PK Flashcards

1
Q

Important sources of variability on pharmacokinetics

A
  1. Genetics
  2. Organ Impairment
  3. Critical Illness
  4. Age and body size
  5. Concomitant Drugs
  6. Sex
  7. Pregnancy
  8. Adherence
  9. Environmental
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2
Q

When is TDM useful?

A

-Experimentally determined relationship
-High variability in PK
-Narrow therapeutic window
-No competing drugs that DONT need monitoring

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3
Q

TDM is used for these drugs:

A

-ABX
-Cardiac (procain/dig/lido)
-Bronchodilators (theo)
-Seizure (carb/pheny/val)
-Mood (lithium)
-Psychotics
-IS (CTS)

ABC SIMP

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4
Q

What is monitored and when?

A

-serum/plasma
-whole blood
-oral fluid, urine

samples can be collected after SS but not necessary

specimens at peak/pre dose/random

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5
Q

If observed and expected values differ, determine possible reasons:

A

Pre analytical
* Hemolyzed specimens
* Clotted specimens
* Interferences
* Collection conditions (temperature, light, freeze/thaw)

Non adherence

Dosing issues

Altered abs (food)

Drug interactions

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6
Q

TDM in Outpatient Setting

A

-Missed doses
-Dose time relative to sampling time
-Previous drug conc
-Formulation changes
-Diet changes
-Assay differences
-Pt characteristics, lab data

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7
Q

Individualized dose recommendations using Bayesian estimation of PK parameters

A

uses drug clearance, VD, body weight, renal function, PK parameters to develop precise dosing recommendation

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8
Q

Bayesian

A

-utilizes drug’s behavior in previous patient populations (Vd/Cl) with pt specific info (BW/RF), measured drug concentrations, and PK parameters
-calculated based on the administered dosing regimen (a posteriori), to develop a precise dose recommendation for a specific patient

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