination?

Answer 34

atracurium (but also by ester hydrolysis) and cisatracurium

Question 35

What two NMBs are metabolized primarily by biliary excretion?

Answer 35

vecuronium and rocuronium (both are secondary by renal excretion)

Question 36

What is the difference in metabolism of cisatracurium and atracurium?

Answer 36

Nimbex is ONLY metabolized by Hoffman elimination, whereas Atracurium (tracrium) is eliminated by ester hydrolysis (non-specific esterases) and Hoffman (pH and temperature dependent degradation)

Question 37

Which NMBs elicit the release of histamine?

Answer 37

succinylcholine, mivacurium, atracurium, d-tubocurarine, metocurarine

Question 38

Why does succinylcholine have the potential to produce bradycardia?

Answer 38

mimics the action of acetylcholine and directly stimulates muscarinic receptors in the SA node

Question 39

Which NMBs can produce significant hypotension?

Answer 39

succinylcholine, d-tubocurarine, and metocurarine

Question 40

Which NMBs can produce significant hypertension?

Answer 40

pancuronium and gallamine

Question 41

What is the main cause related to administration of Mivavurium for hypotension and reflex tachycardia?

Answer 41

seen with rapid administration of high doses (>0.25mg/kg)

Question 42

Which of the commonly used NMBs DO NOT have histamine release?

Answer 42

cisatracurium, vecuronium, rocuronium, pancuronium

Question 43

Why is mild hypertension sometimes noted with the administration of pancuronium?

Answer 43

from an increase in HR d\t moderate antagonism of acetylcholine at the SA node

Question 44

How much can K levels rise after administration of Succinylcholine to a patient? to a burn patient?

Answer 44

plasma K+ concentration may increase by 0.5 mEq/liter in normal patients; 5-10 mEq/liter in burn, trauma, or head injury patients

Question 45

What conditions are associated with proliferation of extrajunctional postsynaptic cholinergic nicotinic receptors?

Answer 45

This occurs when nerve action potentials to skeletal muscle are interrupted–> post synaptic nicotinic receptors up-regulate and spread from the NMJ to the entire muscle fiber–> K exits the cells when the nicotinic receptor is stimulated

burns, paraplegia or hemiplegia, skeletal muscle trauma, upper motor neuron injury (head injury, CVA, parkinson’s)

Question 46

If a nerve stimulator is used on the right wrist of a patient with right sided hemiplegia, will the twitch be , or same as left?

Answer 46

it will be greater than the left d\t the upregulation of nicotinic receptors

Question 47

What are some of the criteria for the diagnosing of malignant hyperthermia?

Answer 47

unexplained signs of pyrexia (fever), tachycardia, cyanosis, rigidity 75%, or failure of the masseter muscle to relax (trismus) 50%

Question 48

What are the serum composition changes that can be seen with malignant hyperthermia?

Answer 48

increased H+, K+, Ca+, and CO2; decreased O2

Question 49

What is the defect in malignant hyperthermia?

Answer 49

failure of the sarcoplasmic reticulum to sequester calcium, so sustained contractions with increased metabolism result

Question 50

What is the treatment for malignant hyperthermia?

Answer 50

dantrolene–> acts on the sarcoplasmic reticulum to decrease the release of calcium to contractile proteins

Question 51

What is one of the earliest and most sensitive signs of malignant hyperthermia?

Answer 51

unexplained doubling or tripling in end-expiratory CO2; sympathetic hyperactivity manifested by increased HR is also an early sign of increased metabolism

Question 52

What agents can trigger malignant hyperthermia?

Answer 52

Succinylcholine and halogenated inhalational agents (isoflurane, desflurane, halothane, enflurane, sevoflurane)

Question 53

What effect does local anesthetics have on NMBs?

Answer 53

amides can increase block; reduce dose by 1/3 to 1/2

Question 54

What effect does volatile inhalational agents have on NDMBs?

Answer 54

block increased; reduce dose by one third to one half in presence of halogenated inhalational agent

Question 55

Is NDM blockade affected by Myasthenia Gravis?

Answer 55

block increased

Question 56

What is the effect of age when considering NDMBs?

Answer 56

block increased d\t organs of elimination less effective

Question 57

What effect does a thermal (burn) injury have on NDMBs?

Answer 57

block DECREASED; manifests 10 days after injury; peaks at 40 days; and declines after 60 days

Question 58

What effect does antibiotics have on NMBs?

Answer 58

block increased: gentamycin, neomycin, streptomycin, tatracycline
block unchanged: PCN, chloramphenicol, cephalosporins

Question 59

What effect does anticholinesterase agents have on succinylcholine?

Answer 59

block increased by cholinesterase inhibitors (edrophonium, neostigmine, physostigmine, echothiophate) as well as other drugs that depress this enzyme (like ester local anesthetics such as procaine and phenothiazines such as chlorpromazine)

Question 60

What effect does lithium and CCBs have on NMBs?

Answer 60

block increased

Question 61

What is the appropriate level of blockade for abdominal surgery?

Answer 61

90% blockade; 1 of 4 twitches

Question 62

While it is NOT an indicator of recovery, tidal volume returns to normal (>5ml/kg) when approx ______ % of receptors are occupied by NMBs.

Answer 62

75-80%

Question 63

If a patient has 4/4 twitches, how many receptors can still be blocked?

Answer 63

70-75% blockade can still remain

Question 64

What are some indicators that approx 50% or less receptors are occupied by NMBs?

Answer 64

pass inspiratory pressure test at least -40cm; head lift for 5 seconds; sustained strong hand grip; sustained bite, very reliable indicator of recovery

Question 65

Data suggests that conditions for intubation are appropriate when approx ____ % of receptors are blocked.

Answer 65

95% (diaphragm moves… no twitch with TOF)

Question 66

% blockade that is present with TOF 1/4.

Answer 66

90%– good for abdominal procedures

Question 67

% blockade that is present with TOF 4/4.

Answer 67

70-75%

Question 68

What is a phase 1 block?

Answer 68

depolarizing (phase 1) neuromuscular block— succinylcholine; amplitude of single twitch contractions decreases in proportion to the severity of the block

Question 69

When can a phase 2 block occur with Sux?

Answer 69

higher doses or prolonged exposure of the motor end plate to Sux leads to development of phase II, or desensitization block–> ion channels of the motor end plate close for reasons that are unknown, and the motor end plate repolarizes–> has characteristics of nondepolarizing block (mimics NDMBs)

Question 70

Ganglionic blockade is a side effect produced by which two NDMBs?

Answer 70

D-tubocurarine and metocurarine (ANS BLOCKADE)

Question 71

Which two NDMBs has antimuscarinic actions?

Answer 71

pancuronium and gallamine

Question 72

It is best to reverse a patient when ____ twitches are observed, but acceptable if only _____ is present.

Answer 72

2-3; 1

Question 73

Is the ventral horn located anteriorly or posteriorly?

Answer 73

ANTERIOR, but is EFFERENT

Question 74

What type of muscle fiber are motor neurons?

Answer 74

A alpha–> largest, most myelinated–> fastest conduction velocity

Question 75

Are nicotinic receptors found presynaptically or postsynaptically?

Answer 75

BOTH

Question 76

Explain the steps involved in neuromuscular impulse transmission; including the role of the presynaptic nicotinic receptor vs the postsynaptic receptor.

Answer 76

action potential travels motor nerve axon to the presynaptic nerve terminal-> depolarizes presynaptic terminal–> voltage gated calcium channels open–> Ca+ diffuses into terminal causing vesicles to release AcH (quantal release) into the synaptic cleft (exocytosis)–> presynaptic nicotinic receptor responds to the increased ACh in the synaptic cleft by increasing the synthesis and mobilization of ACh (positive feedback)–> ACh traverses the synaptic cleft to reach the postsynaptic nicotinic receptor of the motor end plate–> ACh binds to BOTH alpha subunits and opens the ion channel–> Na, Ca diffuse in, K diffuses out–> depolarization–> contraction (excitation-contraction coupling)–> acetylcholinesterase (aka true, specific, genuine, or type 1 cholinesterase) breaks down ACh into choline and acetate (by hydrolysis)–> choline is transported back into the nerve terminal where it is used to re-synthesize ACh

Question 77

What is the explanation for the phenomenon of fade seen with NDMB’s and with the phase II block seen with Sux?

Answer 77

the positive feedback system seen with the presynaptic nicotinic receptor–> causes increase in synthesis and mobilization of ACh containing vesicles (storage pools)

Question 78

What is the potential reason that larger initial doses of muscle relaxants are normally given compared to maintenance doses?

Answer 78

b\c the initial release of ACh is approx 125 quanta, each containing 10,000 ACh molecules–> this is a transient release and subsequent releases are much less… requiring less muscle relaxant doses

Question 79

What does the release of neurotransmitters from any nerve terminal (including motor nerve terminal DUH!) depend on?

Answer 79

the entry of Ca+ ions into the nerve terminal; “calcium comes in, neurotransmitter goes out”

side note: so…. hypocalcemia results in a decrease in the neurotransmitter release, and hypercalcemia causes an increase in the neurotransmitter release
magnesium concentration has the OPPOSITE effect

Question 80

Name what things acetylcholinesterase is responsible for degrading.

Answer 80

ACh, ester local anesthetics, neostigmine, edrophonium, remifentanil, and esmolol

Question 81

In regards to Sux… how common are fasciculations? how is it metabolized?

Answer 81

60-90% and myalgia within 24-48 hours after; not metabolized by true acetylcholinesterase, instead by plasma cholinesterase

Question 82

Name 5 common characteristics of nondepolarizing blocks (phase II):

Answer 82

1) MOA is competitive inhibition
2) fade follows high frequency stimulation (>0.1Hz)
3) exhibits post-tetanic facilitation
4) antagonized by anticholinesterases
5) no fasciculations

Question 83

What are 2 other names for Sux?

Answer 83

anectine, diacetylcholine; composed of two acetylcholine molecules linked together

Question 84

What are some other names for plasma cholinesterase?

Answer 84

pseudo-, butyro-, benzoyl-, false, non-specific, and type II cholinesterase

Question 85

Name 6 common characteristics of depolarizing blocks (phase I):

Answer 85

1) decreased single twitch height
2) response to high frequency stimulation is maintained
3) minimal or no fade after TOF
4) antagonized by nondepolarizers
5) potentiated by anticholinesterase
6) muscle fasciculations precede block

Question 86

Name 5 common properties of neuromuscular relaxants:

Answer 86

1) 100% ionized at physiologic pH
2) very highly protein bound
3) DO NOT cross BBB (ions do not cross lipid bilayers)
4) DO NOT cross placenta
5) trapped in renal tubule after filtration because high degree of ionization (all NMBs can be excreted by the kidney if other routes are unavailable)

Question 87

What response is seen in serum K level change after giving succinylcholine?

Answer 87

increase by 0.5 meQ/liter in normal pt and 5-10 meQ/liter in burn, trauma, or head injury pt

Question 88

Why is bradycardia seen with succinylcholine?

Answer 88

b\c of increased K+, especially after repeated dosing

Question 89

What effect can succinylcholine have on intraocular pressure?

Answer 89

increase by 5-15mmHg

Question 90

The termination of a drug and the elimination are two different actions. What NMB’s are terminated by redistribution?

Answer 90

R-VRAC

redistribution–> vecuronium, rocuronium, atracurium, cisatracurium

Question 91

If you use a nerve stimulator on the right wrist of a patient with right sided hemiplegia, will the twitch be less than, the same as, or greater than the twitch on the left?

Answer 91

GREATER than d\t upregulation of extrajunctional receptors (nicotinic receptors)

Question 92

When nerve action potentials to skeletal muscle are interrupted, postsynaptic nicotinic receptors up-regulate and spread from the neuromuscular junction to the entire muscle fiber…. K+ exits when the receptor is stimulated… risk for hyperkalemia…. What are 5 primary conditions that this can occur with?

Answer 92

1) thermal trauma (burns)
2) spinal cord transection (para or hemiplegia)
3) skeletal muscle trauma
4) upper motor neuron injury (head injury, CVA, parkinsons)
5) prolonged immobility

Question 93

What are some common signs of MH?

Answer 93

unexplained signs of increased ETCO2, pyrexia (fever), tachycardia, cyanosis, rigidity, trismus (masseter muscle spasm)

Question 94

What are changes in serum composition seen with MH?

Answer 94

increased H+, K+, Ca++, and CO2; decreased O2

Question 95

What is the primary defect involved in MH?

Answer 95

mutation of the RyR1 (ryanodine receptor), which is embedded in the sarcoplasmic reticulum of skeletal muscle–> causes constant calcium release from the SaRet–> sustained contractions with increased metabolism

Question 96

What is the role of Dantrolene in the treatment of MH?

Answer 96

acts on the sarcoplasmic reticulum to decrease the release of calcium to contractile proteins

Question 97

How often is trismus (masseter muscle spasm) seen with MH?

Answer 97

50%

Question 98

How often is whole body rigidity seen in patients with MH?

Answer 98

75%

Question 99

What is the earliest and second earliest signs of MH?

Answer 99

elevation of ET CO2, followed by tachycardia in response to increased metabolism (sympathetic hyperactivity)

Question 100

What are the primary agents that can trigger MH?

Answer 100

succinylcholine and halogenated inhalational agents (isoflurane, desflurane, halothane, enflurane, sevoflurane)

Question 101

Why isn’t cardiac muscle directly involved in malignant hyperthermia?

Answer 101

cardiac myocytes (muscle fibers) express the RyR2 isoform of the ryanodine receptor

Question 102

What are two other ways of saying the the “block” was increased?

Answer 102

potentiated=prolonged=increased=augmented

Question 103

What effect does local anesthetics and volatile anesthetic agents have on the degree of nondepolarizing neuromuscular blockade?

Answer 103

LA- block is increased by amides–> dose of NDMB can be reduced by 1/3 to 1/2
VA- block increased–> dose can be reduced 1/3 to 1/2 in presence of halogenated agent
**block unchanged in Sux administration with VA’s

Question 104

What is the effect of K+ on the degree of blockade in regards to a depolarizing block vs a nondepolarizing block?

Answer 104

NDMB- in presence of decreased K, block increased

DMB- in presence of hyperkalemia, block increased

Question 105

What antibiotics can increase the degree of NMB’s?

Answer 105

neomycin, streptomycin, tobramycin, dihydrostreptomycin, kanamycin, gentamicin, polymyxin B, colistin, linomycin, tetracyline
**unchanged by: PCN, chloramphenicol, cephalosporins, erythromycin

Question 106

What is the % of receptors occupied for the following? :
complete paralysis (0/4 TOF)

Answer 106

99-100%

Question 107

What is the % of receptors occupied for the following? :
diaphragm moves (0/4 TOF)

Answer 107

95%

Question 108

What is the % of receptors occupied for the following? :

head lift >5 sec, sustained hand grip, sustained bite

Answer 108

50%

Question 109

What is the % of receptors occupied for the following? :

sustained tetanus at 50Hz for 5 sec; VC at least 20ml/kg

Answer 109

70%

Question 110

What is the % of receptors occupied for the following? :

no palpable fade in double burst stimulation, more sensitive than TOF as indicator

Answer 110

60-70%

Question 111

What is the % of receptors occupied for the following? :

abdominal relaxation is adequate for most intra-abdominal procedures (1/4 TOF)

Answer 111

90%

Question 112

What is the % of receptors occupied for the following? :

tidal volume returns to normal (>5ml/kg), single twitch as strong as baseline (not an indicator of recovery)

Answer 112

75-80%

Question 113

What is the % of receptors occupied for the following? :

No palpable fade in TOF, useful as a gauge of recovery

Answer 113

70-75%

Question 114

What is the effect of cholinesterase inhibitors on the level of blockade of a NDMB vs a DMB?

Answer 114

NDMB- block is antagonized by agents that inhibit true acetylcholinesterase (edrophonium, neostigmine, pyridostigmine)
DMB- block is enhanced (augmented) by cholinesterase inhibitors (edrophonium, neostigmine, pyridostigmine)

Question 115

Does fade occur with a depolarizing muscle blockade?

Answer 115

No… only with NDMB’s… also no post tetanic facilitation (post-tetanic potentiation) will be present with DMB’s

Question 116

What is the difference in a phase I and phase II blockade?

Answer 116

Phase I is a depolarizing blockade

Phase II is a densensitization blockade

Question 117

What is a phase II block in regards to succinylcholine administration?

Answer 117

typically Sux will cause a phase I block… however prolonged exposure of the motor end-plate to Sux leads to a phase II (desensitization) blockade… will show characteristics of NDMB like fade and post-tetanic facilitation