Brainscape's Knowledge GenomeTM

Browse over 1 million classes created by top students, professors, publishers, and experts.


See full index

Pharmacology for Anaesthetists > Digoxin > Flashcards

Digoxin Flashcards

1
Q

What is the class and chemistry of digoxin

A

It is an anti-arrhythmic agent

It is a cardiac glycoside derived from the Balkan Foxglove plant

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
2
Q

How can digoxin be administered

A

PO - 2 - 3 hours onset of action

IV - immediate onset of action

(theoretically IM too)

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
3
Q

What is responsible for the portion of digoxin not absorbed

A

80%

P-glycoprotein (PGP) is an enterocyte efflux pump that secretes digoxin back into the GIT after absorption.

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
4
Q

Describe the important pharmacokinetics of digoxin especially with relevance to administration to critically ill patients

A

Hepatic clearance 16%

Kidneys: most of digoxin is excreted by the kidneys unchanged.

Protein bound: 25%

Basically insoluble in water

So overall:

  1. High volume of distribution
  2. Cleared by kidneys

In the critically ill: often increased Vd (increased third spa

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
5
Q

Describe the presentation of digoxin with explanation

A

40% Propylene glycol
10% Ethyl alcohol
50% Distilled water

It has a pKa of 7.15 and is basically insoluble in water.

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
6
Q

Why is a loading dose required for Digoxin

A

Because it has a very high volume of distribution 5.1 - 7.4 L/kg. Loading dose is therefore required to achive a steady state concentration in the body fluids within a reasonable time frame.

Further more, the high volume of distribution makes digoxin entirely unsuitable for dialysis

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
7
Q

Summarise digoxin’s elimination and excretion

A
  1. 16% metabolised in the liver
  2. The rest is excreted unchanged in the kidneys
  3. Vd 5.1 - 7.4 (HIGH)
  4. High lipid solubility

So Elimination t1/2 = 36 - 44 hours

Poor efficacy of dialysis

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
8
Q

Describe the mechanism of action of Digoxin

A

INCREASED MYOCARDIAL CONTRACTILITY

  1. Na is exchanged for Ca by the Na/Ca exchanger during phase 1 of the action potential.
  2. Increased availability of intracellular Na leads to increased subsequent Ca+ entry
  3. Increased Ca availability –> increased contractility
  4. Na usually pumped out of cell by Na/K ATPase

DIGOXIN BLOCKS Na/K ATPase –> increased IC Na –> increased IC Ca –> increased contractility

ANTIARRHYTHMIC EFFECT (INCREASE VAGAL TONE)

  1. AV node blocker (like BB, CCB, Amiodarone)
  2. Slowed conduction time through AV node (rate control in AF) but does not change conduction time in HIS (narrow QRS)
  3. Mechanisms (Potentiates the PSNS)
    - -> Activate baroreceptors (stimulating vagus)
    - -> Sensitise PSNS ganglia
    - -> Sensitize myocardium to Ach

INCREASED AUTOMATICITY (in pacemaker tissues)

  1. Phase 4 of cardiac action potential –> digoxin increases the gradient of the slope of this phase in pacemaker tissues

INCREASED IRRITABILITY (ectopics)

  1. Phase 4 of cardiac action potential –> digoxin increases the gradient of the slope of this phase in purkinje fibres
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
9
Q

Summarise the effects of digoxin on the cardiac action potential

A 
Phase 0 - Lengthened
Phase 1 - shortened
Phase 2 - shortened
Phase 3 - lengthened
Phase 4 - increased slope in pacemaker tissue and purkinje fibres
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
10
Q

When is digoxin indicated?

A
  1. AF in patients with heart failure
    - -> USA: Digoxin is 2nd line agent (i.e. added to a beta blocker)
    - -> Europe: Digoxin is 1st line for severely volume overloaded or haemodynamically unstable patients, but in combination with amiodarone
  2. A possible addition for heart failure
    - -> Consider in symptomatic patients in sinus rhythm to reduce all cause heart failure hospitalizations
    - -> but no effect on mortality
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
11
Q

Should digoxin be used in the ICU as an inotrope with rate control properties

A

Other agents are better

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
12
Q

List the ECG findings characteristic of the digoxin effect vs digoxin toxicity

A

Digoxin effect

  1. Salvadore Dali sagging (reverse tick) ST segments
  2. Flat, inverted or biphasic t waves
  3. Short QT
  4. PR prolonged
  5. Prominent U waves / Peaked terminal portion t waves)
  6. J point depression

DIGOXIN TOXICITY

  1. Supraventricular tachycardia (increased automaticity)
  2. Slow ventricular response (AV node block)

Also
PVCs, Sinus brady, 1/2/3rd degree block, Slow AF, Regularized AF, VT, polymorphic and bidirectional VT

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
13
Q

Why does digoxin have many drug interactions despite having minimal hepatic metabolism

A
  1. Depends on active secretion in renal tubule

2. GIT P-glycoprotein efflux pump (clogged by competing substrates)

How well did you know this?
1
Not at all
2
3
4
5
Perfectly
14
Q

List the pharmacokinetic and pharmacodynamic drug interactions for digoxin

A

PHARMACOKINETIC

  1. Decrease absorption (Antiacids)
  2. Increased absorption
    - -> Amiodarone, verapamil, rifampicin - block PGP efflux
    - -> Macrolides and tetracyline - decr. Gi bacteria metab

PHARMACODYNAMIC

  1. Diuretics: decrease Mg and K –> predispose to digoxin toxicity
  2. Succinylcholine: ? mechanism –> increased irritability –> VF
  3. BB, CCB –> additive AV blockade
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
15
Q

List the side effects of digoxin

A

Cardiac

  • Bigeminy and ectopics
  • Bradycardia + heart block

Non-Cardiac

  • N,V
  • Visual disturbance
  • Delirium and agitation
How well did you know this?
1
Not at all
2
3
4
5
Perfectly
16
Q

List the characteristic features of severe digoxin toxicity

A
  1. Heart block / asystole
  2. Tachyarrhythmias (almost any)
  3. Vasoconstriction
  4. CNS toxicity (almost any)
  5. Hyperkalaemia (Na/K ATPase blocked)
17
Q

Describe the pathophysiology of changing concentrations of potassium on resting membrane potential and nerve excitability

A

DECREASED POTASSIUM
(State Nernst potential becomes more negative)
–> The [K] in vs [K} gradient is now increased –> more positively charged K exits intracellular space and moves extracellular –> less positive charge inside cell (neuron) –> greater electrical potential difference in vs. out –> hyperpolarisation –> reduced nerve excitability –> weakness, ECG changes, bradycardia.

INCREASE POTASSIUM
Opposite effect to above
–> Increase chance of spontaneous action potentials –> high risk VF.

CALCIUM

  • -> Ca+ ensures normal function of Na channels
  • -> Low Ca activates Na channels –> this brings the threshold potential more negative and closer to the resting membrane potential –> spontaneous depolarisation of neurons, tetany and paraesthesias.

Also Ca++ administration (in hyperkalaemia) creates a membrane stabilising effect. Ca++ bind glycoproteins on the outside surface of membrane providing increased positive charge directly apposed to the extracellular side of the membrane which causes temporary hyperpolarization of the RMP.

18
Q

What is the surface charge hypothesis and when is it applicable

A

The administration of Ca++ in hyperkalaemia for ‘membrane stabilisation’. Ca++ attaches to glycoproteins on the extracellular surface of neurons increasing the amount of positive charge directly opposite intracellular side –> temporary hyperpolarisation of RMP and reduces likelihood of spontaneous action potential

Pharmacology for Anaesthetists (37 decks)

Brainscape helps you reach your goals faster, through stronger study habits.
© 2024 Bold Learning Solutions. Terms and Conditions