Bioavailability Studies
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Feb 11, 2013
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About This Presentation
Bioavailability Studies
Slide Content
1
-: Presented By :--: Presented By :-
Amruta S. SambarekarAmruta S. Sambarekar
11
stst
Year M.Pharm Year M.Pharm
Dept. of PharmaceuticsDept. of Pharmaceutics
M M C P, BELGAUMM M C P, BELGAUM
BIOAVAILABILITYBIOAVAILABILITY
-: Presented By :--: Presented By :-
Amruta S. SambarekarAmruta S. Sambarekar
11
stst
Year M.Pharm Year M.Pharm
Dept. of PharmaceuticsDept. of Pharmaceutics
M M C P, BELGAUMM M C P, BELGAUM
BIOAVAILABILITYBIOAVAILABILITY
2
CONTENTSCONTENTS
Concept of Bioavailability
Objectives of Bioavailability Studies
Considerations in Bioavailability
Studies
CONTENTSCONTENTS
Concept of Bioavailability
Objectives of Bioavailability Studies
Considerations in Bioavailability
Studies
3
INTRODUCTIONINTRODUCTION
Bioavailability is defined as a measure, of
the rate and amount of drug, which reaches
the systemic circulation unchanged
following the administration of a dosage
form.
INTRODUCTIONINTRODUCTION
Bioavailability is defined as a measure, of
the rate and amount of drug, which reaches
the systemic circulation unchanged
following the administration of a dosage
form.
4
In other words, it is the fraction of
administered dose that actually reaches
the systemic circulation in contrast to that
stated on the label.
Bioavailability is usually determined by
comparing the rate and extent of
absorption of drug from the formulation
under evaluation, to the data of a
reference standard.
Cont….Cont….
In other words, it is the fraction of
administered dose that actually reaches
the systemic circulation in contrast to that
stated on the label.
Bioavailability is usually determined by
comparing the rate and extent of
absorption of drug from the formulation
under evaluation, to the data of a
reference standard.
Cont….Cont….
5
If the reference standard is an IV dose, it is
referred as Absolute Bioavailability. If
the reference standard is any other dosage
form than IV it is referred as Relative
Bioavailability.
Reference standard can be IM injection,
oral solution or a fine suspension.
Bioavailability usually ranges from 0 to 1.
Cont….Cont….
If the reference standard is an IV dose, it is
referred as Absolute Bioavailability. If
the reference standard is any other dosage
form than IV it is referred as Relative
Bioavailability.
Reference standard can be IM injection,
oral solution or a fine suspension.
Bioavailability usually ranges from 0 to 1.
Cont….Cont….
6
An absolute bioavailability of 1 (or 100% )
indicates complete absorption.
Relative bioavailability of 1 (or 100%)
implies that bioavailability of drug from
both the dosage form is the same but does
not indicate the completeness of
absorption.
Cont….Cont….
An absolute bioavailability of 1 (or 100% )
indicates complete absorption.
Relative bioavailability of 1 (or 100%)
implies that bioavailability of drug from
both the dosage form is the same but does
not indicate the completeness of
absorption.
Cont….Cont….
7
Bioavailability of drug from dosage form Bioavailability of drug from dosage form
depends upon following,depends upon following,
- Properties of the drug
- Important physiological factors
- Characteristics of the dosage form
Bioavailability of drug from dosage form Bioavailability of drug from dosage form
depends upon following,depends upon following,
- Properties of the drug
- Important physiological factors
- Characteristics of the dosage form
8
Bioavailability StudiesBioavailability Studies
Two types are there, The first type
involves an assessment of the
bioavailability of a new drug formulation.
The second type study involves a
comparison of a test formulation with that
of a reference standard dosage form that is
proved to have a therapeutic safety and
efficacy.
Bioavailability StudiesBioavailability Studies
Two types are there, The first type
involves an assessment of the
bioavailability of a new drug formulation.
The second type study involves a
comparison of a test formulation with that
of a reference standard dosage form that is
proved to have a therapeutic safety and
efficacy.
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ObjectivesObjectives
Primary stage of development for suitable
dosage form for a new drug entity.
Determination of influence of excipients,
patient related factors and possible
interaction with other drugs on the
efficiency of absorption.
ObjectivesObjectives
Primary stage of development for suitable
dosage form for a new drug entity.
Determination of influence of excipients,
patient related factors and possible
interaction with other drugs on the
efficiency of absorption.
10
For a approved drugs to develop a new
dosage form or to improve an existing
dosage form.
To find out the influence of
physicochemical properties of drug and
dosage form on biological performance of
the drug.
Cont….Cont….
For a approved drugs to develop a new
dosage form or to improve an existing
dosage form.
To find out the influence of
physicochemical properties of drug and
dosage form on biological performance of
the drug.
Cont….Cont….
11
Useful in determining the safety and
efficacy of the drug product.
Cont….Cont….
Useful in determining the safety and
efficacy of the drug product.
Cont….Cont….
12
Considerations in Bioavailability Considerations in Bioavailability
StudiesStudies
Selection Of Subjects
Study Design
Washout Period
Single Vs Multiple- Dose Study Design
Considerations in Bioavailability Considerations in Bioavailability
StudiesStudies
Selection Of Subjects
Study Design
Washout Period
Single Vs Multiple- Dose Study Design
13
Study Conditions
Pharmacological Effects of Metabolite
Assay Method
Study Conditions
Pharmacological Effects of Metabolite
Assay Method
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Selection Of SubjectsSelection Of Subjects
A number of factors such as health, age,
weight, enzyme status and number are
concern.
It is better to have the subjects of similar
kinetics to avoid major variations.
Health :Health : Subjects should be of great health
that is ascertained by various biochemical
and medical examination.
Selection Of SubjectsSelection Of Subjects
A number of factors such as health, age,
weight, enzyme status and number are
concern.
It is better to have the subjects of similar
kinetics to avoid major variations.
Health :Health : Subjects should be of great health
that is ascertained by various biochemical
and medical examination.
15
Age : Age :
Elderly and children have different
kinetics to adults. Subjects between 18 – 35
years are preferred.
Number :Number :
Number of participants should be kept
minimum required for carrying out a
reliable, well designed study.
Age : Age :
Elderly and children have different
kinetics to adults. Subjects between 18 – 35
years are preferred.
Number :Number :
Number of participants should be kept
minimum required for carrying out a
reliable, well designed study.
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Weight :Weight :
The apparent volume of distribution is
usually proportional to weight in subjects
of normal weight and height.
However, in overweight and underweight
Vd may be different. Hence, to better
match the subject , normal weights are
preferred. Usually 140-200lb
Weight :Weight :
The apparent volume of distribution is
usually proportional to weight in subjects
of normal weight and height.
However, in overweight and underweight
Vd may be different. Hence, to better
match the subject , normal weights are
preferred. Usually 140-200lb
17
Enzyme Status :Enzyme Status :
Enzyme activity can be altered by altered
kinetics of the drug in case of smokers or
subjects taking other drugs leading to
drug-drug interaction.
Enzyme Status :Enzyme Status :
Enzyme activity can be altered by altered
kinetics of the drug in case of smokers or
subjects taking other drugs leading to
drug-drug interaction.
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Usually, a complete cross over study
design is used. With this design each
subject receives all products with a
washout period between each dose
administration.
This is a Latin square crossover design
where each subject receives each drug
product only once . Here each subject act
as his own control and subject to subject
variation is reduced.
Study DesignStudy Design
Usually, a complete cross over study
design is used. With this design each
subject receives all products with a
washout period between each dose
administration.
This is a Latin square crossover design
where each subject receives each drug
product only once . Here each subject act
as his own control and subject to subject
variation is reduced.
Study DesignStudy Design
19
Washout Period :Washout Period :
The time interval between two treatments
is called “washout period”.
It is required for the elimination of the
administered dose of a drug so as to avoid
a carryover effect
Washout Period :Washout Period :
The time interval between two treatments
is called “washout period”.
It is required for the elimination of the
administered dose of a drug so as to avoid
a carryover effect
20
Usually, a period of 10 half-lives should be
allowed between two treatments ensuring
elimination of 99.9% of the administered
dose.
The number of washout period depends
upon the type of crossover study design
used and number of formulations to be
evaluated.
Cont….Cont….
Usually, a period of 10 half-lives should be
allowed between two treatments ensuring
elimination of 99.9% of the administered
dose.
The number of washout period depends
upon the type of crossover study design
used and number of formulations to be
evaluated.
Cont….Cont….
21
In case of Digitoxin,
Half –life : 6 to 9 days
Study design :Latin square crossover
design for four formulations.
Duration : 1 year
Cont….Cont….
In case of Digitoxin,
Half –life : 6 to 9 days
Study design :Latin square crossover
design for four formulations.
Duration : 1 year
Cont….Cont….
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Single- Dose Studies Recommended ForSingle- Dose Studies Recommended For
Dosage forms that are to be evaluated only
for bioequivalence purpose.
Dosage forms meant for a single dose
administration for a therapeutic benefit
such as analgesic for relief of headache.
Single Vs. Multiple- Dose Study DesignSingle Vs. Multiple- Dose Study Design
Single- Dose Studies Recommended ForSingle- Dose Studies Recommended For
Dosage forms that are to be evaluated only
for bioequivalence purpose.
Dosage forms meant for a single dose
administration for a therapeutic benefit
such as analgesic for relief of headache.
Single Vs. Multiple- Dose Study DesignSingle Vs. Multiple- Dose Study Design
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Multiple Dose Studies Recommended ForMultiple Dose Studies Recommended For
Dosage forms designed to achieve special
release profiles. e.g. time-release products,
enteric-coated preparations.
Drugs undergoing first pass metabolism.
Special dosage regimens such as Loading
dose.
Multiple Dose Studies Recommended ForMultiple Dose Studies Recommended For
Dosage forms designed to achieve special
release profiles. e.g. time-release products,
enteric-coated preparations.
Drugs undergoing first pass metabolism.
Special dosage regimens such as Loading
dose.
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Study conditionsStudy conditions
Subject should be maintained on a
uniform diet and none of them should
have taken any drug at least one week
prior to the study.
Before the commencement of study it is
necessary to define the study condition
such as fasting period before the
administration, time period after drug
product administration, during which
fasting is continued.
Study conditionsStudy conditions
Subject should be maintained on a
uniform diet and none of them should
have taken any drug at least one week
prior to the study.
Before the commencement of study it is
necessary to define the study condition
such as fasting period before the
administration, time period after drug
product administration, during which
fasting is continued.
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In general studies are carried out on
subjects fasted overnight.
Cont….Cont….
In general studies are carried out on
subjects fasted overnight.
Cont….Cont….
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Pharmacological Effects of Pharmacological Effects of
MetabolitesMetabolites
Bioavailability measurement is based on
the unchanged drug.
Drugs having biologically active
metabolites, their concentration in
systemic circulation can influence greatly
the therapeutic efficacy of the drug.
Pharmacological Effects of Pharmacological Effects of
MetabolitesMetabolites
Bioavailability measurement is based on
the unchanged drug.
Drugs having biologically active
metabolites, their concentration in
systemic circulation can influence greatly
the therapeutic efficacy of the drug.
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It was found especially significant for
drugs which exhibits first pass metabolism
during pre-absorptive phase.
Phenacetin has more side effects than, its
metabolite acteaminophen, which is also
pharmacologically active form.
In case of aspirin its metabolite salicylic
acid is pharmacologically inactive and
exhibits serious toxicity.
Cont….Cont….
It was found especially significant for
drugs which exhibits first pass metabolism
during pre-absorptive phase.
Phenacetin has more side effects than, its
metabolite acteaminophen, which is also
pharmacologically active form.
In case of aspirin its metabolite salicylic
acid is pharmacologically inactive and
exhibits serious toxicity.
Cont….Cont….
28
Based on above findings, it is good
practice in bioavailability studies to
examine the presence of major metabolites
in blood and urine, to determine their
concentration and, if possible,
pharmacological activity of each.
Cont….Cont….
Based on above findings, it is good
practice in bioavailability studies to
examine the presence of major metabolites
in blood and urine, to determine their
concentration and, if possible,
pharmacological activity of each.
Cont….Cont….
29
Assay methodAssay method
The analytical method used to quantitate
the levels of drug and/or its metabolites
must be selective e.g., for the unchanged
drug in presence of its metabolites.
It must be sensitive enough to measure the
expected low drug levels in the samples
collected last.
Assay methodAssay method
The analytical method used to quantitate
the levels of drug and/or its metabolites
must be selective e.g., for the unchanged
drug in presence of its metabolites.
It must be sensitive enough to measure the
expected low drug levels in the samples
collected last.
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““Text Book Of Biopharmaceutics & Text Book Of Biopharmaceutics &
PharmacokineticsPharmacokinetics”,”, Dr. Shobha Rani R. Hiremath.
Pg no. 31-35.
““Biopharmaceutics & Pharmacokinetics”Biopharmaceutics & Pharmacokinetics”
Venkatesh Pg no. 331, 336-338.
““Biopharmaceutics & pharmacokinetics”,Biopharmaceutics & pharmacokinetics”,
D.M.Brahmankar, S.B.Jaiswal, Pg.no. 283.
REFERENCEREFERENCE
““Text Book Of Biopharmaceutics & Text Book Of Biopharmaceutics &
PharmacokineticsPharmacokinetics”,”, Dr. Shobha Rani R. Hiremath.
Pg no. 31-35.
““Biopharmaceutics & Pharmacokinetics”Biopharmaceutics & Pharmacokinetics”
Venkatesh Pg no. 331, 336-338.
““Biopharmaceutics & pharmacokinetics”,Biopharmaceutics & pharmacokinetics”,
D.M.Brahmankar, S.B.Jaiswal, Pg.no. 283.
REFERENCEREFERENCE
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