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DETERMINATION OF PK PARAMETERS FROM URINARY DATA

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CHAPTER 5 DETERMINATION OF PK PARAMETERS FROM URINARY DATA Calculation of kel from Urinary Excretion Data after I.V. Injection kel can be calculated from urinary ... – PowerPoint PPT presentation

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Title: DETERMINATION OF PK PARAMETERS FROM URINARY DATA


1
CHAPTER 5
  • DETERMINATION OF PK PARAMETERS FROM URINARY DATA

2
Calculation of kel from Urinary Excretion Data
after I.V. Injection
  • kel can be calculated from urinary
  • excretion data.
  • The excretion rate of the drug is
  • assumed to be first order.
  • ke is the renal excretion rate
  • constant.
  • Du is the amount of drug excreted
  • unchanged in the urine.

3
Elimination
  • kel ke km

4
Scheme of the Model
  • For a single i.v. dose,

DB CpVd
ke
IV Dose
Du
km
dDu/dt keDB
5
Rate of Drug Excretion in the Urine
  • Equations
  • But DB DB0e-kelt
  • Therefore,

dt
6
Plotting on a Semilog Paper
  • Plot dDu/dt vs. Time

7
Example
Time Du (mg) Du/t mg/hr t (hr)
0.25 160 160/0.25 640 0.125
0.5 140 140/0.25 560 0.375
1.0 200 200/0.5 400 0.750
2.0 250 250/1 250 1.50
4.0 188 188/2 94 3.0
6.0 46 46/2 23 5.0
8
Difference between t and t
  • t is the time interval for collection of urine
  • sample.
  • t is the midpoint of collection period.
  • Assuming renal clearance is constant, Du/t
  • is proportional to plasma drug conc, and
  • plotting Du/t vs. t is like plotting Cp vs.
    time.
  • The measured urinary excretion rate reflects
  • the average plasma concentration during
  • the collection interval.

9
Why t ?
  • Because the drug urinary excretion rate
  • (dDu/dt) cannot be determined
  • experimentally at any given instant.
  • In practice, urine is collected over a
  • specified time interval, and the urine
  • specimen is analyzed for drug.
  • An average urinary excretion rate is then
  • calculated for that collection period.
  • The average dDu/dt is then plotted against
  • the average time (t).

10
Determination of the non-renal rate constant (knr)
  • knr is the elimination rate constant for any
    route of elimination other than renal excretion.
  • kel - ke knr
  • Since drug elimination occurs mainly through
    renal excretion and metabolism,
  • knr ? km
  • kel ke km

11
Determination of renal clearance
  • Renal clearance, ClR, is defined as the volume of
    plasma that is cleared of drug per unit of time
    through the kidney

12
Sigma-Minus Method
  • Also called the Amount of Drug Remaining to
  • be Excreted Method.
  • It is an alternative method for the calculation
  • of kel from urinary excretion data.
  • It is more accurate than the previous method.
  • ke/kel is the fraction of drug excreted
  • unchanged in the urine.
  • (ke/kel)Dose total amount of drug excreted
  • unchanged in the urine.

13
Sigma-Minus Method (cont)
  • Equations
  • Where,
  • Du is the cumulative amount of drug excreted
  • unchanged in the urine until time t.
  • (1- e-kelt) is the fraction of drug lost from
    the
  • body.

14
Sigma-Minus Method (cont)
  • The amount of drug that is ultimately excreted at
    time infinity will be equal to Du?
  • Du? ke/kel (D0) (2)
  • By substituting in the previous equation (1)
  • Du? - Du Du? e-kelt (3)
  • To obtain a linear equation
  • Ln (Du? - Du) ln Du? - kelt (4)
  • Where, (Du? - Du) is the amount of drug remaining
    to be excreted.

15
Sigma-Minus Plot
  • On a semilog paper

16
Example
  • Use these data to calculate kel

Time (hr) Du (mg) Du (cum) Du? - Du
0.25 160 160 824
0.5 140 300 684
1.0 200 500 484
2.0 250 750 234
4.0 188 938 46
6.0 46 984 0
17
Cumulative Amount of Drug Excreted in the Urine
  • Plot

One needs to collect urine samples for a minimum
of 7-10 half-lives of the drug to assure all the
drug is excreted into the urine.
Du?
Cumulative amount excreted
Time
18
Renal clearance
  • Renal clearance can be determined from model
    independent equation

19
Fraction of drug excreted
  • The fraction of drug excreted unchanged in the
    urine (fe) can be calculated as follows

20
Comparison between the Rate and the Sigma-Minus
Method
  • 1- In the rate method, Du? need not be known, and
    the loss of one urine specimen does not
    invalidate the entire study.
  • 2- The sigma-minus method needs accurate
    determination of Du? which requires urine
    collection until drug excretion is complete.
  • 3- Fluctuations in the rate of drug elimination
    and experimental errors (such as incomplete
    bladder emptying) cause considerable departure
    from linearity in the rate method.

21
Comparison (cont)
  • 4- The sigma-minus is less affected by
    fluctuations in the rate of drug elimination.
  • 5- The rate method is applicable to zero-order
    elimination process, while sigma-minus method is
    not.
  • 6- The ke can be obtained from the rate method
    but not from the sigma-minus method.

22
Problems in Obtaining Valid Urinary Excretion Data
  • 1- A significant fraction of unchanged drug must
    be excreted in the urine( at least 20 ).
  • 2- The assay technique must be specific.
  • 3- Frequent sampling is necessary for a good
    curve description.
  • 4- Urine samples should be collected until almost
    all drug is excreted(7 t half)
  • 5- Variation in urinary pH and volume cause
    significant variation in urinary excretion rates.
  • 6- Subjects should be instructed to the
    importance of complete bladder emptying.
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