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Section IBasic principlesfor clearance define the removal of drug from the body, which is the product of the
rate constant for elimination k 10 and V 1 , the volume of distribution of the central
compartment. For example, propofol has a k 10 of approximately 0.12, so about 1/8
of the plasma-equivalent volume has drug removed by elimination in unit time. For
propofol, V 1 is about 16 litres and k 10 is approximately 0.12, so the clearance of propo-
fol is 16×0.12, which is about 2 litres per minute. Remifentanil has a much smaller
central compartment volume but a higher k 10 ,sothe clearance of remifentanil is 5.1
×0.5, which is 2.5 litres, quite similar to that of propofol. If we do not know V 1 we
could use Vintialas an estimate but it is often inaccurate due to sampling artefacts at
early times when mixing has not taken place. Instead, clearance is usually calculated
from the area under the concentration–time curve:Clearance=Dose/AUC.Elimination of drug from the model represents both metabolism and excretion of
unchanged drug. Metabolism may occur in many sites and be organ-dependent
or independent; a clearance that is greater than hepatic blood flow suggests that
hepatic elimination is not the only route of elimination – either there are other sites
of metabolism or the drug is excreted unchanged, for example through renal or
pulmonary routes. Remifentanil has a very high clearance because it is eliminated
bynon-specific esterase in both plasma and tissue.
Inter-compartmental clearance relates to the movement of drug between
compartments; C 12 and C 13 define drug transfer between compartments 1 and 2 and
1 and 3, respectively. For drugs with comparable compartmental volumes, the higher
the inter-compartmental clearance the more rapidly distribution and re-distribution
takes place.Time constant and half-life (t1/2)
Inthe single-compartment model there is just a single exponential relationship
between plasma concentration and time. The time constant defines how quickly
the plasma concentration falls with time and is defined as the time it would have
taken plasma concentration to fall to zero if the original rate of elimination had con-
tinued (Figure6.11). Time constantτhas units of time, usually minutes. The half-life
is the time taken for the plasma concentration to fall to 50% of its initial value. In the
mathematics section we saw that half-life is related to time constant by a constant of
proportionality and half-life is ln2.τ, that is, half-life is 0.693.τ; the half-life is shorter
than the time constant. Note that either half-life or time constant may be used to rep-
resent the time dependency of an exponential process. In the multi-compartment
models there are several hybrid time constants each of which relates to one of the
distinct exponential phases of drug elimination. As mentioned above, these do not
relate directly to any one of the individual rate constants in the model.