Lecture 14 (Exam 3) - Non-depolarizing Muscle Relaxants

Question 1

What is the only Short-Acting non-depolarizing NMBD (that is not used anymore)?

Answer 1

Mivacurium (Mivacron)

(slide 37)

Question 2

Which receptor do Non-Depolarizing muscle relaxants work on?

Answer 2

Nicotinic Acetylcholine Receptors

Slide 3

Question 3

What is Mivacurium(Mivacron):
Intubating dose:
Onset:
DOA:

With it’s DOA, what has to be considered?

Answer 3

0.15mg/kg
2-3 min
12-20min

Since its DOA is so short, may have to give supplemental doses.

(slide 37)

Question 4

True or False:
Non-depolarizing drugs only bind to one alpha-subunit

Answer 4

False - They compete for both alpha-subunits. 💁🏻‍♀️

Slide 3

Question 5

With Mivacurium(Mivacron) what conditions/side effects are less desirable?

And why does this drug have these?

Answer 5

Still causes s/e like coughing and spitting with inductions

Due to this drug being less “dense” of a block.
AKA “move-a-cron”

(slide 37)

Question 6

Since there is no conformational change in the nicotinic acetylcholine receptor, there are no shifts in which electrolytes?

Answer 6

Sodium and Potassium
Slide 3

Question 7

TOF ratio of _________ is indicative of a successful Non-Depolarizing NMBA block.

Answer 7

< 0.7

Slide 4

Question 8

What is the only Long-acting NMBD that we have to know/use?

What class of drug is it considered?

What properties does it have?

Induction dose:
Onset:
Duration:

Answer 8

Pancuronium (Pavulon)

Class: Bisquaternary aminosteroid

Properties: Vagolytic (inhibits actions of the vagus nerve)

Induction dose: 0.1 mg/kg
Onset: 3-5 mins
Duration: 60-90 mins

(slide 20)

Question 9

How many stereoisomers does Mivacurium (Mivacron) have and what are they? Which ones actually have neruomuscular blocking activity?

Answer 9

3 stereoisomers:
Cis-cis
*Cis-trans
*Trans-trans

*NM blocking ability

(slide 38)

Question 10

You give your patient Rocuronium for intubation, which drug should you give to maintain the paralysis?

Answer 10

Rocuronium - non-depolarizing drugs potentiate the action of other non-depolarizing drugs so both duration and recovery are long if you give a different drug

Slide 4

Question 11

How is Mivacurium(Mivacron) cleared?

Answer 11

by plasma cholinesterase

(slide 38)

Question 12

Does Mivacurium (Mivacron) release histamine?
And what additional detail or symptoms are seen about your answer?

Answer 12

Yes it can.

But only at doses that are >3X ED95 (this is never done- almost OD)

Would see:
- Transient MAP drop
- More common with rapid, large doses
- MAP drop more in HTN pts than non-HTN pts

(slide 39)

Question 13

Pancuronium majorily is eliminated how?

By how much percent?

Answer 13

80% eliminated unchanged in the urine

(slide 21)

Question 14

This term is used to suggest that some fibers are contracting while some are still blocked…

Answer 14

Fade

Slide 5

Question 15

CV adverse effects are due to what three things?

Answer 15

1. Release of histamine
2. Effects on cardiac muscarinic receptors
3. Effects on nACh-Rs at autonomic ganglia

Slide 7

Question 16

Difference between dose that produces blockade (ED95) and the dose that creates circulatory effect.

Answer 16

Autonomic Margin of Safety

Slide 7

Question 17

The “autonomic margin of safety” for Pancuronium is the ________ dose

Answer 17

Same

Slide 7

Question 18

Pancuronium produces ___________ at ED95 dose

Answer 18

Tachycardia ❤️‍🩹

Slide 7

Question 19

In the presence of RENAL FAILURE, what should we expect when considering administering Pavulon?

__-__% ⬇️ plasma clearance

Answer 19

Would expect much longer duration of effects of Pavulon 2/2 renal failure.

30-50% ⬇️ plasma clearance

(slide 21)

Question 19

Skeletal muscle weakness that occurs weeks to months after NMBDs are discontinued…

Answer 19

Critical Illness Myopathy

Slide 8

Question 20

Giving what drugs prior to NMBD may enhance risk for critical illness myopathy?

Answer 20

Glucocorticoids

Slide 8

Question 21

What two things would you want to give patients with critical illness myopathy?

Answer 21

More sedation
More analgesia

Slide 8

Question 22

In the presence of LIVER DX, what would we expect when considering the administration of Pavulon?

_________ volume distribution
______ initial dose needed
Prolonged ___________ ___ time

Answer 22

D/t deficient protein production, fluid leaks out grossly throughout the body, thereby causing the following:

⬆️ VD
Larger initial dose is needed
Prolonged elimination 1/2 time

(slide 21)

Question 23

What kind of drug normally causes critical illness myopathy?

Answer 23

Aminosteroid blocker (roc, vec, panc)

Slide 8

Question 24

Would 75-year-old Pee-paw be a good candidate for receiving Pancuronium?

Why or why not?

Answer 24

No!

Pee-paw has seen more moons than most and thus has a ⬇️ plasma clearance d/t ⬇️ renal function.

(slide 21)

Question 25

You give Pavulon to your pt undergoing a sloppabotomy (i.e., irrelevant procedure). What cardiovascular effects would you expect to see?

Why?

Where does this medication affect most often?

Will the BP ⬆️ or ⬇️?

Answer 25

⬆️ in HR, MAP, and CO

d/t vagal blockade (remember it’s a vagolytic)

occurs mostly at the SA node

BP increases d/t HR

(slide 22)

Question 26

CV effects of Pavulon continued.

Why else might we see an ⬆️ in HR, MAP, and CO? (we already said vagal blockade in a prev card)

What does that mean?

Does this mean we’ll have changes in the SVR or inotropy?

Answer 26

d/t SNS activation

This means that we’ll have release of NE presynaptically AND a simultaneous blockade of NE reuptake

No, there will not be changes in SVR or inotropy

(slide 22)

Question 27

T/F: Pancuronium will cause histamine release

Answer 27

False

(slide 22)

Question 28

When comparing Intermediate-acting NMBDs with Long-acting NMBDs, we would see a similar _____ of maximum ________.

Intermediate NMBDs would also have a _____ of the duration of Long-acting NMBDs.

Would CV effects be minimal or profound with Intermediate NMBDs?

What type of drugs could antagonize the intermediate NMBDs?

How long before this drug-mediated antagonism would take place?

Answer 28

onset; blockade

1/3

minimal/absent CV effects with Intermediate NMBDs

Anticholinesterase drugs would antagonize Intermediate NMBDs

would take ~20 mins after giving a full induction/intubation dose before antagonism would occur

(slide 24)

Question 29

List the 4 Intermediate-acting NMBDs.

Answer 29

Vecuronium
Rocuronium
Cisatracurium
Atracurium

(slide 23)

Question 30

How does acute hypokalemia alter response to NMBD?

Answer 30

1. Acute hypokalemia hyperpolarizes cell membrane (increased transmembrane potential)
2. Resistance to depolarizing NMBDs.
3. ↑ sensitivity to non-depolarizing NMBDs.

Slide 14

Question 31

How does acute hyperkalemia alter the response to NMBD?

Answer 31

1. Acute hyperkalemia decreases membrane potential (partially depolarizes cell membrane)
2. ↑ effects of depolarizing NMBDs.
3. Resistance to non-depolarizing NMBDs.

Slide 14

Question 32

When do you see NMBD resistance in Burn patients?

Answer 32

Resistance to NMBD begins approx. 10 days post-injury and declines after 60 days.
And 30%BSA or > burn( she didn’t explain very well)
(if pt with bad burn comes to ER, you use a regular dose to intubate)

Slide 15

Question 33

Vecuronium(Norcuron)

Is it an Aminosteroid?
Intubation dose?
Onset?
Duration?

Answer 33

Yes

Intubating Dose: 0.1 mg/kg

Onset: 3-5 minutes

Duration: 20-35 minutes

(Slide 25)

Question 34

1. Where is Vecuronium(Norcuron) metabolized?
2. What is the metabolite pathway?

Answer 34

1. The liver! Principle organ of elimination (*70% metabolized in liver).
2. Vecuronium is metabolized to 3-desacetylvecuronium [50-80% as potent].
   3-desacetylvecuronium is then rapidly converted to metabolite with 1/10 the effects!

(Slide 26)

Question 35

How is Vecuronium(Norcuron) excreted from the body?

Answer 35

Through the kidneys! [Approx 30% appears unchanged (*70% metabolized in liver)]

(Slide 26)

Question 36

Why should you be cautious in giving your renal dysfunction patient Vecuronium(Norcuron)?

Answer 36

Elimination ½ time prolonged

(Slide 26)

Question 37

What offsets the resistance of NMBD in burn patients?

Answer 37

Using 1.2mg/kg dose of rocuronium

Slide 15

Question 38

What is the proposed mechanism behind the resistance of NMBD in burn patients?

Answer 38

Burns alter the affinity of nACH receptors. Not related to altered density (or number or receptors)

Slide 15

Question 39

Why do Repeated doses or infusion of Vecuronium(Norcuron) cause cumulative effects?

Answer 39

Due to the cumulative effects from the active metabolites!!!

(Slide 26)

Question 40

Why do we need to be cautious when using Vecuronium(Norcuron) with the elderly?

Answer 40

1. Decreased volume of distribution (less muscle mass) (dehydration from ACE inhibitors)(Low CO and low blood flow)
2. Decreased plasma clearance (less hepatic flow)
   *Single dose mechanics unchanged
   *Delayed recovery with infusions

(Slide 27)

Question 41

Why do we need to be cautious when using Vecuronium(Norcuron) with obstetrics?

Answer 41

**Insignificant effects to fetus*

1. Increased clearance time in 3rd trimester (Due to progesterone)
2. Prolonged duration early postpartum (give IBW)

(Slide 27)

Question 42

How does pH effect Vecuronium(Norcuron)?

Answer 42

1. If you give your patient Vecuronium when they are already acidotic then there is no change in the duration of the drug!
2. If you give your patient Vecuronium and then your patient become acidotic, then you will prolong the duration of Vecuronium.
   [Concern postop with hypoventilation]
   *Acidosis decreases bound amount
   *Change in ionization at receptor increases attachment time

(Slide 28)

Question 43

In terms of resistance to NDNMBD, the Paretic arm (weakened or paralyzed) has _____resistance compared to the unaffected arm.

Answer 43

Higher

(so you want to use TOF on both side of the arms to compare in stroke patients.)

Slide 16

Question 44

In terms of NMBD resistance, the unaffected side of the stroke patient still has _____resistance compared to normal people who do not have a stroke.

Answer 44

greater
(Stroke patients: greater resistance in affected side than unaffected side and greater resistance in unaffected side than normal people)

Slide 16

Question 45

What is the proposed MOA of NMBDs on paresis or hemiplegia?

Answer 45

Due to the proliferation of extra junctional nACh receptors. ( more drugs needed to block the affected side)

Slide 16

Question 46

Cardiovascular concerns with Vecuronium(Norcuron)?

Answer 46

Essentially none

No histamine release

(Slide 29)

Question 47

What NMBDs are more likely to have allergic reaction to and less likely to have allergic reaction to?

What is the name of the NMBD that is least likely to have allergic reaction to?

Answer 47

More likely –> Succinylcholine

Less likely –> Pavulon, Vecuronium, Rocuronium (Aminosteroids)

Least likely –> Cisatricurium (Benz)

Slide 17

Question 48

What group of drugs is it possible to see cross sensitivity with?

Answer 48

Quaternary ammonium group

Slide 17

Question 49

Can you develop allergic reaction to quaternary ammounium group NMBD if you are allergic to soaps and cosmetics that contain quaternary ammonium?

Answer 49

Yes.
Slide 17

Question 50

Rocuronium (Zemuron) is an _________ acting ND-NMBA.

Is it an aminosteroid or benzylisoquinolone?

*bonus: will Sugammedex work reverse this?

Answer 50

Intermediate acting

Aminosteroid

Sugammadex should work to reverse!

slide 30

Question 51

Which gender is more sensitive to NMB, men or women? And why?

Answer 51

Women. They have less muscle mass than men.
Slide 18

Question 52

You give ___ less vecuronium and ___ less rocuronium to women than men.

Answer 52

22% less vec
30% less roc
Slide 18

Question 53

Rocuronium (Zemuron)

Dose:
Onset:
Duration:

What is the double dose of this med and what does it mimic? What would the onset be?
What is the risk of doing this?

Answer 53

Dose: 0.6mg/kg
Onset: 3-5 mins
Duration: 20-35 mins

Double dose: 1.2mg/kg
-will mimic SCh with an onset of 1-2 mins but it will last as long as Pancuronium.

slide 30

Question 54

Where is Rocuronium metabolized?

10-30% is excreted where?

Answer 54

Liver
⚠️ in liver failure & elderly pt’s (⬆ Vd)

Excreted via kidneys.

slide 31

Question 55

What are the cardiovascular effects of Rocuronium (Zemuron)?

Answer 55

No significant effects…lolz

-slight vagolytic effect BUT this is hard to tell bc of the Fentanyl and Prop you just gave.

slide 32

Question 56

Does Rocuronium (Zemuron) release histamine?

Answer 56

Not that we know of 😁

slide 32

Question 57

What effect does volatile gases have on NMB’s?

Answer 57

Dose dependent enhancement

Slide 9

Question 58

In what order do the volatile gases enhance NMB effect? (From greatest to least)

Answer 58

Des > Sevo > Iso

Slide 9

Question 59

What effects do diuretics, reglan, local anesthetics, and corticosteroids have on a NMB?

Answer 59

Prolonged or enhanced effect of the NMB.

Slide 10

Question 60

What effect does magnesium have on non-depolarizing agents? and how?

Answer 60

Magnesium enhances the blockade by decreasing prejunctional release of ACh and decreasing sensitivity to postjunctional membranes.

Slide 11

Question 61

What effect does magnesium have on depolarizing agents? and how?

Answer 61

Magnesium enhances the blockade of SCh. We dont know for sure.

**Mg sits its big ass in the way of Ca++ (all i remember from Schmidtty)

Slide 11

Question 62

What effect does an SNS stimulating drug have on a NMB?

Answer 62

Faster onset time of the NMB d/t increase in CO and skeletal muscle flow.

Slide 12

Question 63

What effect does an SNS inhibiting drug have on a NMB?

Answer 63

Delays onset of the NMB d/t decrease in CO and skeletal muscle flow.

Slide 12

Question 64

What effect does temperature have on Vecuronium and Pancuronium?

Answer 64

Mild hypothermia can double the duration.

Decreased temperature = decrease hepatic enzyme activity = decrease in drug metabolism.

Slide 13

Question 65

Dose, onset, duration, and chemical class of cisatracurium?

Answer 65

Dose: 0.1 mg/kg
Onset: 3 - 5 min
Duration: 20 - 35 min
Benzylisoquinoline
(Slide 33)

Question 66

Cisatracurium vs Atracurium- which is cleared more by plasma cholinesterase?

Answer 66

Atracurium = cleared via plasma cholinesterase.

Cisatracurium = cleared via Hoffman elimination (temp and pH dependent)
(Slide 34)

Question 67

Does onset change in the elderly with cisatracurium administration?

Answer 67

Yes, but onset delayed only by one minute. (🫥)
(Slide 35)

Question 68

How should dosing of cisatracurium be changed with obese patients?

Answer 68

Per lecture , obese pts will have prolonged duration of action –> Kane emailed and said its actually on IBW

(Slide 35)

Question 69

CV effects of Nimbex/cisatracurium?

Answer 69

CV stable and no histamine release.
(Slide 36)

Question 70

How does atracurium differ from cisatracurium?

Answer 70

Atracurium does cause a histamine release and is eliminated primarily via plasma cholinesterase. (Written on slide 36 during lecture)

Question 71

Will it take a long time to recover once a Nimbex drip is stopped?

Answer 71

No! The beauty of nimbex/cisatracurium is that it is eliminated quickly via Hoffman elimination, so not dependent on organs for clearance. Therefore, recovery from infusion is not affected by time.
(Slide 34)