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Oral Delivery of Drugs

Oral Delivery of Drugs. Session One of TIP Project. Advantages of taking oral drugs. Convenient (storage, portability, pre-measured dose) economical non-invasive, often safer route requires no special training like IV drugs or subcutaneous drugs require.

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Oral Delivery of Drugs

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  1. Oral Delivery of Drugs Session One of TIP Project TIP 2009 GEPHART

  2. Advantages of taking oral drugs • Convenient (storage, portability, pre-measured dose) • economical • non-invasive, often safer route • requires no special training like IV drugs or subcutaneous drugs require. • Many are also available over-the- counter TIP 2009 GEPHART

  3. Disadvantages of taking oral drugs • Drug delivery is often erratic and incomplete • It is highly dependent upon patient compliance • There are increased sources of drug-drug and drug-nutrient toxins • Many drugs degrade in GI environment • Exposes drugs to first-pass effect TIP 2009 GEPHART

  4. Oral administration • The action of a drug is dependent upon it reaching its site of action whereby it delivers an effective response for therapeutic action. • The important processes involved in the pharmacokinetic phase of drug action are: • Absorption of the drug • Distribution of the drug • Metabolism of the drug • Elimination of the drug TIP 2009 GEPHART

  5. Absorption of the drug • Most orally administered drugs are absorbed through the membranes of the GI tract. • The rate of absorption will depend upon the following: • the rate of dissolution of the solid (pill) into a solution • the pH of the medium containing the drug • the lipid-aqueous medium partition coefficient of the drug • the surface area of the absorbing region of the GI tract. TIP 2009 GEPHART

  6. Rate of dissolution of the solid into solution • When a drug is administered orally via tablet, capsule, or suspension, the rate of absorption often is controlled by how fast the drug particles dissolve in the fluid at the site of administration. Hence, the dissolution rate often is the rate-limiting (slowest) step in the following sequence: dissolution Absorption Solid Drug Drug in Systemic circulation Drug in solution Step 1 Step 2 TIP 2009 GEPHART

  7. Rate of dissolution of the solid into solutioncontinued • Factors controlling dissolution, such as solubility, ionization, or surface area, will then control the overall dissolution process. • dC/dt = dissolution rate • D is the coefficient of the dissolving material of the drug • h is the thickness of the diffusion layer surrounding the dissolving solid particles • S is the surface area of the dissolution solid • the drug concentration in the diffusion layer is equal to Cs TIP 2009 GEPHART

  8. pH of the medium containing the drug • Solubility is another factor determining the rate of dissolution. • Salts of weak acids and weak bases generally have much higher aqueous solubility than the free acid or base; therefore, if the drug can be given as a salt, the solubility can be increased, and should have improved dissolution. For weak acids: For weak bases: The dissolution rate of weak bases will decrease with increasing pH and the dissolution rate of weak acids decreases with increasing hydrogen ion concentration. TIP 2009 GEPHART

  9. The pH of a particular drug has an effect on the movement of a drug through a membrane. It also has an effect on the dissolution of the drug into the solvent it is placed in. Please go to the link to the right to complete this activity. Please go to the following:http://www.icp.org.nz/html/ph.htmto complete the activity TIP 2009 GEPHART

  10. Lipid-aqueous medium partition coefficient of the drug • A drug has to pass through a number of biological membranes in order to reach its site of action. • Organic medium/aqueous system partition coefficients were the obvious parameters to use as a measure of the ease of movement of the drug through these membranes. • The n-octanol- water system is frequently chosen because it appears to be a good mimic of lipid polarity and has an extensive database. TIP 2009 GEPHART

  11. Partition coefficient Definition The partition coefficient is the ratio of the equilibrium concentrations of a dissolved substance in a two-phase system containing two largely immiscible solvents (water and n-octanol) Since the differences are usually on a very large scale, Log10(P) is used. TIP 2009 GEPHART

  12. Partition coefficient (cont.) 1-octanol water OH O H H More accurate results may be obtained if the organic phase is matched to the area of biological activity being studied. n-octanol usually gives the most consistent results for drugs absorbed in the GI tract while less polar solvents give more consistent correlations for drugs crossing the blood-brain barrier. More polar substances give more consistent values for buccal absorption (soft tissues in the mouth). TIP 2009 GEPHART

  13. Surface Area • The surface area per gram (or per dose) of a solid drug can be changed by altering the particle size • Generally, as the surface area increases, the drug will dissolve more rapidly. Therefore, many poorly soluble and slowly dissolving drugs currently are marketed in a micronized or microcrystalline form TIP 2009 GEPHART

  14. Drug absorption and permeation • Lipinski Rule of Five • The Lipinski ‘rule of 5’ was derived by an analysis of the key properties of 2,245 drug molecules believed to have entered Phase II clinical trials. • States that compounds are likely to have good absorption and permeation in biological systems and are more likely to be successful drug candidates if they follow the rule of “five.” TIP 2009 GEPHART

  15. Lipinski Rule of Five • Five or fewer hydrogen-bond donors • Ten or fewer hydrogen-bond acceptors • H-bond donors are expressed as the sum of OH’s and NH’s and H-bond acceptors as the sum of O’s and N’s. • Molecular weight less than or equal to 500 • Calculated logP less than or equal to 5 • Compound classes that are substrates for biological transporters are exceptions to the rule. TIP 2009 GEPHART

  16. Drug absorption • Drugs absorbed from the GI tract must pass through the GI tract membrane, liver, and other organs in order to reach the general circulation system. • The physiology of drug absorption from the GI tract has a direct effect on the bioavailability (F) of a drug. TIP 2009 GEPHART

  17. The oral availability of a drug can be compared by examining the drug absorption and the first pass metabolism of the drug. The activity provided here will give you the opportunity to examine the conditions under which the drug will reach the blood stream. Please complete all activities provided. Please complete the activity at:http://www.icp.org.nz/html/oral_availablity.html TIP 2009 GEPHART

  18. Area under the curve • Since the area under the plasma concentration-time curve (AUC) for a drug is a measure of the total amount of drug reaching the general circulatory system, the bioavailability of a drug may also be defined in terms of the AUC as: • F = AUC/dose • Or absolute bioavailability is: F = AUCpo/AUCiv TIP 2009 GEPHART

  19. Absorption and elimination • The increase in plasma concentration occurs as a drug is absorbed. It is accompanied by elimination, which starts from the instant the drug is absorbed. • The rate of elimination increases as the concentration of the drug in the plasma increases to the maximum absorbed dose. Figure 1: graph of the concentration vs. time of a drug that is intravenously administered (red arrow) and one that is orally administered (blue arrow). (Lemke, Williams, Roche, & Zito, 2008) TIP 2009 GEPHART

  20. The plasma concentration (Cp) is directly proportional to the dose rate, and inversely proportional to the clearance. As you complete this activity, examine the relationship between the plasma concentration, the dose rate, and the clearance. Please go to: http://www.icp.org.nz/html/drug_clearance_1.htmlto complete the above activity TIP 2009 GEPHART

  21. Compartmental concepts • The most commonly employed approach to pharmacokinetic characterization of a drug is to depict the body as a system of compartments, even though these compartments often do not have any apparent physiologic reality. • The one-compartment model considers the body as a single homogenous unit (central compartment). This simplest model is particularly useful for pharmacokinetic analysis of plasma concentration vs. time for drugs that are very rapidly distributed in the body. The two-compartments model consists of a central component, which includes the plasma and other highly perfused organs, connected to a peripheral or tissue compartment. Each compartment can be considered to include a group of tissues, fluids, or parts of organs. (Lemke, Williams, Roche, & Zito, 2008) TIP 2009 GEPHART

  22. One and Two compartment models Figure 2: Schematic representation of the one-compartment (I) and the two-compartment (II) models commonly used in pharmacokinetics. Arrows represent transfer of a drug because of the first-order process. C, central compartment (plasma, highly perfused organs); P, peripheral (tissue) compartment. (Lemke, Williams, Roche, & Zito, 2008) TIP 2009 GEPHART

  23. The compartment models illustrated show the volume of distribution of drugs dependent upon their properties. Please complete all sections of this activity. Please click below to complete above activity:http://www.icp.org.nz/html/volume_of_distribution.html TIP 2009 GEPHART

  24. The amount of time it takes the concentration of a drug to fall to half its original value is known as its biological half-life (t1/2). For drugs that exhibit first order elimination kinetics t1/2 = 0.693/kel Half-life TIP 2009 GEPHART

  25. The half-life of a drug is the time it takes for the concentration to halve. Examine the activity here and look at the relationship between the concentration, volume delivered and the t-1/2 value. Please click below to complete above activity:http://www.icp.org.nz/html/half_life.html TIP 2009 GEPHART

  26. ( Volume of distribution relationships to dosing Lemke, Williams, Roche, & Zito, 2008) TIP 2009 GEPHART

  27. Therapeutic effects and dosing of oral medications • When a single dose of a drug is administered orally, its plasma concentration increases to a maximum value (Cmax) at tmax before falling with time.’ • The change in plasma concentration-time curve for a single oral dose shows the time (tlag) for the drug to reach its therapeutic window concentration, the tmax, and the Cmax. • All of these measurements are useful in determining the correct dosage form for a drug and also the selection of analogues for development. TIP 2009 GEPHART

  28. Oral Dosing Click here for video Minimum toxic concentration Minimum effective concentration TIP 2009 GEPHART

  29. Dosing: Single dose oral drugs can be compared to multiple dosing. Loading helps to bring the initial concentrations up to an effective concentration more quickly. Compare the different types of dosing within the activity provided. Compare the therapeutic windows of each trial. Please click below to complete above activity: http://www.icp.org.nz/html/dose.html TIP 2009 GEPHART

  30. Conclusion • The therapeutic effect of oral drugs depends upon the absorption, distribution, metabolism, and elimination of the drug within the body system. • The absorption and distribution of a drug can be influenced by the particle size, pH, partition coefficient, and the molecular weight of the drug. • The rate of absorption and elimination affect the therapeutic levels that can be achieved within the body. • Dosing of a drug is dependent upon the rate of absorption and the rate of elimination. The kinetics of these processes help to determine the frequency and dosage form of the drug. TIP 2009 GEPHART

  31. References • Lemke, T. L., Williams, D. A., Roche, V. F., & Zito, S. W. (2008). Foye's Principles of Medicinal Chemistry . Philadelphia: Wolters Kluwer. • Lipinski's Rule of Five. (1997). Retrieved February 12, 2009, from Group Seminar Lipinski Rule of Five: bioinfo3d.cs.tau.ac.il/Education/CS01a/GroupSeminar/LipinskiRuleOfFive.ppt • Thomas, G. (2003). Fundamentals of Medicinal Chemistry. West Sussex, England: Wiley. TIP 2009 GEPHART

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