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Multicompartment Models

VNS Group of Institutions - Faculty of Pharmacy, Bhopal (M.P.) India
VNS Group of Institutions - Faculty of Pharmacy, Bhopal (M.P.) India

Biopharmaceutics

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MULTICOMPARTMENT MODELS Prepared By Girijesh Kumar Pandey M.Pharm. (Pharmaceutics)
Contents • Introduction • Two-Compartment Open model • Intravenous bolus administration • Intravenous Infusion • Extra vascular administration • Conclusion • References
Introduction • One compartment is described by mono- exponential term i.e. elimination. • For large class of drugs this terms is not sufficient to describe its disposition. • It needs a bi- or multi- exponential terms • The body is composed of a heterogeneous group of tissues each with different degree of blood flow and affinity for drug and therefore different rates of elimination. • Multi-compartment characteristics are best described by administration as i.v. bolus.
Two Compartment Model • The simplest and commonest is the two compartment model which classifies the body tissues in two categories : 1) Central compartment or Compartment 1 2) Peripheral or Tissue Compartment or Compartment 2. • Compartment 1 comprises of blood and highly perfused tissues like liver, lungs, kidneys, etc. • Elimination usually occurs from this compartment. • Compartment 2 comprises of poorly perfused and slow equilibriating tissues such as muscles, skin, adipose, etc.
Two Compartment Model • General Grouping of Tissue According to Blood Supply
Two Compartment Model • Depending upon the compartment from which the drug is eliminated, the 2 compartment model can be further categorised into : - With elimination from Central compartment - With elimination from peripheral compartment - With elimination from both the compartments
Two Compartment Model
Two compartment Open model- I.V. bolus administration: • Elimination from central compartment 1 Central 2 Peripheral • After the iv bolus of a drug the decline in the plasma conc. is bi-exponential. • Two disposition processes- distribution and elimination. • These two processes are only evident when a semilog plot of C vs t is made.
Two compartment Open model- I.V. bolus administration: • Model Structure for Two Compartment Model
Two compartment Open model- I.V. bolus administration: • Where, X 0 = IV bolus dose administered C c = X 1 = amount of drug in the central compartment C p = X 2 = amount of drug in the peripheral compartment k 12 = rate constant for transfer of drug from the central to the peripheral compartment k 21 = rate constant for transfer of drug from the peripheral to the central compartment k E = first order elimination rate constant. Elimination of drug out of the central compartment
Two compartment Open model- I.V. bolus administration: • The second, slower rate process, is called as the post- distributive or elimination phase. • In contrast to central compartment, the conc of drug in the peripheral compartment first increases and reaches its max. • The Rate change in drug conc. in the central compartment is given by, • Extending the relationship X= V d C • Where, V c and V p = apparent volumes of C1 and C2
Two compartment Open model- I.V. bolus administration: • The rate of change in drug conc in the peripheral component is given by: • On integration equation gives conc. of drug in central and peripheral compartments at given time t :
Two Compartment Open Model – Intravenous Infusion • The plasma or central compartment conc of a drug when administered as constant rate (0 order) i.v. infusion is given as:
Two Compartment Open Model – Intravenous Infusion • At steady state the second and the third term in the bracket becomes zero and the equation reduces to: Now, The loading dose
Two-Compartment Open Model- Extravascular administration • First - Order Absorption • The model can be depicted as follows : • The rate of change in drug conc. in the central compartment is described by three exponents : An absorption exponent, and • Two usual exponents that describe drug disposition.
Two-Compartment Open Model- Extravascular administration • The plasma conc at time t is, • Where, L, M & N are coefficients
Conclusion • The future should involve the use of models capable of incorporating physico -chemical data and biological information . • Compartment modelling is useful in Characterize the behavior of drug in patient, predicting conc. of drug in various body fluids with dosage regimen , calculating optimum dosage regimen for individual patient, evaluating bioequivalence between different formulation, explaining drug interaction.
References • D.M.Brahmankar & S.B. Jaiswal , Biopharmaceutics & pharmacokinetics. A.treatise , First edition, Vallabh Prakashan, P.No . 290-299, • Leu and febiger , Biopharmaceutics & clinical pharmacokinetics by Milo Giberldi , Fourth edition, Philadelphis , 1991. P.No . 213-230. • Leon shargel and Andrew Yu, A pplied Biopharmaceutics and pharmacokinetics, Fourth edition. page no. 47-62. • Milo Gibaldi , Biopharmaceutics and clinical pharmacokinetics Fourth edition . page no.14-23, • http://www.authorstream.com/Presentation/abhijit_26- 1830737-multi-compartment-models/

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Multicompartment Models

  • 1. MULTICOMPARTMENT MODELS Prepared By Girijesh Kumar Pandey M.Pharm. (Pharmaceutics)
  • 2. Contents • Introduction • Two-Compartment Open model • Intravenous bolus administration • Intravenous Infusion • Extra vascular administration • Conclusion • References
  • 3. Introduction • One compartment is described by mono- exponential term i.e. elimination. • For large class of drugs this terms is not sufficient to describe its disposition. • It needs a bi- or multi- exponential terms • The body is composed of a heterogeneous group of tissues each with different degree of blood flow and affinity for drug and therefore different rates of elimination. • Multi-compartment characteristics are best described by administration as i.v. bolus.
  • 4. Two Compartment Model • The simplest and commonest is the two compartment model which classifies the body tissues in two categories : 1) Central compartment or Compartment 1 2) Peripheral or Tissue Compartment or Compartment 2. • Compartment 1 comprises of blood and highly perfused tissues like liver, lungs, kidneys, etc. • Elimination usually occurs from this compartment. • Compartment 2 comprises of poorly perfused and slow equilibriating tissues such as muscles, skin, adipose, etc.
  • 5. Two Compartment Model • General Grouping of Tissue According to Blood Supply
  • 6. Two Compartment Model • Depending upon the compartment from which the drug is eliminated, the 2 compartment model can be further categorised into : - With elimination from Central compartment - With elimination from peripheral compartment - With elimination from both the compartments
  • 8. Two compartment Open model- I.V. bolus administration: • Elimination from central compartment 1 Central 2 Peripheral • After the iv bolus of a drug the decline in the plasma conc. is bi-exponential. • Two disposition processes- distribution and elimination. • These two processes are only evident when a semilog plot of C vs t is made.
  • 9. Two compartment Open model- I.V. bolus administration: • Model Structure for Two Compartment Model
  • 10. Two compartment Open model- I.V. bolus administration: • Where, X 0 = IV bolus dose administered C c = X 1 = amount of drug in the central compartment C p = X 2 = amount of drug in the peripheral compartment k 12 = rate constant for transfer of drug from the central to the peripheral compartment k 21 = rate constant for transfer of drug from the peripheral to the central compartment k E = first order elimination rate constant. Elimination of drug out of the central compartment
  • 11. Two compartment Open model- I.V. bolus administration: • The second, slower rate process, is called as the post- distributive or elimination phase. • In contrast to central compartment, the conc of drug in the peripheral compartment first increases and reaches its max. • The Rate change in drug conc. in the central compartment is given by, • Extending the relationship X= V d C • Where, V c and V p = apparent volumes of C1 and C2
  • 12. Two compartment Open model- I.V. bolus administration: • The rate of change in drug conc in the peripheral component is given by: • On integration equation gives conc. of drug in central and peripheral compartments at given time t :
  • 13. Two Compartment Open Model – Intravenous Infusion • The plasma or central compartment conc of a drug when administered as constant rate (0 order) i.v. infusion is given as:
  • 14. Two Compartment Open Model – Intravenous Infusion • At steady state the second and the third term in the bracket becomes zero and the equation reduces to: Now, The loading dose
  • 15. Two-Compartment Open Model- Extravascular administration • First - Order Absorption • The model can be depicted as follows : • The rate of change in drug conc. in the central compartment is described by three exponents : An absorption exponent, and • Two usual exponents that describe drug disposition.
  • 16. Two-Compartment Open Model- Extravascular administration • The plasma conc at time t is, • Where, L, M & N are coefficients
  • 17. Conclusion • The future should involve the use of models capable of incorporating physico -chemical data and biological information . • Compartment modelling is useful in Characterize the behavior of drug in patient, predicting conc. of drug in various body fluids with dosage regimen , calculating optimum dosage regimen for individual patient, evaluating bioequivalence between different formulation, explaining drug interaction.
  • 18. References • D.M.Brahmankar & S.B. Jaiswal , Biopharmaceutics & pharmacokinetics. A.treatise , First edition, Vallabh Prakashan, P.No . 290-299, • Leu and febiger , Biopharmaceutics & clinical pharmacokinetics by Milo Giberldi , Fourth edition, Philadelphis , 1991. P.No . 213-230. • Leon shargel and Andrew Yu, A pplied Biopharmaceutics and pharmacokinetics, Fourth edition. page no. 47-62. • Milo Gibaldi , Biopharmaceutics and clinical pharmacokinetics Fourth edition . page no.14-23, • http://www.authorstream.com/Presentation/abhijit_26- 1830737-multi-compartment-models/