Anti-Arrhythmic Drugs Flashcards

1
Q

List the classes of anti-arrhythmic drugs.

A

(I) Na voltage channel blockers; (II) ß-adrenergic receptor blockers; (III) drugs that prolong phase 2 and delay repolarization; and (IV) calcium-channel blockers

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2
Q

Describe how class I anti-arrhythmic drugs prevent re-entry.

A

Class I drugs block sodium channels, thereby slowing the phase 0 upstroke and hence slowing conduction and delaying repolarization; lengthened repolarization

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3
Q

Describe the function of class II drugs.

A

Class II drugs block the ß-adrenergic receptors, which lowers the heart rate in SA and AV nodal cells.

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4
Q

Class I drugs primarily work on ___________.

A

fast-contracting myocytes

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5
Q

Class Ib drugs only affect _________.

A

sodium channels, thus they shorten action potential duration

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6
Q

Class Ia and Ic drugs also affect __________.

A

potassium channels, so phase 2 is lengthened

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7
Q

Class Ib drugs do not ___________.

A

prolong phase 2, but they do lengthen action potential duration

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8
Q

The three main class Ia blockers are __________.

A

quinidine, procainamide, and disopyramide

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9
Q

The three main class Ib blockers are ___________.

A

lidocaine, phenytoin, and mexiletine

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10
Q

Of the class I drugs, _____ have the most powerful effect on prolonging the refractory period.

A

Ic (such as propafenone and felcainide)

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11
Q

Describe the “use-dependent” blocking effects of class I drugs.

A

Sodium channels are only blocked by class I drugs when they are open, so drugs tend to affect cells whose sodium channels are hyperactive; this effect is important both for myocytes that are firing too quickly and for pain receptors.

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12
Q

Blocking sodium channels prolongs the refractory period because many class I drugs ____________.

A

have a higher affinity for the inactive state of the channel, thus blocking the channels well into the next cycle and decrease the availability of channels to open upon the next depolarization

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13
Q

Class I drugs are great at treating re-entrant arrhythmias because they ____________.

A

slow conduction velocity (which results in a dampened current that passes through the bloc) and lengthen the refractory period

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14
Q

ß-blockers are used to treat arrhythmias that result from ___________.

A

AV node re-entry, because ß-blockers preferentially lengthen the refractory period in AV and SA myocytes

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15
Q

ß-blockers make it harder for myocytes to depolarize because they ________; they also lengthen phase 2 by __________.

A

inactivate I(funny) channels; dampen the CaL and Ikr/Iks response

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16
Q

Most, but not all, class III drugs block ________.

A

Ikr

17
Q

Class IV drugs also lengthen phase 2, but they do so by ___________.

A

blocking CaL channels, which slows the phase 0 upstroke and decreases the extent of depolarization; with a decreased depolarization peak, fewer Ik channels open and phase 2 is prolonged

18
Q

Adenosine is an ___________; it works by ____________.

A

unclassified antiarrhythmic drug; binding to a GPCR that inhibits adenylate cyclase (and thus works like a ß-blocker) and then activates a subunit which then activates potassium channels

19
Q

The fibrillations which are manageable with meds are ________.

A

atrial, most of which arises from re-entry; all other are better treated with ICDs

20
Q

What’s the most important class III drug?

A

Amiodarone

21
Q

_______ and ________ are pure potassium-channel blockers/

A

Ibutilide and dofetilide

22
Q

The antiarrhythmic with the shortest half-life is __________.

A

adenosine