Drug Interactions Flashcards

1
Q

4 characteristics of drugs that are most likely to pose interaction problems

A
  • Narrow therapeutic index
  • Steep dose-response curve
  • High first-pass metabolism
  • Single, inhibitable route of elimination
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2
Q

2 mechanisms of drug interactions

A
  • Pharmacodynamic
  • Pharmacokinetic
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3
Q

Explain pharmacodynamic drug interactions

A

The intended or expected effect produced by a given plasma level of a drug in the presence of a second drug is altered:

  • Change in drug action w/o altering plasma concentration
  • Concurrent administration of 2 drugs that have a similar/opposite effect
  • Synergistic or antagonistic
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4
Q

Explain pharmacokinetic drug interactions

A

The duration and intensity of a drug’s action is a function of the plasma level of the drug, which is directly related to the drug’s rate of:

  • Absorption
  • Distribution
  • Metabolism
  • Excretion

Measured by a change in one or mre kinetic parameters (i.e. max serm conc and half-life amount of drug excreted)

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5
Q

Explain how PPI’s may affect drug absorption

A

Increase in gastric pH –> may reduce the absorption of drugs (i.e. ketoconazole & itraconazole) which are best absorbed in an acidic environment

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6
Q

3 factors affecting rate of drug metabolism

A
  • Largely the result of oxidation reactions catalyzed by CYP450 enzyme system
  • CYP3A4 alone is involved in the metabolism of about half of all drugs currently prescribed
  • May be increased or decreased based on enzyme induction or inhibition
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7
Q

Consequence of induction

A

Increased rate of metabolism, enhanced oral first pass metabolism, reduced bioavailability –> decreased drug plasma concentration

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8
Q

Substrate for induction and its inducer

A

Substrate: Ibuprofen

Inducer: Phenytoin

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9
Q

Consequene of inhibition

A

Increase in plasma concentration of parent drug –> exaggerated prolonged pharmacologic effect & reduction in metabolite –> possible toxicity

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10
Q

Substrate for inhibition and its inhibitor

A

Substrate: rosiglitazone

Inhibitor: metronidazole

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11
Q

Interaction of NSAID’s with lithium

A
  • Increase plasma lithium concentration
  • Lithium toxicity –> nausea & vomiting, tremors –> slurred speech, confusion –> seizures, coma, CV collapse
  • Mechanism unknown, possibly decreased renal clearance of lithium
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12
Q

Interaction of NSAID’s with ACE inhibitors

A
  • Diminished antihypertensive effect of ACE inhibitors
  • Most concern w/ long term use
  • Mechanism possibly related to ability of prostaglandins to reduce synthesis of vasodilating renal prostaglandins
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13
Q

Interaction of NSAID’s with methotrexate

A

Has been shown to decrease the clearance of methotrexate, probably by reduction on vasodilating renal prostaglandins

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14
Q

Interaction of NSAID’s with warfarin (4)

A
  • Increased risk of warfarin-related bleeding by inhibition of platelet function
  • ASA most significant risk
  • Possible mechanism = displacement of warfarin from plasma protein-binding sites
  • ASA & NSAIDs also produce gastric erosion
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15
Q

Interaction of acetaminophen with warfarin (3)

A
  • Acetaminophen appears to increase anticoagulant effect of warfarin in dose-dependent manner
  • More likely w/ continued daily doses of approx 2g/day acetaminophen
  • Mechanism unknown (inhibition of CYP450 suggested)
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16
Q

Primary interaction of macrolides with other drugs

A

Inhibtion of hepatic microsomal metabolism (inhibit CYP3A-mediated metabolism of many drugs)

17
Q

Exception to general interaction of macrolide with other drugs

A

Increase in digoxin bioavailability caused by erythromycin’s suppression of gut bacteria that normally degrades some digoxin prior to absorption

18
Q

Interaction of metronidazole with other drugs

A
  • Imidazole ring found in many other drugs known to inhibit hepatic drug metabolism (similar shape –> similar effect)
  • Important interaction with warfarin: inhibit metabolism of warfarin –> enhanced anticoagulation effect
19
Q

Interaction of antibiotics with oral contraceptives

A
  • First report of interaction with rifampin (antituberculosis drug and potent inducer of CYP-450 enzyme system) –> increased metabolism of oral contraceptives
  • Failure with other antibiotics less clear –> possible lack of induction of P-450 –> reduced plasma level of steroids