PHARM - General Anesthesia

Question 1

what is the MOA of most general anesthetics?

what are the exceptions? and what are their MOAs?

Answer 1

• potentiation of GABAa channel activity
  
  • exceptions:
    
    • N₂O: blocks NDMA receptor
    • ketamine: blocks NMDA receptor
    • dexmedetomidine: activates a2 adrenergic receptors

Question 2

which anesthetics have an additional MOA on top of GABA potentiation?

what is this MOA?

Answer 2

volatile agents (sevoflurane)

also enhance the activity of 2-pore K+ channels

Question 3

what is the role of hyponotics in general anthesia?

which barbituate?

Answer 3

barbituates - methohexital, specifically

for induction of electroconculsive therapy

Question 4

what is the role of anxiolytics in general anesthesia?

Answer 4

benzodiazepines - midazolam, specifically

can be used for preoperative sedation & seizure suppresion

Question 5

general anesthetics come in what two routes of adminstration?

Answer 5

• intravenous
• inhaled

Question 6

propofal

• clinical use
• advantages
• AEs

Answer 6

• clinical use: IV sedation (w/ no analgesia) - inducation & maintenance
• advantages
  
  1. NO post-op nausea & vomitting
  • pt wakes up 8-10 min post injection w no hangover d/t
    
    • rapid clearance and recovery
    • low context sensitive T_1/2
• AEs: CV & respiratory depression

Question 7

etomidate

• clinical use
• advantages
• AEs

Answer 7

• clnical use: IV sedation (w/ no analgesia) - induction, but NOT continuous infusion!
• advantages: less CV / respiratory affects - good for unstable cardiac patients ​
• AEs
  
  • nausea and vomitting
  • ​adrenocortial suppresion - no second dose
  • myoclonus

Question 8

which two IV sedative are hyponotic agents without analgesia?

how do their properties differ?

Answer 8

• propofal - for induction AND maintenace
  
  • no N&V
  • but, CV / resp depression
  • other: no hangover
• etomaidate - for induction ONLY
  
  • causes N&V
  • but less CV / resp depression - good for CV unstable patients
  • other: adrenocortiosuppresion

Question 9

ketamine

• clinical use
• MOA
• advantages
• AE/CI

Answer 9

• clinical use: IV sedation + profound analgesia
• MOA: blocks NDMA receptor
• advantages:
  
  • profound analgesia
  • CV stimulation via indirect sympathomimetics
    
    • good for shock patients
• AE: disorientation / illusions on emergenace
• CI: in pts with ischemic heart disease

Question 10

dexmedetomidine

• clinical use
• MOA
• advantages
• MOA

Answer 10

• clinical use: IV sedation + mild analgesia
• MOA: a2 receptor agonist. inhibits inhibitors of VLPO -> GABA release
• advantages: more like physiologic sleep than other agents
• AE: severe CV & respiratory depression - hypoTN, bradycardia

Question 11

what is the role of opioids in general anesthesia?

Answer 11

fentanyl can be used for perioperative anesthesia

is rapid onset and causes profound analgesia

Question 12

which IV sedatives have important CV effects and what are they?

Answer 12

• etomidate: provides cardiovascular stability
• ketamine: cardiovascular stimulant
• propofal & dexmedetomidine: cardiovasculature depression

Question 13

which IV sedative is C/I in patients with ischemic heart disease?

conversely, what is it useful for?

Answer 13

ketamine (CV stimulant)

common used for shock / severely hypotensive patients

Question 14

which IV sedative is useful in hemodynamically unstable patients?

why?

Answer 14

etomidate

causes minimal CV or respiratory suppression

Question 15

which IV sedative is anti-emetic?

Answer 15

propofal

Question 16

which IV sedative is the most severe CV depressant?

Answer 16

dexmedtomidine

Question 17

the rate of induction of inhaled anesthesics depends on which four factors?

Answer 17

1. inspired gas concentration
2. alveolar ventilation rate
3. pulmonary blood flow
4. solubility - inversely

Question 18

how is the concentration of inspired anesthetic controlled?

Answer 18

by modifying the alveolar partial pressure (PP) of the gas containing the anesthetic

at equilibrium the PP in the lungs, blood and brain will all be the same, so the concentration of anesthetic in the lungs = concentation of anesthetic in the brain

Question 19

what determines the solubility of anesthesia?

how is solubility related to to the anesthesia’s rate of induction?

Answer 19

• determined by: blood gas partition coefficient
• is inversely related to the rate of induction

Question 20

list the induction speeds of the inhaled anesthetics from slowest to fastest

Answer 20

halothane -> isoflurane -> sevoflurane -> desflurane -> NO

• halothane = most soluble, slowest induction
• NO = least soluble, fastest onset

Question 21

describe the metabolism of inhaled anesthetics

Answer 21

most are not metabolized and are immediately exhaled by the lung.

volatile agents (esp halothane) undergo some hepatic metabolism

Question 22

what is MAC?

Answer 22

minimum alveolar concentration

lowest concentration of anesthetic at which 50% of patients will not remove in response to a surgical excision

the higher the potency of the anesthetic, the lower the MAC value

Question 23

which inhaled anesthetics have the lowest and highest MAC values?

what does this mean?

Answer 23

• halothane: lowest MAC (< 10%) = highest potency
• NO: highest MAC (> 100%) = lowest potency

Question 24

NO

• what kind of drug
• pharmokinetic properties
• advantages
• AEs

Answer 24

• inhaled anesthetic used in combo w/ other agents to reduce their dosage requirements
• PK properties
  
  • fastest induction (least soluble)
  • lowest potency (highest MAC) - why it cant be used alone*
• advantages:
  
  • little affect on CV / respiratory system
  • NO malignant hyperthermia!!
• AE: hematotoxicity - via inactivation of Vit B-12 dependent enzymes

Question 25

halogenated agents

• what kind of drugs?
• includes what drugs
• pharmokinetic properties
• AEs

Answer 25

• inhaled anesthetics
• includes: halothane, desflurane, sevoflurane, isoflurance methoxyflurane
• PK properties: overall - slower induction & higher potency than NO
  
  • potency: halothane > isoflurance > sevoflurane > desflurane
  • induction: halothane < isoflurance < sevoflurance < desflurane
• AE:
  
  • CV depression
  • malignant hyperthermia

Question 26

malignant hyperthermia

• cause
• presentation
• triggers
• treatment

Answer 26

• cause: mutation of ryanodine receptor leads to Ca++ release from SR
• presentation: muscle rigidity + rapid rise in body temp
• triggers:
  
  • volatile anesthetics (- fluranes)
  • succinylcholine (depolarizing NMB)
• treatment: dantrolene

Question 27

what is the treatment of malignant hyperthermia?

how does it work?

Answer 27

dantrolene

blocks release of Ca++ from the SR

Question 28

what anesthetics can be given if there is a concern for malignant hyperthermia?

Answer 28

non volatile agents - NO, propofal

Question 29

which anesthetic is especially good for inducing anesthesia?

why?

Answer 29

sevoflurane

low pungency

Question 30

which inhaled anesthetic has the most rapid onset?

Answer 30

NO

Question 31

which anesthetic is highly pungent?

what does this mean?

Answer 31

desflurance

means it is NOT good for inducing anesthesia