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Bioavailability Metrological aspects Assessment of parameters

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Title: Bioavailability Metrological aspects Assessment of parameters

1
BioavailabilityMetrological aspectsAssessment
of parameters
Update july /211/2006
2
Bioavailability

Bioavailability quantifies the proportion of a
drug that is absorbed and available to produce
its systemic effect
extent
rate

3
Bioavailability

Definition
Absolute
amount of administered drug which enters the
systemic (arterial) circulation and the rate at
which the drug appears in the blood stream
Relative
to compare formulations (bioequivalence)
to compare routes of administration

4
Bioavailability vs. absorption
5
Bioavailability vs. absorption

Absorption movement of drug from the site of
administration into the blood which drains the
site of administration
Bioavailability refers to the amount of drug
which actually gains the access to the systemic
(arterial) circulation

6
Bioavailability vs. Bioequivalence
7
Assessment of drug absorption and bioavailability
8
Assessment of drug absorption and bioavailability

in silico predictive model
Physicochemical methods
in vitro methods
in situ methods
in vivo methods

9
Screening for absorption
screen order
increased degree of complexity
in vivo/ human data
intestinal loop
bioavailability absorption profile throughout
the gastro-intestinal tract "Loc-i-Gut"
perfusion in situ
awake animal absorption in specified region
perfusion in vitro
liver
Ussing chamber
blood flow
cell cultures
well defined flow Differentiates between
apsorption and absorption
intestinal sacs or rings
cell suspensions membrane vesicles
well defined flow
hetero-genous cells cell layers
W/O partition
Ungell, Drug Dev. Indus.Pharm. 1997 23 879-892
10
Assessment of drug absorption and bioavailability

In silico
models based on molecular structure
many physicochemical parameters (H. bounding, MW,
LogP, pKa, polar surface area) and solubility can
be generated automatically from chemical
structures
many software to achieve these measurements

11
Assessment of drug absorption and bioavailability

Physicochemical methods
experimental determination of physicochemical
parameters to predict permeability

12
Assessment of drug absorption and bioavailability

In vitro methods cell based methods
Caco2 (human colonic cell lines)
drawback 21 days culture / overexpression of P-gp
do not model paracellular passages (water soluble
molecules of low MW)
3 days culture Caco-2
Madin-Darby canine kidney (MDCK)
3 days correlation with Caco-2 culture
Caco-2 cells engineering to express CYP3A4

13
Assessment of drug absorption and bioavailability

In vitro methods tissue based methods
Ussing chamber technique
Everted gut sac
perfused isolated intestinal segment
unlike Caco-2 cells these models possess an
apical mucus layer
possibility to study drug transport in
combination with intestinal metabolism

14
Assessment of drug absorption and bioavailability

In situ model
perfusion of segment of small intestine
sampling from mesenteric and portal vein

15
Assessment of drug absorption and bioavailability

IN VIVO METHODS

16
Bioavailability in man prediction from rodents,
primates dogs
From Grass ADDR 2002 pp433
17
Main steps for bioavailability (oral route)
18
Main steps for bioavailability (oral route)
Administered dose
Disintegration
in vitro dissolution test
Fab
Dissolution
F
caco-2, everted sac ex vivo
Absorption
Fh
Hepatic first pass effect
hepatocytes culture (intrinsic clearance)
Pulmonary first pass effect
Fp
in vivo difference A.V.
bioavailable fraction of the dose (reaching the
systemic circulation)
19
Bioavailability oral route and first pass effect
30 60
30
fp 0.50
Gut
Portal vein
PO
60
80
Lung
Vena cava
100
30
60
20
60 80
CD
GG
fh 0.75
80 100
20
Heart
fabs 0.8
30
arterial circulation 30
30
F fabs x fh x fp 0.8 x 0.75 x 0.5 0.3
20
First pass effect (oral route)
Gut Lumen
Gut Wall
Portal vein
CYP P-Gp
Liver
To site of measurement
Gut Metabolism
Hepatic Metabolism
To feces
21
Bioavailability by oral route

F fabs x ffirst pass
ffirst pass fraction escaping the different
first pass effects

fabs absorbed fraction
22
Sites of first-pass elimination

Intestinal mucosa
- Cyp enzymes
Liver
- Cyp enzymes

- P-glycoprotein
23
Non-nitrogenous Substances that Effect Drug
Metabolism by Forming Complexes with CYPs

Grapefruit juice - CYP 3A4 inhibitor highly
variable effects unknown constituents
D.G. Bailey, et al. Br J Clin Pharmacol 1998,
46101-110
Isosafrole, safrole - CYP1A1, CYP1A2 inhibitor
found in root beer, perfume
Piperonyl butoxide alcohol -CYP1A1, CYP1A2
inducer insecticide constituent

24
Grapefruit Juice Facts

GJ or G (not OJ) elevates plasma peak drug
concentration, not elimination t1/2
GJ reduced metabolite/parent drug AUC ratio
GJ caused 62 reduction in small bowel enterocyte
3A4 and 3A5 protein liver not as markedly
effected (i.v. pharmacokinetics unchanged)
GJ effects last 24 h, require new enzyme
synthesis
Effect cumulative (up to 5x Cmax) and highly
variable among individuals depending upon 3A4
small bowel basal levels

25
Drugs with first-pass metabolism or
P-glycoprotein transport
Aldosterone morphine Cyclosporine nortriptyline
Isoproterenol organic nitrates Lidocaine proprano
lol
26
Reasons for knowing the absolute bioavailability

To assess a possible major source of therapeutic
variability
if mean F close to 100 no inter-individual
variability of AUC
if mean F is low (eg 10) large
interindividual variability due to formulation or
physiological condition

27
Absolute bioavailability and interindividual
variability
125
100
75
CV ()
50
25
0
0
25
50
75
100
125
150
F
Hellriegel et al, 1996 Clin. Pharmacol. Ther
28
Drawback of a low absolute availability
overexposure of some animals (side effects)
AUC
undesired concentration
therapeutic concentration
Bioavailability
underexposure of some animals (therapeutic
failure, resistance)
1
3
2
Dose
29
Why is an intravenous PK study required ?

To know absolute bioavailability because
absolute low bioavailability is generally
correlated with a poor intersubject
reproducibility
and
poor intersubject reproducibility generally leads
to a more than proportional increase in dose rate
to ensure drug efficacy in animals with the
lowest bioavailabilty

30
Drawback of a low absolute availability

Possible interaction with a spurious increase of
bioavailabilty
The case of felodipine

31
Effect of Grapefruit Juice on Felodipine Plasma
Concentration
Review- D.G. Bailey, et al. Br J Clin Pharmacol
1998, 46101-110
32
BioavailabilityRelevance of the rate of
absorption

The 3 AUC are equal
The rates of absorption are different

CE1
CE2
33
The main steps of bioavailabilityImportance of
the rate of absorption
Administered dose
mean disintegration time
Disintegration
mean dissolution time
Dissolution
MRToral
Absorption
mean absorption time
First pass effect (Lung, Liver)
mean disposition time
Arrival in the systemic circulation
34
The absolute bioavailability
35
Bioavailability

By IV route 100 by definition
(except if it is a prodrug e.g. Ramipril)

36
Corticosteroid preparations

Methylprednisolone (medrol)

CH3
37
Methylprednisolone (MP) and methylprednisolone
succinate (MPS) disposition after an IV
administration of MPS or MP (4 mg/kg)
plasma concentration (ng / ml)
105
104
MP, IV
103
MP after MPS
102
MPS
10
0
60
120
240
360
480 minutes
Toutain, J. Pharm. Sci.
38
How to measure an absolute bioavailability?

Principle
Dose IV AUC IV x Cl IV
Dose EV AUC EV x Cl EV
Assumption Cl IV Cl EV
F x 100

Dose EV Dose IV
AUC EV AUC IV
39
How to measure an absolute bioavailability?

If the doses are equal
F x 100
If IV and EV doses are different
F x x 100
Other possible methods (metabolite, urinary data,
in steady state conditions, without IV, )

AUCEV AUCIV
AUCEV DoseIV AUCIV DoseEV
40
How to measure an absolute bioavailability?

Assumption Cliv Clev
crossover design risk of carryover effect
induction / inhibition
appropriate washout (PK and PD)

41
Bioavailability estimation by semisimultaneous
drug administration
Karlsson Breberg J Pharmacokinet Biopharm 1990
18 pp102
42
Influence of permanent cannulation of the jugular
vein on PK parameters of antipyrine(low
extraction drug, not bound to plasma protein)
2h 48h
T1/2 (Hr) 1.5 1.9
Vd (L/kg) 0.87 0.95
Cl (ml/kg/min) 6.84 5.66
Chindaviak et al JPET 1988 246 1075-1079
43
Bioavailability of antipyrine in ratsinfluence
of permanent cannulation
Sequence Washout 4days IV then Oral Oral then IV
AUCiv 1219 (OK) 1735 (overestimated)
AUCoral 2038 (overestimated) 1294
F 173 74 (OK)
Torres-Molina et al Pharmac Res 1992 9 1587-1591
44
How to measure an absolute bioavailability?

Assumption Cliv Clev
correction by the terminal half-life

AUCEV AUCIV
t1/2IV t1/2EV
F x x 100
Warning! illicit correction if flip-flop
45
How to measure an absolute bioavailability?
With a metabolite
AUC EV,metab AUC IV,métab
Dose IV Dose EV
x 100
F x
N.B.1 the metabolite should not be formed at
the administration site or by a first-pass
effect N.B.2 note 1 does not hold for a
relative bioavailability
46
How to measure an absolute bioavailability?

Problem of the analytical techniques
The case of Enrofloxacin
Using microbiological assay
? overestimation of F

Ciproflox
Liver Enroflox
Enroflox
Enrofloxacin
47
Absolute bioavailability

Using urinary drug concentrations
Drug itself

?
Xu,EV Xu,IV
Dose IV Dose EV
x 100
F x
?

A metabolite
Not formed by a first pass effect

48
How to measure an absolute bioavailability when
an IV administration is not possible
49
How to measure an absolute bioavailability
without IV administration?
Dose AUCIV

IV Cltot ClR ClnR
PO Cltot/F

ClR F
Dose AUCPO
ClnR F
50
How to measure an absolute bioavailability
without IV administration

Measurement possible from oral data only
Condition the renal clearance is known and
displays a large interindividual variance

constant
variable
1 F
1 F
Dose AUCpo
x ClR ClNR
Y a X b
51
How to measure an absolute bioavailability
without IV administration
Measure possible with oral data only
Dose AUCpo
1 F
1 F
ClNR
Clrenal
52
METHODS FOR ASSESSMENT OF ABSOLUTE BIOAVAILABILITY

Conventional method iv and oral doses
Usually given on two separate occasions
requires two study sessions
Requires two sets of blood samples
Assumes no change in disposition
Parameters between studies.

Stable isotope method
One study and set of blood samples
Special synthesis requirements
Mass spectrometer assay required

53
NAPA-13C2
54
SIMULTANEOUS ADMINISTRATION OF ORAL NAPA AND IV
NAPA-C13
From Atkinson AJ Jr, et al. Clin Pharmacol Ther
198946182-9.
55
Thoughts about absolute bioavailability studies

Absolute bioavailability is usually
Studied in healthy subjects, not in
The patient population for whom its
use is intended.
The stable isotope method is ideally
Suited for studies in special
populations (e.G. Pediatrics, pregnant
Women) and other patient groups.

56
Relative bioavailability
57
Relative bioavailability

Single dose

AUCA AUCB
x 100
F
AUCA
AUCB
58
Relative bioavailability

Under steady state conditions

Formulation A Formulation B (after
equilibrium) (after new equilibrium)
Plasma
AUCA
AUCB
Time
Condition linearity and stationarity
F (AUCA / AUCB) ? 100
59
Bioavailability

Evaluation of AUC

60
Bioavailability
Measurement of AUC sampling strategy (1)

If the samples are numerous and appropriately
spaced, the AUC is accurately determined

61
Bioavailability
Measurement of AUC sampling strategy (2)

Not enough samples in the ascending phase. The
AUC is under-estimated

62
Bioavailability
Measurement of AUC sampling strategy (3)

Not enough samples in the descending phase. The
AUC is over-estimated

63
BioavailabilityAssessment of the rate of
absorption
64
BioavailabilityRate of absorption

Cmax et Tmax

Cmax
Tmax
65
Are Cmax and Tmax suggestive of the absorption
rate of the drug ?
this can be very misleading
66
BioavailabilityRate of absorption

Cmax and Tmax are hybrid parameters
Cmax
F, Ka, K10
Tmax
Ka, K10

67
Tmax

Monocompartmental model

Ka
Ln Ka - Ln K10
Tmax
Ka - K10
K10
!
Ka varies with bioavailability
!
flip-flop situation
68
Terminal half-life
Ka1 absorption
Ka2 Irreversible loss of drug from the injection
site
K10 Elimination from the central compartment
69
Tmax

Monocompartmental model

1
1
0
0.2
0.2
1
Ln1 - Ln0.2
Ln2 - Ln0.2
Tmax 2.01 h
Tmax 1.27 h
1 - 0.2
2 - 0.2
F 50
F 100
70
Baignoire avec fuite
(K10)
71
Tmax bioavailabilty

Tmax is observed more early in case of low
bioavailability .

72
Tmax and Bioavailability of Cefadroxil in foal
Age (months) 0.5 1 2 3 5
F 99.6 67.6 35.1 19.5 14.4
Tmax (h) 2.1 1.60 1.60 0.96 0.90
Duffee JVPT 1997 20 427
73
Tmax and flip-flop situation
74
Tmax and flip-flop situation
K10 of A or Ka of B
Ka of A or K10 of B
Tmax 2.55 h

Drug A Ka 1.0 K10 0.1 t1/2 abs 0.693 h
Drug B Ka 0.1 K10 1.0 t1/2 abs 6.93 h

75
Bioavailability and half-life

In case of flip-flop, bioavailability may
influence the terminal half-life

76
BioavailabilityHow to evaluate Ka?

Curves fitting
Interpretation of Ka when F lt 100

K12
Ka1
Ka
K21
Ka2
K10
Ka1 Ka1 Ka2
What is measured is not Ka1 but Ka Ka1Ka2 t1/2
Ka measures the rate of drug disappearance at the
administration site
F
77
What is the meaning of the terminal half-life
after an extravascular drug administration?
Half-absorption or half-elimination ?

a rate-limited absorption
(flip-flop) must be recognized
(C)
100
10
EV rate of absorption
IV
EV rate of elimination
1
time
0.1
0
5
10
15
20
25
30
78
Terminal half-life and the flip-flop case
K12
Slow process of absorption
Ka1
K21
Ka2 negligible
K10
(ng/ml)
100
KaKa1Ka2 Ka1 flip-flop
10
elimination
1
Ka1 Ka1 Ka2
F ? 100
0.1
Time
0
5
10
15
20
25
30
79
Terminal half-life and the flip-flop case
K12
Ka1
K21
K10
Ka2 ()
Ka1 Ka1 Ka2
F low
(ng/ml)
100
Lack of flip-flop due to low bioavailability not
to an increase of the rate of absorption (Ka1)
10
1
elimination
KaKa1Ka2 Ka2
Time
0.1
0
5
10
15
20
25
30
80
Tmax and flip-flop situation

For the same drug
Formulation Ka (h-1) K10 (h-1) Tmax (h) t1/2abs
(h)
A 1.0 0.1 2.56 0.693
B 0.1 0.1 10.0 6.93
C 0.01 0.1 25.6 69.3

!
The Tmax ratios do not reflect the t1/2 abs
ratios
81
The true meaning of Ka

Remember
Ka is the apparent first order absorption rate
constant derived from plasma data
This parameter may also contain processes
parallel to the true absorption step such as
degradation of drug in the administration site

82
The true meaning of Ka
Ka1 absorption
Ka1Ka2
Ka1Ka2
Ka2 Irreversible loss of drug from the injection
site
K10 Elimination from the central compartment
83
Lufenuron SQ vs oral administration
interpretation of the terminal phase
SC
Ka1 Ka1 Ka2
Ka1
F
Skin
Blood
Ka2
Ka Ka1 Ka2
If Ka2 ? ?F ? and t1/2 ?

In flip-flop conditions, F and t1/2 are linked

84
How to evaluate the rate of absorption
85
How to evaluate Ka accurately

1- Directly from the ascending phase
2- By peeling method
3- Wagner-Nelson, Loo-Riegelman (deconvolution)
4- Statistical moments

86
BioavailabilityHow to evaluate Ka?

Fitting plasma concentrations

Ka
Ka

Computation of Ka, constant of absorption
t1/2 Ka 0.693 / ka

87
BioavailabilityHow to evaluate Ka?

Curves fitting
How to know Ka

k a1
k 10
?
k a
k a2
?
IM route
?
?
k a1
k 12
k a
k 21
k a2
k 10
k 10
88
BioavailabilityHow to evaluate Ka?

Curves fitting
Interpretation of Ka when F lt 100

K12
Ka1
K21
Ka2
K10
Ka1 Ka1 Ka2
What is measured is not Ka1 but Ka Ka1Ka2 t1/2
Ka measures the rate of drug disappearance at the
administration site
F
89
BioavailabilityHow to evaluate Ka?

Curves fitting
Problem of undistinguishability

K12
Ka
K21
K10
If Ka K21, the plasma concentrations curve will
be identical to the classical Bateman curve and
Ka will not be properly estimated
90
BioavailabilityHow to evaluate ka?

Remember
Ka is the apparent first order absorption rate
constant derived from plasma data
This parameter may also contain processes
parallel to the true absorption step such as
degradation of drug in the administration site

91
BioavailabilityAssessment of the rate of
absorption