A Textbook of Clinical Pharmacology and Therapeutics

FURTHER READING

Rowland M, Tozer TN. Therapeutic regimens. In: Clinical pharmacoki-

netics: concepts and applications, 3rd edn. Baltimore, MD: Williams

and Wilkins, 1995: 53–105.

Birkett DJ. Pharmacokinetics made easy (revised), 2nd edn. Sydney:

McGraw-Hill, 2002. (Lives up to the promise of its title!)

begins slowly and accelerates as plasma concentration
falls (Figure 3.7).
2.The time required to eliminate 50% of a dose increases
with increasing dose, so half-life is not constant.
3.A modest increase in dose of such a drug disproportionately
increases the amount of drug in the body once the drug-
elimination process is saturated (Figure 3.8). This is very
important clinically when using plasma concentrations of,
for example, phenytoinas a guide to dosing.

16 PHARMACOKINETICS

Case history

A young man develops idiopathic epilepsy and treatment

is started with phenytoin, 200 mg daily, given as a single

dose last thing at night. After a week, the patient’s serum

phenytoin concentration is 25μmol/L. (Therapeutic range is

40–80μmol/L.) The dose is increased to 300 mg/day. One

week later he is complaining of unsteadiness, there is nys-

tagmus and the serum concentration is 125μmol/L. The

dose is reduced to 250 mg/day. The patient’s symptoms

slowly improve and the serum phenytoin concentration

falls to 60μmol/L (within the therapeutic range).

Comment

Phenytoin shows dose-dependent kinetics; the serum con-

centration at the lower dose was below the therapeutic

range, so the dose was increased. Despite the apparently

modest increase (to 150% of the original dose), the plasma

concentration rose disproportionately, causing symptoms

and signs of toxicity (see Chapter 22).

Key points

• Two-compartment model. Following a bolus dose the
  plasma concentration falls bi-exponentially, instead
  of a single exponential as in the one-compartment
  model. The first ( ) phase mainly represents
  distribution; the second () phase mainly represents
  elimination.


• Non-linear (‘dose-dependent’) kinetics. If the
  elimination process (e.g. drug-metabolizing enzyme)
  becomes saturated, the clearance rate falls.
  Consequently, increasing the dose causes a
  disproportionate increase in plasma concentration.
  Drugs which exhibit such properties (e.g. phenytoin)
  are often difficult to use in clinical practice.