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A SEMINAR ON
      TYPES OF EQUIVALENT
              AND
 MEASUREMENT OF BIOAVAILABILITY




PRESENTED BY:
GANDHI SONAM MUKESHCHANDRA
1ST YR M.PHARM
DEPT. OF INDUSTRIAL PHARMACY
CONTENTS

   Introduction & importance

   Types of equivalents

   Methods for assessing the

    bioavailability
Introduction & Importance

   There are several formulations of same
    drug, in the same dose, in a similar
    dosage form and given through same
    route. Substitution of one product for
    another can be made equally effective,
    therapeutically as per standards. In order
    to ensure clinical performance of such
    drug products bioequivalence studies
    should be performed.
EQUIVELENTS
 It is a term that compares one product is
  similar with respect to a specific
  characteristic or function to another, or to
  the defined set of the standards.
 There are four types of equivalences:
 1. Chemical equivalence
 2. Pharmaceutics equivalence
 3. Therapeutic equivalence
 4. Bioequivalence
   Chemical equivalence:
    two or more formulations contain the
    same labelled chemical substance as an
    active ingredient in the same amount.

   Pharmaceutics equivalence:
    two or more formulations are identical in
    strength, quality, purity, content
    uniformity and disintegration and
    dissolution characteristics.
   Therapeutic equivalence:
    It indicates that two or more drug products
    that contain the same therapeutic active
    ingredients elicit same pharmacologic effects
    and can control the disease to the same
    extent.

   Bio equivalence:
    It is a relative term which denotes that the
    drug substance in two or more identical
    dosage forms reaches systemic circulation at
    same relative rate and to the same relative
    extent i.e. their plasma concentration-time
    profiles will be identical without significant
    statistical differences.
Methods for assessing the bioavailability
   Pharmacokinetics methods
      This method reflects the therapeutic
    effectiveness of a drug. Thus these are indirect
    methods.

   Plasma-level time studies
   Urinary excretion studies

Pharmacodynamic methods
   This method involves direct measurement of
 drug effect on a physiologic process as a function
 of time.
 acute pharmacologic response
 therapeutic response
Pharmacokinetic methods
   Cmax: it gives indication whether drug is
    sufficiently absorbed systematically to
    provide therapeutic response

   Tmax: the peak time that gives an
    indication of rate of absorption

   AUC: it gives a measure of the extent of
    absorption or amount of drug that
    reaches the systemic circulation.
   Extent of bioavailability can be
    determined by following equations


   F=[AUC]oral Div/[AUC]iv Doral

 Fr=[AUC]test Dstd/ [AUC]std D test
Pharmacodynamic methods
1.(dXu/dt)max: it is obtained from the peak of plot
  b/w rate of excretion v/s mid point time of urine
  collected period.
2. (tu)max: it is analogues to the tmax of plasma
    level data, its value decrease as absorption rate
    increases.
3. Xu: it is related to the AUC of plasma level data
    and increases as the extent of absorption
    increases.
   Extent of bioavailability can be
    determined by following equations

   F = (Xu α)oral Div/ (Xu α)iv Doral

   Fr= (Xu α)test Dstd/ (Xu α) std Dtest
Acute pharmacological response
 In this method acute pharmacologic
  effect such as change in ECG or EEG
  readings, pupil diameter etc. is related to
  the time course of the given drug.
 Bioavailability can be determined by
  construction of pharmacological effect-
  time curve as well as dose response
  graph.
 THERAPEUTIC RESPONSE
 This method is based on observing the
  clinical response to a drug formulation
  given to patients suffering from disease
  for which it is intended to be used.
References
 Dr. Shobha rani, R Hiremath, Textbook of
  Biopharmaceutics & Pharmacokinetics. Pg
  no.32-47.
 D.M. Brahmankar, Sunil B. Jaiswal.
  Biopharmaceutics & Pharmacokinetics A
  TRETISE.Pg.no.285-289.
 Milo Gibaldi. Biopharmaceutics & Clinical
  Pharmacokinetics. Fourth edition. Pg.15
 Leon shargel, applied Biopharmaceutics
  and pharmacokinetics. Fifth
  edition.2005.Pg.no.460-465.
THANK YOU

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Types of equivalent and measurement of bioavailability

  • 1. A SEMINAR ON TYPES OF EQUIVALENT AND MEASUREMENT OF BIOAVAILABILITY PRESENTED BY: GANDHI SONAM MUKESHCHANDRA 1ST YR M.PHARM DEPT. OF INDUSTRIAL PHARMACY
  • 2. CONTENTS  Introduction & importance  Types of equivalents  Methods for assessing the bioavailability
  • 3. Introduction & Importance  There are several formulations of same drug, in the same dose, in a similar dosage form and given through same route. Substitution of one product for another can be made equally effective, therapeutically as per standards. In order to ensure clinical performance of such drug products bioequivalence studies should be performed.
  • 4. EQUIVELENTS  It is a term that compares one product is similar with respect to a specific characteristic or function to another, or to the defined set of the standards. There are four types of equivalences:  1. Chemical equivalence  2. Pharmaceutics equivalence  3. Therapeutic equivalence  4. Bioequivalence
  • 5. Chemical equivalence: two or more formulations contain the same labelled chemical substance as an active ingredient in the same amount.  Pharmaceutics equivalence: two or more formulations are identical in strength, quality, purity, content uniformity and disintegration and dissolution characteristics.
  • 6. Therapeutic equivalence: It indicates that two or more drug products that contain the same therapeutic active ingredients elicit same pharmacologic effects and can control the disease to the same extent.  Bio equivalence: It is a relative term which denotes that the drug substance in two or more identical dosage forms reaches systemic circulation at same relative rate and to the same relative extent i.e. their plasma concentration-time profiles will be identical without significant statistical differences.
  • 7. Methods for assessing the bioavailability  Pharmacokinetics methods This method reflects the therapeutic effectiveness of a drug. Thus these are indirect methods.  Plasma-level time studies  Urinary excretion studies Pharmacodynamic methods This method involves direct measurement of drug effect on a physiologic process as a function of time.  acute pharmacologic response  therapeutic response
  • 8. Pharmacokinetic methods  Cmax: it gives indication whether drug is sufficiently absorbed systematically to provide therapeutic response  Tmax: the peak time that gives an indication of rate of absorption  AUC: it gives a measure of the extent of absorption or amount of drug that reaches the systemic circulation.
  • 9. Extent of bioavailability can be determined by following equations  F=[AUC]oral Div/[AUC]iv Doral  Fr=[AUC]test Dstd/ [AUC]std D test
  • 10.
  • 11. Pharmacodynamic methods 1.(dXu/dt)max: it is obtained from the peak of plot b/w rate of excretion v/s mid point time of urine collected period. 2. (tu)max: it is analogues to the tmax of plasma level data, its value decrease as absorption rate increases. 3. Xu: it is related to the AUC of plasma level data and increases as the extent of absorption increases.
  • 12. Extent of bioavailability can be determined by following equations  F = (Xu α)oral Div/ (Xu α)iv Doral  Fr= (Xu α)test Dstd/ (Xu α) std Dtest
  • 13. Acute pharmacological response  In this method acute pharmacologic effect such as change in ECG or EEG readings, pupil diameter etc. is related to the time course of the given drug.  Bioavailability can be determined by construction of pharmacological effect- time curve as well as dose response graph.
  • 14.  THERAPEUTIC RESPONSE  This method is based on observing the clinical response to a drug formulation given to patients suffering from disease for which it is intended to be used.
  • 15. References  Dr. Shobha rani, R Hiremath, Textbook of Biopharmaceutics & Pharmacokinetics. Pg no.32-47.  D.M. Brahmankar, Sunil B. Jaiswal. Biopharmaceutics & Pharmacokinetics A TRETISE.Pg.no.285-289.  Milo Gibaldi. Biopharmaceutics & Clinical Pharmacokinetics. Fourth edition. Pg.15  Leon shargel, applied Biopharmaceutics and pharmacokinetics. Fifth edition.2005.Pg.no.460-465.