Vet Pharmacokinetics Print File #1

Course Information
(Pharmacokinetics section of BMS 444)

Opening Remarks

• Name: Gordon L. Coppoc, DVM, PhD
• Dr. Mary Ann Elchisak is professor in charge of the course
• First two weeks -- clinical pharmacokinetics
• For assistance: Office -- Lynn G182
  Door Open, come in
  Door Closed, make appointment with me before or after class
• Reference: VPT95, Ch 3, pp 18-36.
• Main Goal:
  To help you understand and to use clinical pharmacokinetics
• See Internet for more information
• On SVM computers, click on "Netscape"
• Then on successive menus in "netscape" "Schools of Purdue University" --> "Veterinary Medicine" --> "Departments" --> "Basic Medical Sciences" --> "Course Syllabi" --> "Clinical Pharmacokinetics -- BMS444 [html]"
• EASIER: type the following into the web browser locator:
  www.vet.purdue.edu/bms/courses/pkin
• Experimental approach, please give me feedback

Veterinary Clinical Pharmacokinetics

• Course information
• General goals
• Typical clinical cases
• Interim summary of cases
• What kinds of drugs do we monitor?
• Detailed goals
• Steady state
• Major pharmacokinetic parameters
• Pharmacokinetic models
• Withdrawal time
• Formulae that must be recalled from memory
• Homework problems

Pharmacokinetics Goals

General Goals

• Pharmacokinetics vs pharmacodynamics
• Diagnosis of toxicoses
• Establishing / adjusting dosage regimens
• Understanding withdrawal times for food safety

Detailed Goals

• Understand terms
  • Steady State
  • First- & Zero-order kinetics / Michaelis-Menten plots
  • Loading Dose / Volume of Distribution
  • Clearance
  • Ke (Elimination Rate) & Half-Life
  • Bioavailability
  • Compartment modeling
    • One compartment model
    • Two (and more) compartment models
• Adjust dose
  • Be able to establish new dose regimens:
  • Be able to account for dose forms available
  • Be able to predict, at steady state, the Peak and Trough concentrations
  • Timing of samples
• Withdrawal time -- primarily for veterinary students
  • Be able to describe significance of withdrawal times
  • Be able to predict theoretical withdrawal time given key parameters
  • Be able to describe effects of changes in dose regimen on withdrawal time

Phenobarbital Case #1

Date: 5/16/95
Name: Kissie
Signalment: Canine, Female, 11 yrs, 12 pounds
History: Seizures started 12/94. Medications started 4/95. Chemistry panel normal
Current Status: No seizures since started current dose regimen
Dose: 12 mg (elixir), PO Dose Interval: 12 h
Time on Dose:3 weeks
Serum Concentration #1: 20.2 mcg/mL @ 2 h #2: 19.9 mcg/mL @ 12 h 

Graphing the data

• Plot data from case on arithmetic graph paper
  • make "y" axis 0 to 50 (mcg/mL serum)
  • make "x" axis 0 to 14 (hours)
  • Plot 2 hr concentration = 20.2 mcg/mL
  • Plot 12 hr concentration = 19.9 mcg/mL

Questions about graph

• What fluid was measured? Why?
• How were sample times chosen?
• Does the concentration change much during the dose interval?
• During this dose interval, will the concentration more than likely go | higher | lower | than the reported values?
• What might the "curve" look like if one had all the data?
  Draw a light dotted line representing your notion of the curve's shape
• Given the two concentrations and sample times, predict whether this drug is eliminated | rapidly or slowly |.
• [scan ] What you should have produced
• [drawing][scan] Graph of phenobarbital concentration versus time
  (scan is figure 1, Ravis et al, AJVR 45:1283-1286, 1984)

Questions regarding the significance of the data

• The concentration is approximately 20.2 ug/mL at 2 hours ... So what?
• The concentration is approximately 19.9 ... So what?
• How does serum/plasma drug concentration relate to effect?
• Procainamide concentration vs effect (Koch-Weser73: , 5th Int. Cong. Pharmacol. Pharmacology and Future of Man. Problems of Therapy, Vol. 3, 1973)

Areas of the graph

• Draw two heavy horizontal lines across graph --
  one at 20 ug/mL -- Label it Minimum Effective Concentration (MEC)
  one at 40 ug/mL -- Label it Minimum Toxic Concentration (MTC)
• Write "often toxic" above the 40 ug/mL line
• Write "insufficient effect" below the 20 ug/mL line

Questions about areas of the graph

• What name might one give to the "middle" area of the graph?
• How might one establish the "minimum toxic" and "minimum effective" concentrations?
• Are these concentrations "absolute"?

Evaluation of the regimen

• Look at the observed concentrations in this case vis-a-vis the therapeutic window you have made
• Note that the "Kissie" has not had seizures for 3 weeks

Questions about the dose regimen

• Should one change the dose and/or schedule for Kissie?
• Why or why not?

Phenobarbital Case #2

Date: 8/9/95
Name: SweetPea
Signalment: Canine, Female, 10 yrs, 5.3 pounds
History:CBC / Chem / VA ---> WNL
Current Status: Improving
Dose:8 mg, PO Dose Interval: 12 h
Time on Dose:2 weeks -- started on 6/14/95, then owners stopped. Started again 2 weeks ago.
Serum Concentration #1: 10.2 mcg/mL @ 11 h #2: none submitted

Plot data

• Plot data from case on arithmetic graph paper
  • May use same graph as did for Case #1, if wish
  • make "y" axis 0 to 50 (mcg/mL serum)
  • make "x" axis 0 to 14 (hours)
  • plot concentration #1 (10.15 mcg/mL @ 11 h)
  • Note: there is no concentration #2

Questions

• Does this value more nearly approximate a "peak" or a "trough"?
• Will the concentration go lower during this dose interval?
  Given what you know about the speed at which phenobarbital is eliminated what is your prediction?
• How was this sample time probably chosen?
• Is it ideal? ...practical?
• Will it introduce significant error in dose adjustment?

Questions regarding the significance of the data

• The concentration is approximately 10.2 mcg/mL at 11 hours ... So what?
• Is the concentration within the target concentration range?
• Is "SweetPea" still having seizures?
• Should the dose be adjusted?
• How might you adjust the dose?

Adjust regimen

• Desired trough concentration is 20 mcg/mL serum
• Measured "trough" concentration was 10.2 mcg/mL serum
• Setup simple proportion formula
  

  New dose = Old dose x (Conc desired / Conc measured)

• Do the calculation

Questions about dosage adjustment

• New dose regimen is approximately 16 mg q12h
• What does q12h mean? bid? q6h? q1d? q1m?
• Will this new regimen result in the drug concentration being in the therapeutic window for the entire dose interval?
• Look at plot for case #1 and predict on the graph paper a Peak for this animal?
• Why can we get away with using only one measurement for phenobarbital in some cases?
• When would it be crucial to know the approximate peak concentration?

Advice to referring veterinarian

Concentration at the trough is approximately half the normally recommended minimum. Because SweetPea is still having seizures, advise increasing dose to 15 mg q12h. If this produces excessive sedation and/or incoordination for more than 3 to 4 days, the evening dose should be decreased to 7.5 mg. After two to three weeks on the new dose, advise submitting a "trough" sample for analysis if SweetPea is still experiencing seizures.

Questions about the recommendation

• Why might sedation and / or incoordination last only 3 to 4 days?
• Why not just decrease both AM and PM doses instead of only one?
  (Hint: what dose forms are there for the medication?)
• Why wait two to three weeks to submit another sample?

Phenobarbital Case #3

Date: 5/18/95
Name: Yukon
Signalment: Canine, Male, 10 yrs, 88 pounds
History:Epileptic for 7-8 years -- last 2 weeks has break through seizures and liver enzymes are elevated
Current Status: Seizures are occurring more often -- 2 last Wednesday
Dose:180 mg, PO Dose Interval: 12 h
Time on Dose:1 year
Serum Concentration #1: 48.4 ug/mL @ 3 h #2: none submitted

Graphing the data

• Plot data from case on arithmetic graph paper
  • May use same graph as did for Case #1 & 2, if wish
  • make "y" axis 0 to 50 (mcg/mL serum)
  • make "x" axis 0 to 14 (hours)
  • plot concentration #1 (48.4 mcg/mL @ 3 h)
  • Note there is no sample #2

Question

• Is this value closer to the "peak" or to the "trough"?
  On what do you base this estimate?
• Will the concentration go lower during this dose interval?
  Given what you know about the speed at which phenobarbital is eliminated what is your prediction about how much lower?
• How was this sample time probably chosen?
• Is it ideal? ...practical?
• Will it introduce significant error in dose adjustment?

Questions regarding the significance of the data

• The concentration is approximately 48.4 mcg/mL at 3 hours ... So what?
• Is the concentration within the target concentration range?
• Is "Yukon" still having seizures?

Adjust regimen

• Normally recommended maximum concentration is 40 mcg/mL
• Should the dose be decreased for Yukon?
• If yes, use same proportion as before, BUT...
• Setup simple proportion formula
  

  New dose = Old dose x (Conc desired / Conc measured)

• Do the calculation

Questions about adjusting regimen

• What is rationale for decreasing the dose?
• What is the probability that phenobarbital alone (at tolerable doses) will ever stop the seizures in Yukon?
• How important would it have been to know the trough concentration in this case?

Advice to referring veterinarian

Concentration at "peak" (48.4 mcg/mL) is clearly above the maximum recommended level of 40 mcg/mL. Because the seizures are not being controlled at this dosage and because the liver enzymes are already elevated (a sign of potential hepatotoxicity), it is unlikely that phenobarbital will be satisfactory as a sole agent. Advise considering reducing dosage by 1/3 and adding KBr to the regimen.

Gentamicin Sample Case

Date: 5/24/95
Name: Allie's 95 cria
Signalment: Llama, Female, born 5/20/95, 29 pounds
History:Cria weak, FPT (plasma transfusion 5/23/95)
Current Status:improving
Dose:27.3 mg IV Dose Interval: 12 h
Time on Dose:since 5/22/95 at 8 PM
Serum Concentration #1: 5.0 mcg/mL @ 1 h #2: 0.9 mcg/mL @ 12 h

Graphing the data

• Plot data from case on arithmetic graph paper
  • make "y" axis 0 to 20 (mcg/mL serum)
  • make "x" axis 0 to 14 (hours)
  • Plot concentration #1 (5.0 mcg/mL @ 1 h)
  • Plot concentration #2 (0.9 mcg/mL @ 12h )

Questions about the graph

• Is this the highest the concentration is likely to be (or have been) during this dose interval?
• Will the concentration go lower during this dose interval?
• Draw your idea of what might the "curve" look like if one had all the data?
• Does the concentration change much during the dose interval?
• What does this change indicate about the "rate of elimination" -- fast? slow?
  Note contrast relative to phenobarbital.
• Is this a first time dose? Can one tell?
• How were sample times probably chosen?
• What fluid was measured? Why?

Questions regarding the significance of the data

• The concentration is approximately 5 mcg/mL @ 1 hour, ... So what?
• The concentration is approximately 0.88 mcg/mL @ 12 hours, ... So what?
• How does the ratio of trough to peak compare to that in the phenobarbital example?

Review of therapeutic window

• Draw horizontal lines across graph at --
  • 12 mcg/mL
  • 5 mcg/mL
  • 1 mcg/mL
• Write "often toxic" above the 12 mcg/mL line, the MTC
• Write "insufficient effect" below the 5 mcg/mL line, the MEC
• Write "need to drop below" below the 1 mcg/mL line, (another MTC?)

Questions about "therapeutic window"

• Where is the therapeutic window in this graph?
• What is the meaning of the "need to drop below" statement
• How might his relate to toxicity of gentamicin
• Are these concentrations "absolute"?
• Note: this is the traditional understanding of ideal gentamicin dosage regimens. New concepts will be presented in the chemotherapeutic section.

Evaluation of the regimen

• Look at the observed concentrations in this case vis-a-vis the therapeutic window
• Note that the "cria" was said to be "improving" -- What does this mean for advising the veterinarian?

Questions about the dose regimen

• Should one change the dose and/or schedule for the Llama cria?
• Why or why not?

Summary

Summary

• Primary hypothesis of target concentration strategies
• Why we use plasma/serum for sampling
• Drug concentration (C) vs Time (t) plots -- proper graphing
• Minimum Effective Concentration (MEC)
• Minimum Toxic Concentration (MTC)
  (added concept of "need" to have low trough in some cases)
• Therapeutic Window; Target Concentration Range
  (related concept of "Therapeutic Index")
• Dosage adjustment -- simple cases --> Simple proportion
• Assumptions for "simple" dose adjustment
  • Dose interval (T) stays same
  • No significant change in animal's handling of the drug
  • Kinetic processes not dose dependent
• Need to pay attention to whether it is peak or trough that you are adjusting!
• Importance of need for knowing "peak" and "trough" concentrations depends on the drug
  New concept: OSCILLATION during dosage interval (more later)
• Best times to take samples

Types of Drugs Monitored

What kinds of drugs do we monitor?

• Think about safety margins
  Example: penicillin G versus gentamicin
• Think of ease of "bioassaying" the drug in the patient, i.e., presence of easily detectable and rapid response
  Example: anticonvulsant versus anesthetic agent
• What if signs of too little and too much drug are similar?
  Example: digoxin
• When interindividual variation is much greater in
  DOSE vs PLASMA CONCENTRATION than in
  PLASMA CONCENTRATION vs EFFECT!