two compartment model
TRANSCRIPT
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Presented Presented By:
Roll Rooma Khalid
M.phil Pharmaceutics
(2014-2016)
ISLAMIA UNIVERSITY BAHAWALPUR
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INTRODUCTION
COMPARTMENT MODELS
TWO COMPARTMENT MODEL(I.V BOLUS)
METHOD OF RESIDUAL
PARAMETERS OF TWO COMPARTMENT
INTRAVENOUS INFUSION
CLINICAL APPLICATIONS
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PHARMACOKINETICS:
pharmacon:drug
kinesis-motion/change of rate
pharmacokinetics is the study of kinetics
of absorption,distribution,metabolism and
excretion(ADME) of drugs and their
corresponding pharmacologic,therapeutic
or toxic responses in man and animals.
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Compartment models are classical
pharmacokinetic models that simulate the
kinetic processes of drug absorption,
distribution and elimination with little
physiologic detail.
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A physiological system is described by
decomposition into number of interacting
substances called compartments.
Mass of well mixed ,homogenous material.
Behaves uniformly.
Exchange material.
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OPEN MODEL:
Administered drug dose is
eliminated from the body by an excretory
mechanism.
CLOSED MODEL:
The drug dose is not eliminated
from the body.
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Many drugs given in single IV bolus dose
demonstrate a plasma level time curve that
does not decline as single exponential
process
In two compartment model drugs the
plasma drug conc. Declines biexponentially
as the sum of two first order process, i.e
distribution and elimination
Does not equilibrate throughout the body
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Drug distributes in 2 compartments
i.e central compartment &
tissue/peripheral compartment.
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Represents the blood ,extracellular fluid
and highly perfused tissues
Drug distributes rapidly and uniformly
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Contains tissues in which drug equilibrates more
slowly
Drug transfer b/w the two compartments is
assumed to be take place by first order processes
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BLOOD SUPPLY TISSUE GROUP
Highly
perfused
Slowly
perfused
Heart,brain,hepatic
portal vein,kidney and
endocrine glands,skin and
muscles
Adipose tissue and
marrow
Bone,ligaments,tendons,c
artilage,teeth and hair
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They differ in whether the drug elimination
occurs from:
the central compartment(Model 1)
the peripheral compartment(Model 2)
or both(Model 3)
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MODEL 1:
Major sites of drug elimination occurs in
organs such as kidney and liver(highly
perfused with blood).
MODEL 2:
Drug is assumed to follow the first order
kinetics
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Rate constants k12 and k21 represents the
first order rate transfer constants for the
movement of drug from compartment 1 to
compartment 2 i.e k12
And from compartment 2 to 1 i.e k21
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Blood sampling
Analyzed for drug content
Distributive phase: drug is diffused into
peripheral compartment till equillibrium is
attained
Elimination phase
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t=0
After an I.V dose drug levels will first
increase,reach maximum and then decline
tmax
Distribution equilibrium
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Values of microconstants cannot be
determined by direct method,graphical
method is used
a+b=k12+k21+k
Biphasic equation:
Cp=Ae-ᵃᵗ+Be-ᵇᵗ
A=D◦(a-k21)/Vp(a-b) : B=D◦(k21-b)/Vp(a-
b)
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Useful procedure for fitting a curve to the
experimental data of a drug when drug
does not clearly follow one compartment
model
I.V administration of drug
Blood sampling
Assay
Data is obtained and plotted on semilog
graph paper,curve line is obtained
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Curve line realationship b/w the log of the
plasma conc.and the time indicates that
the drug is distributed in more than one
compartments
So from data biexponential equation is
derived:
Cp=Ae-ᵃᵗ+Be-ᵇᵗ
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t1/2= 0.693/b
From b ,the regression line for the
terminal exponential/b phase is
extrapolated to y axis
Y-intercept is equal to B
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Values from the extrapolated line are then
subtracted from the original experimenatl
values
Residual plasma conc. Is obtained
Straight line is obtained
Residual plasma conc.
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Apparent volume of distribution
Drug clearance
Biological half life
Elimination rate constant
AUC
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Relates plasma conc. to the amount of
drug in the body
Drugs with large extravascular
distribution,apparent Vd is generally large
Drugs with high peripheral tissue binding
also have large apparent Vd
For polar drugs,apparent Vd is small
Reflects the extent of drug distribution
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Several Vd are calculated as:
Volume of central compartment
Apparent Vd at the steady state
Extrapolated volume of distribution
volume of distribution by area
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Useful for determining drug conc.directly
after an IV injection into the body
Also called initial volume of distribution
Generally smaller than the terminal Vd
Vp as mass balance factor
By plasma conc. and from AUC
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D◦=VpCp
Vp=D◦/A+B
Vp=D◦/k[AUC]
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The rate of drug entry into the tissue
compartment from central compartment is
equal to the rate of drug exit from tissue
compartment into the central compartment
Dtk21=Dpk12
Dt=k12Dp/k21 [Dp=CpVp]
Dt=k12.CpVp/k21
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Vd=D◦/Cp
(Vd)ss=Dt+Dp/Cp
(Vd)ss=Vp(1+k12/k21)
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(VD)ss is a function of transfer constants
k12 and k21 which represents rate
constants of drug going into and out of
time compartment
Magnitude of (VD)ss is dependent on:
a. hemodynamic factors for drug
distribution
b. physical properties of drug
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It is calculated by :
Vd=D◦/Cp
(Vd)exp=D◦/B
B=D◦(k21-b)/Vp(a-b)
(Vd)exp=Vp(a-b)/(k21-b)
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This equation shows that a change in the
distribution of drug which is observed by
change in the value for vp,will be reflected
in change in (Vd)exp
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reduced drug clearance from the body
may increase AUC such that (Vp)ᵦ is eitherreduced or unchanged depending on thevalue of b.
(Vp)ᵦ=(Vd)area=Do/b[AUC]͚͚◦
Cl=Do/[AUC]͚◦
(Vd)ᵦ=Cl/b
(Vd)ᵦ=k.Vd/b
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(VD)b is affected by changes in the overall
elimination rate and by the change in the
total body clearance of the drugs
Useful in calculation of clearance
(Vd)exp>(Vd)ᵦ>Vp
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Changes in disease state may not result in
different pharmacokinetic parameters.
Changes in pk parameters should not lead
to the physiologic changes.
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Apparent Vt is conceptual volume only and
does not represent the true anatomic
volume
Vt=Vpk12/k21
Dt=[k12Dp◦](e-ᵇᵗ_e-ᵃᵗ)/a-b
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Clearance is the volume of plasma that is
cleared of drug per unit time.
Cl=Vd)b
Useful in determining average drug conc.
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Elimination rate constant of central
compartment and tissue compartment
Because of redistribution of drug out of
tissue compartment ,b is smaller than k.
Three rate constants are associated
with two compartment model
k21=Ab+Ba/B+A
k10=ab/k21
k12=a+b-k21-k10
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Biological half life can be determined from
the rate constant.
t1/2=0.693/b
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TWO STEP METHOD:
1. Trapezoidal method
AUCt-∞=Co/ke
2. By using equation
AUCtotal=Co/k10
AUC=B/b+A/a
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I.V infusion requires a distribution and
equillibrium of the drug before the stable
blood level is reached.
Distribution equillibrium.
Constant drug conc. In tissue.
No net change in the amount in the tissue
occurs during steady state.
Time needed to reach steady state blood
level depends entirely on the distribution
half life of drug.
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Equation describing plasma drug
concentration:
Cp=R/Vpk[1-(k-b/a-b)e-ᵅᵗ_(a-k/a-b)e-
ᵇᵗ]
At steady state:
Css=R/Vpk
Infusion rate:
R=CssVpk
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Drugs with long half lives require a loading
dose to more rapidly attain steady state
plasma drug levels
Rapid therapeutic drug levels can be
achieved by using a loading use
Drugs equilibrate slowly into extravasular
tissues,drug equilibrium is not immediate
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Dtk21=Dpk12
Dt=k12Dp/k21
Dt=k12CpVp/k21
Conc. Of drug in the central compartment
at steady state:
(Vd)ss=Dp+Dt/Cp
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(Vd)ss=CpVp+k12VpCp/k21/Cp
(Vd)ss=Vp+k12/k21Vp
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Hydromorphone studies
Drug distribution of Loperamide
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Pharmacokinetic models predict drug
disposition after drug administration.
Statistical methods are used for the
estimation and data interpretation of
pharmacokinetic parameters.
Useful in drug formulation and treatment
regimen.
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The drug behaviour within the body
might be able to fit different
compartmental models depending upon
the route of drug administration.
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