PPT neuromuscular blocking and reversal

Question 1

First successful administration of NMB?

Answer 1

Curare in 1912 by Arthur Lawen a German Surgeon.

Question 2

What type of antagonist is a nondepolorizing NMB?

Answer 2

competative antagonist.

Question 3

Tell me how Succ works?

Answer 3

Succ. produces a prolonged depolarization of the endplate region that results in desensitization of nicotinic acetylcholine receptors; inactivation of voltage gated sodium channels at the neuromuscular junction and increase in potassium permeability in the surrounding membrane. Thus producing the failure of the action potential generation due to membrane hyperpolarization and a block ensues

Question 4

what is responsible for the rapid hydorlysis of released acetylcholine to acetic acid and choline?

Answer 4

acetylcholinesterase (true cholinesterase)

Question 5

what hydrolysis succ, and where does it occur?

Answer 5

plasma cholinesterase or pseudocholinesterase and it occurs mainly in the plasma.

Question 6

what are all neuromuscular blockers structurally related to?

Answer 6

acetylcholine

Question 7

what is the one NMB that is not a synthetic alkaloid?

Answer 7

tubocurarine which is extracted from the Amazonian vine (cheaper this way)

Question 8

Nondepolorizing NMB what twho classes are their?

Answer 8

Steroidal

Benzylisoquinoinium

Question 9

example of a Benzylisoquinolinium?

Answer 9

South American Indian’s arrow poisons. Tubocurarine is the most important curare alkaloid.
Atracurium
cisatracurium (nimbex)

Question 10

what type of patients should you not use tubocurarine with?

Answer 10

not suitable for renal or liver failure patients.

Question 11

intubating dose of tubocurarine?

Answer 11

.5-.6mg/kg

Question 12

Atracurium (what is important about it’s metabolism?)

Answer 12

can undergo ester hydrolysis

Question 13

what does laudanoisine depend on?

Answer 13

depends on the liver for clearance with ~70% excreted in bile with remainder in the urine

Question 14

what is laudanoisine?

Answer 14

a metabolite of the neuromuscular-blocking drugs atracurium and cisatracurium with potentially toxic systemic effects. It crosses the blood-brain barrier easily and may cause excitement and seizure activity

Question 15

what patients would laudanoisine be a problem with?

Answer 15

not good for liver patients, liver cirrhosis (according to class notes from Hammon talking)

Question 16

cisatracurium tell me about it?

what does it come from, what elimination does it use, histamine? What patients would you use it with?

Answer 16

Isomer of atracurium
hoffman elimination to laudanosine and monoquatenary alcohol metabolie.
Hoffman is 77% of clearance
does not cause histamine release like atracturium if given in clinical dose range.
Good for patients with renal issues.

Question 17

where does hoffman elimination occur?

Answer 17

in the plasma?

Question 18

list steroidal NMB?

Answer 18

Pancuronium
Vecuronium
Rocuronium

Question 19

Pancuronium remains stable for how long at room temp?

Answer 19

6 months

Question 20

Vecuronium, if you have what kind of issues this med will last longer on you?

Answer 20

liver issues (principal elimination is liver)

Question 21

which will you have to re-dose more often Vec or Roc?

Answer 21

Vecuronium

Question 22

Rocuronium, onset time and potency?

Answer 22

fast onset (1-3 min depending on dose)
6 times less potent than vecuronium.

Question 23

Roc is stable at room temp for how long?

Answer 23

60 days

Question 24

in relation to NMB ED50 and ED95 would mean?

Answer 24

ED50 is 50% reduction in twitch height, and ED95 is 95% reduction in twitch height.

Question 25

inhalation anesthetics potentiate the NMBlocking effects of NMB, list from most to least to potentiate.

Answer 25

DES>SEVO>ISO>HALO>Nitrous Oxide>barbiturate>propofol

Question 26

Can Des affect your Rocuronium?

Answer 26

YES! Potentiates it.

Question 27

Can antibiotics potentiate NMB? If so then how?

Answer 27

Yes, All inhibit the prejunctional release of acetylcholine and also depress postjunctional nicotinic acetylcholine receptor sensitivity to acetylcholine

Question 28

Whats the relationship between clindamycin, penicillin and Ancef?

Answer 28

Clindamycin was given to people with allergy to penicillin at one time, so that is why you will see it, otherwise they take ancef.
Link thought between penicillin and ancef, but has now been found false.

Question 29

what antibiotics potentiate NMB?

Answer 29

aminoglycosides
polymyxins
lincomycine
clindamycin
and tetracycline (exhibits post junctional activity only)

Question 30

name some other conditions or drugs that potentiate blockade of NMBD?

Answer 30

hypothermia
magnesium sulfate
High magnesium concentrations inhibit calcium channels at the presynaptic nerve terminals that trigger the release of acetylcholine

quinidine an antidyshythmic

Question 31

What drugs or conditions will decrease the potency of NMBD?

Answer 31

Chronic use of anticonvulsant therapy

hyperparathyroidism, hypercalcemia is associated with decreased sensitivity to atracurium and thus a short duration of neuromuscular blockade.

Question 32

what will eat up your drugs quicker?

Answer 32

anticonvulsant therapy and street drug usage.

Question 33

link between potency and onset of action of NMBD?

Answer 33

Onset of action is inversely proportional to potency of NMBD

Low potency = rapid onset

High potency = slow onset

Question 34

What NMBD is the exception to the potency and drug onset time inverse rule?

Answer 34

atracurium

Question 35

what is potency expressed in and why?

Answer 35

moles per kilogram

ultimately, we have a variable number of molecules chasing a fixed number of nicotinic receptors. The fewer molecules it takes (per kilogram of body weight) to achieve a given degree of receptor occupancy, the greater the affinity the drug has for the receptor. This is best expressed in micromoles per kilogram rather than in milligrams per kilogram.

Question 36

what is buffered diffusion and what drugs does it occur with?

Answer 36

The process in which diffusion of a drug is impeded because it binds to extremely high-density receptors within a restricted space

Can be seen with high potency but not low potency drugs

Buffered diffusion causes repetitive binding to and unbinding from receptors keeping potent drugs such as tubocurarine in the neighborhood of effector sites and potentially lengthening the duration of effect

Question 37

Explain the autonomic effects of NMBD?

Answer 37

NMBD interacts with nicotinic and muscarinic cholinergic receptors within the SNS and PNS and at the nicotinic receptors of the neuromuscular junction.

Question 38

Adverse effects of tubocurarine?

Answer 38

marked ganglion blockade resulting in hypotension;

histamine manifestations (hypotensin, reflex tachy,bronchospasm) in susceptible patients.

Question 39

adverse effects of pancuronium?

Answer 39

direct vagolytic effect. Can block muscarinic receptors on sympathetic postganglionic nerve terminals resulting in inhibition of a negative feedback mechanism whereby excessive catecholamine release is modulated or prevented Can also stimulate catecholamine release from adrenergic nerve terminals.

Question 40

Benzylisoquinoliniums release histamine what can occur bc of this and which NMBD that falls under this category does not release histamine?

How can you help prevent histamine release?

Answer 40

the exception is cisatracurium.

release histamine can cause increase airway resistance and bronchospasm in patients with hyperactive airway disease
also, skin flushing, hypotension, decreased SVR, increased pulse rate.

slow administration over 60 sec.
prophylactic use of combined histamine H1 and H2 receptor antagonists.

Question 41

In typical doses are steroidal NMBD associated with histamine release?

Answer 41

NO

Question 42

which type of reaction is mediated through immune responses involving immunoglobulin E antibodies fixed to mast cells?

Answer 42

anaphylactic

Question 43

not immune mediated and represent exaggerated pharmacologic responses in very sensitive individuals who represent a very small portion of the population

Answer 43

anaphylactoid reaction

Question 44

Treatment of analyphylaxis?

Answer 44

Turn the gas off and 100% 02

IV epi 10-20 micrograms/kg (subq if no IV)

TELL THE SURGEON bc he needs to close and you are going to wake up the patient.

If IV blows before succ is given then you gas em and get an IV.

consider intubation if angioedema develops

If you give them a pressor and it stops working (push) then give fluids they may need the circulation (give norepinephrine or a phenylephrine)

treat dysrhythmias

Question 45

Succinylcholine what is adequate dose and what do we actually use?

Answer 45

0.3-0.5 mg/kg is adequate, 1.0-1.5 is commonly used.

Question 46

half life of succ?

what order kinetics does it follow?

Answer 46

47 sec.

first order kinetics

Question 47

side effects of Succ?

why does it have these side effects?

when are these side effects most likely to occur?

How do you prevent/treat this side effect?

Answer 47

Sinus brady, junctional rhythm and sinus arrest may follow administration of Sch.

This reflects actions of Sch at cardiac muscarinic cholinergic receptors where it mimics the physiologic effects of acetylcholine

Most likely to occur when two doses are given with in 5 minutes

Atropine is effective in treating and preventing bradycardia.

Question 48

can succ. cause increased HR and increased BP?

Answer 48

YES! reflects succs effect on the autonomic ganglia (acting like acetylcholine)

Question 49

administration of succs during laryngoscopy and tracheal intubation have sometimes resulted in what?

Answer 49

Ventricular dysrhythmias

Question 50

Succs can cause a transient increase in what?

Do to this what patients should not have succs?

Answer 50

transient increased in plasma potassium of 0.5mEq/L (well tolerated in normal patients)

Patients with renal failure are more susceptible to exaggerated potassium increases. caution should be taken in the following patients: renal failure
metabolic acidosis 
closed head injury
burns
hemiplegia or paraplegia
muscular dystrophies, GB
abdominal infections.

Question 51

Is succs used routinely in children?

Answer 51

succs use in children should be for emergency tracheal intubation only bc of the risk of undiagnosed muscle disease leading to death with use in children under the age of 12.

Question 52

myoglobinuria and rhabdo caused in patients due to succs means what?

Answer 52

they have MH or muscular dystrophy

Question 53

Why is succs. not widely accepted in open eye cases?

Answer 53

can cause increased IOP with peak in 2-4 min and duration of 6 min.

Question 54

is regurgitation a problem with succs. use?

Answer 54

NO, does not predispose people to regurgitation.

Question 55

Myalgia and succs?

Answer 55

muscle pain can happen due to succs. use. even with defasciculation dose of non depolarizers.

Question 56

Masseter spasm and succs, tell me about it?

Answer 56

Sch is a trigger for MH, if this was to occur then you may have masseter spasm. OTHER possibilities is you did not give enough succs or you need to let it work longer, these two scenarios should trump the forethought of MH. Masseter spasm would be the earliest sign of MH but not the most sensitive sign.

Question 57

ABSENCE OF FADE AND TETANIC TO TOF describes which kind of NMB?

Answer 57

Depolarizing NMB = Succs. (phase I)

Question 58

what is phase II in relation to succs?

Answer 58

PHASE II BLOCKADE IS PRESENT WHEN THE POST JUNCTIONAL MEMBRANE HAS BECOME REPOLARIZED BUT STILL DOES NOT RESPOND NORMALLY TO ACh (DESENSITIZATION NEUROMUSCULAR BLOCKADE)

Question 59

phase II, how does it act on TOF?

Answer 59

Fade is seen in response to TOF when in phase II (bc in phase one their is no fade seen, just the same all the way across)

Question 60

What is responsible for the fasciculations seen with succs?

Answer 60

SUSTAINED DEPOLARIZATION PRODUCED BY THE INITIAL ADMINISTRATION OF SCh IS INITIALLY MANIFESTED AS TRANSIENT GENERALIZED SKELETAL MUSCLE CONTRACTIONS

Question 61

What mechanism from succs. is responsible for the increased potassium?

Answer 61

SUSTAINED OPENING OF SODIUM CHANNELS PRODUCED BY SCh IS ASSOCIATED WITH LEAKAGE OF POTASSIUM FROM THE INTERIOR OF CELLS

Question 62

is plasma cholinesterase present in the NMJ?

Answer 62

NO, plasma cholinesterase rapidly hydrolyzes and decreases the amount of SCh in the extracellular fluid before reaching the NMJ.

Question 63

SCh should NOT be given to patients 24-72 hours after? and why?

Answer 63

major burns
trauma
extensive denervation of skeletal muscles.

may result in acute high potassium and cardiac arrest.

Question 64

what happens if you give a 2nd dose of SCh within five min of the first dose?

Answer 64

cardiac dysrhythmias are most likely to occur (bradycardia then asystole)

Question 65

what would you give to decease the likelihood of a cardiac response to sux?

Answer 65

atropine 1-3 min before sux.

Question 66

Does atropine IM reliably protect against sux induced bradycardias?

Answer 66

NO IM atropine does not.

Question 67

if you have given a NMB and your patient has four twitches what can that mean?

Answer 67

75% or less receptors are blocked, thus it means 75% of receptors could be blocked and you see four twitches.

Question 68

If you see 0 twitches on TOF after giving a NMB what would that mean?

Answer 68

100% receptors are blocked.

Question 69

Twitches on the TOF with correlating amount of receptors that could be blocked, tell me all of em?

Answer 69

4 = NO DRUGS

4 = WITH DRUG = 75% OR LESS RECEPTORS BLOCKED

3 = WITH DRUG = 85% OR LESS RECEPTORS BLOCKED

2 = WITH DRUG = 95% OR LESS RECEPTORS BLOCKED

1 = WITH DRUG = 99% OR LESS RECEPTORS BLOCKED

0 = WITH DRUG = 100% RECEPTORS BLOCKED

Question 70

what enzyme is highly concentrated at the NMJ?

Answer 70

acetylcholinesterase

Question 71

Acetylcholinesterase is fast, just how fast is it?

Answer 71

it can hydrolyze nearly as fast as the rate of diffusion!

Question 72

In the NMJ what kind of receptors is Ach trying to reach?

Answer 72

nicotinic acetylcholine receptors.

Question 73

What are the three acetylcholinesterase inhibitors?

Answer 73

Neostigmine (common)

Edrophonium

Phridostigmine (less common)

Question 74

How do acetylcholinesterase inhibitors work?

Answer 74

The acetylcholine that accumulates at the neuromuscular junction after administration of neostigmine competes with the residual molecules of neuromuscular blocking drug for the available unoccupied nicotinic acetylcholine receptors at the neuromuscular junction.

Question 75

once the inhibition of Achesterase is complete does administering additional doses of neostigmine serve any purpose?

Answer 75

NO

Question 76

How do you know if neostigmine has done it’s job?

Answer 76

when you get a 4th response on TOF

Question 77

When will you leave your patient tubed after NMB?

Answer 77

if LESS than 4 twitches

Question 78

what should you have before you even give neostigmine?

Answer 78

at least one twitch

Question 79

what will you give neostigmine with and what are the mg of each?

Answer 79

glycopyrrolate 5mg first then neostigmine 4mg to follow.

Question 80

Neostigmine, what is the MAX effective dose range?

Answer 80

60-80mcg/kg

Question 81

Edrophonium what is its range dose?

Answer 81

1.0-1.5mg/kg range

Question 82

of the three NMBD reversals (acetylcholinesterase inhibitors) which has the longest half life?

Answer 82

pyridostigmine

Question 83

Renal excretion is 50% or more for the three NMBD reversals, what does this mean?

Answer 83

Renal failure decreases the plasma clearance of all three as much as or more than that of the longer acting NMBD

Question 84

why is glyco co-administered with acetylcholinesterase inhibitors and anticholinergics?

Answer 84

to minimize the muscarinic cardiovascular side effects. BC by inhibiting the break down of Ach you increase Ach in all synapses all over the body not just at the NMJ.

Question 85

Acetylcholinesterase inhibitor and anticholinergics should be given at what push rate?

Answer 85

slowly over 2-5 min.

Question 86

tell me which Acetylcholinesterase inhibitors and anticholinergics are co-adminstered?

Answer 86

Atropine 7-10 mcg/kg and edrophonium 0.5 – 1.0 mg/kg both are rapid

Glycopyrrolate 7-15 mcg/kg and neostigmine 40-70 mcg/kg both are slower

Glycopyrrolate also pairs with pyridostigmine

Question 87

long acting steroidal NMB? (greater than 50 min)

Answer 87

PANCURONIUM (the other two are intermediate (vec and roc))

Question 88

Benzylispquinolinium long intermediate and short acting NMB.

Answer 88

long= tubocurarine

intermediate = atracurium and cisatracurium

short = mivacurium

Question 89

if someone has a pre-existing cardiac dz which anticholinergic is desired? WHY?

Answer 89

glycopyrrolate over atropine.
Atropine tends to overshoot on the increase in HR which creates myocardial demand for 02 and possibility of heart attack.

Question 90

list the side effects of anticholinergic’s? (atropine, glyco, scopalamine)

Answer 90

hot as a hare
dry as a bone
blind as a bat
red as a beat
mad as a hatter

Question 91

cholinergic mnemonic?

Answer 91

SLUDGEM
saliva
lacrimation
urination
diarrhea
GI cramping
emesis
Miosis/muscle twitching

Question 92

what should be the milligram max of neostigmine and what should be the mcg max?

Answer 92

40-70 or 60-70mcg/kg

5MG SHOULD BE THE MAX!

Question 93

Whats a good dose of glycopyrolate according to the ppt?

Answer 93

7-15mcg/kg is a good dose

Question 94

what two drugs prevent the cardiac muscarnic effects (bradycardia)?

Answer 94

atropine or glycopyrrolate. (robinul most commonly used)

Question 95

Highly water soluble with a hydrophobic cavity large enough to encapsulate steroidal neuromuscular blocking drugs?

Answer 95

SUGAMMADEX

Question 96

What NMB does sugammadex work on?

Answer 96

Rocuronium > Vecuronium&raquo_space; Pancuronium (steroidal)

Question 97

Will sugammadex work on Nimbex, Atrocurium, or Tobac?

Answer 97

NO

Question 98

what is so great about sugammadex and with which NMB does it work the best?

Answer 98

works the best with Rocuromium.

Has a very high associate rate and very low dissociate rate with rocuronium. Estimated for every 30 million Sugammadex-Rocuronium complexes, only one complex will disassociate.

Reversal can be accomplished even during profound neuromuscular block because of its encapsulation method.

Question 99

Does sugammadex bind to plasma proteins?

Answer 99

No

Question 100

how is sugammadex, sugammadex-rocuronium complex eliminated?

Answer 100

urinary elimination is the major route.

Question 101

Rocuronium is eliminated primarily by?

Answer 101

biliary excretion (75%) and renal (10-25%)

Question 102

who would clearance of sugammadex-Roc complex be decreased in?

Answer 102

Patients with substantial renal impairment.

Question 103

who should avoid sugammadex?

Answer 103

patients with a creatinine clearance less than 30ml/min

Question 104

if you have already given sugammadex and want to cause NMBlockade what would you use?

Answer 104

NMBD that is under the cat. benzylisoquinolinium bc Sugammadex does not work on those!

Question 105

can you use sugammadex if no twitches?

Answer 105

yes, max dose for profound block is 8-16mg/kg

Question 106

whats another name for Sugammadex?

Answer 106

BRIDION

Question 107

Which two steroidal NMB drugs will you use Bridion for?

Answer 107

Roc and Vec only (not pancuronium)

Question 108

Bridion can reverse profound block in how long?

Answer 108

2-3 min.

Question 109

Sugammadex- does it have any cardiovascular effects and what weight do we give it based on?

Answer 109

No cardiovascular effects and you give it based on actual body weight.

Question 110

Bridion (sugammadex) and birth control?

Answer 110

use a different non hormonal version of birth control if you have had Bridion. Hormonal contraceptives are less effective after being given Bridion. use this other form of birth control for at least 7 days.

Question 111

dose of Sugammadex based on 2 twitches or 1-2 twitches?

Answer 111

2mg/kg for 2 twitches

4mgkg for 1-2 twitches