Pharmacology - Local Anesthetics - Vandana Sharma Flashcards

1
Q

In dealing with anesthetics, potency correlates to:

A

Lipid solubility

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2
Q

The onset of action of an anesthetic depends on what factors?

A

pKa
Lipid solubility
The more lipid soluble, the faster the onset of the drug

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3
Q

The duration of action of an anesthetic depends on:

A

Protein binding

binding to alpha-1-acid glycoprotein

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4
Q

What is the MOA of local anesthetics?

A

LA bind reversibly to the intracellular portion of the Na channel and inactivate the channel. The threshold for excitation therefore increases, impulse conduction slows, etc.

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5
Q

Short-acting ester local anesthetics are inherently safer w/r/t systemic toxicity due to their clearance by:

A

pseudocholinesterase

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6
Q

What is a potential complication of continuous spinal catheters infusing lidocaine in order to permit repetitive dosing to facilitate adequate anesthesia?

A

Cauda equina syndrome - severe back pain with motor and sensory deficit, loss of bowel and ladder control

An example of local neural toxicity from LA

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7
Q

What is TNS?

A

Transient Neurological Syndrome
transient pain or dysthesia linked to the use of lidocaine for spinal anesthesia, can be severe

Can occur with lidocaine, procaine, mepivicaine

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8
Q

Why are many people allergic to anesthetics containing esters?

A

para-aminobenzoic acid (PABA) metabolites are known allergens (methylparaben is the preservative that metabolizes to PABA)

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9
Q

What is the order of nerve depolarization?

A
  1. Resting membrane potential
  2. Stimulus –> threshold –> voltage-gated Na channels open
  3. Voltage-gated K channels open –> depolarization
  4. At peak, voltage-gated Na channels close
  5. Repolarization phase –> K channels close
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10
Q

What is preemptive analgesia?

A

The nerve block is performed prior to the incision.

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11
Q

LAs all have a similar structure: the aromatic ring, the intermediate linkage, and the terminal amine. What is the function of the aromatic ring?

A

Aromatic ring = lipophilic portion = greater lipid solubility (correlates to high potency)

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12
Q

LAs all have a similar structure: the aromatic ring, the intermediate linkage, and the terminal amine. What is the function of the intermediate linkage?

A

The intermediate linkage determines the biodegradation and elimination of the drug

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13
Q

LAs all have a similar structure: the aromatic ring, the intermediate linkage, and the terminal amine. What is the function of the terminal amine?

A

The terminal amine tail is able to accept a proton and can go from tertiary to quarternary with a positive charge (weak base)

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14
Q

pKa = pH - log ([H]/[HA])

A

HH equation
when base and acid concentration are equal, log 1=0
and pKa = pH

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15
Q

What is pKa?

A

The pH at which 50% of the molecule exists in ionized form and 50% in non-ionized form

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16
Q

What is the effect is there is a big difference between the pH of the blood and the pKa of the anesthetic agent?

A

Creates more ionized and less lipid soluble (and less potent) drug

17
Q

T/F: Smaller nerves and myelinated nerves get blocked earlier than larger and unmyelinated nerves.

A

True

18
Q

Can transient neurologic syndrome occur after administration of Bupivicaine or Clorprocaine?

A

No

More common in lidocaine (and others)

19
Q

What is the cardiac toxicity associated with local anesthetic use?

A

Much higher doses than CNS toxicity;
Na channel blockade –> depression of myocardial contractility and reduced refractory period
**All local anesthetics except cocaine and ropivicaine are vasodilators which can lead to cardiac arrest

20
Q

What anesthetic has the highest cardiac toxicity potential?

A

Bupivicaine

21
Q

Why is ropivicaine generally a better choice for an anesthetic than bupivicaine?

A

Ropivicaine has a larger therapeutic index, less cardiovascular effects and more CNS tolerance than bupivicaine. It’s also slightly less potent