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BIOPHARMACEUTICS CLASSIFICATION SYSTEM

BIOPHARMACEUTICS CLASSIFICATION SYSTEMB asic Absorption and DispositionDrug at Absorption SiteDrug in BodyExcreted DrugMetabolitesabsorptionmetabolismexcre tionClinical Pharmacokinetics, Rowland and Tozer, 2nd Ed, Lea & Febiger, 1989 These models use curve-fitting techniques to estimate kinetic rate constants and other parameters from time-course data for blood, tissue, or excreta; however, the curve-fitted parameters lack biological , J., Pharmac Ther, 12:537-562, 19812 PharmacokineticsDISPOSITION OF DRUGSThe disposition of chemicals entering the body (from Klaassen, Casarett and Doull s toxicology , 5th ed.)

The disposition of chemicals entering the body (from C.D. Klaassen, Casarett and Doull’s Toxicology, 5th ed., New York: McGraw-Hill, 1996). ... Applications of BCS in oral drug delivery technology ... ♫Fortunately, extreme examples are the

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Transcription of BIOPHARMACEUTICS CLASSIFICATION SYSTEM

1 BIOPHARMACEUTICS CLASSIFICATION SYSTEMB asic Absorption and DispositionDrug at Absorption SiteDrug in BodyExcreted DrugMetabolitesabsorptionmetabolismexcre tionClinical Pharmacokinetics, Rowland and Tozer, 2nd Ed, Lea & Febiger, 1989 These models use curve-fitting techniques to estimate kinetic rate constants and other parameters from time-course data for blood, tissue, or excreta; however, the curve-fitted parameters lack biological , J., Pharmac Ther, 12:537-562, 19812 PharmacokineticsDISPOSITION OF DRUGSThe disposition of chemicals entering the body (from Klaassen, Casarett and Doull s toxicology , 5th ed.)

2 , New York: McGraw-Hill, 1996).Introduction BIOPHARMACEUTICS CLASSIFICATION SYSTEM (BCS) Scientific framework for classifying drug substances based on their aqueous solubility and intestinal permeability What is the need for a CLASSIFICATION based on BIOPHARMACEUTICS of the drug? Ans. Its importance in determining bioavailability Route of choice for the formulators Continues to dominate the area of drug delivery technologies. LIMITATIONS Absorption and Bioavailability in the milieu of gastrointestinal tract. Limitations more prominent with the advent of protein and peptide drugs compounds emerging as a result of combinatorial chemistry and the technique of high throughput screening ORAL ROUTE drug solubility drug product quality attributesAPI structure salt form and excipientsBioavailability of drug is determined by extent of drug solubility and permeability Guidance provided by the Food and Drug Administration for predicting the intestinal drug absorptionThe fundamental basis established by Dr.

3 Gordon Amidon Distinguished Science Award (Aug 06 ,FIP) First introduced into regulatory decision-making process in the guidance document on Immediate Release Solid Oral Dosage Forms: Scale Up And Post Approval ChangesBiopharmaceutics CLASSIFICATION SYSTEM Drug development tool that allows estimation of the contributions of 3 major factors, that affect oral drug absorption from immediate release solid oral dosage forms Dissolution Solubility Intestinal BIOPHARMACEUTICS CLASSIFICATION SYSTEM (BCS)(as defined by the FDA after Amidon)

4 SIMILAR IN VIVO DISSOLUTIONSIMILAR IN VIVO ABSORPTIONSIMILAR SYSTEMIC AVAILABILITYD issolution of drug in vivoDrug Concentration in the Membrane DomainIntestinal AbsorptiondeterminesproportionalBasis of BCS (37 100C in aqueous medium with pH range of ) A sufficient number of pH conditions ionization characteristics of the test drug substance A minimum of three replicate determinations of solubility in each pH condition Standard buffer solutions described in pharmacopoeias Methods other than shake flask method (with Justification).

5 E g. acid or base titration methods SOLUBILITY DETERMINATION Not just based on lipophilicity (encompass in vivo effects of efflux and uptake transporters)A. Human studies Mass balance studies Absolute bioavailability studies Intestinal perfusion methods vivo or in situ intestinal perfusion in a suitable animal vitro permeability methods using excised intestinal tissuesD. In vitro permeation studies across a monolayer of cultured epithelial Caco-2 cells or TC-7 cellsDetermination of permeabilityDISSOLUTION DETERMINATION USP apparatus I (basket) at 100 rpm or USP apparatus II (paddle) at 50 rpm.

6 Dissolution media (900 ml): N HCl or simulated gastric fluid, pH buffer, and pH buffer or simulated intestinal fluid. Compare dissolution profiles of test and reference products using a similarity factor (f2). 0 CLASS BOUNDARIESHIGHLY SOLUBLE the highest dose strength is soluble in < 250 ml water over a pH range of 1 to The volume estimate-a glassful (8 ounce)HIGHLY PERMEABLE when the extent of absorption in humans is determined to be > 90% of an administered doseRAPIDLY DISSOLVING when > 85% of the labeled amount of drug substance dissolves within 30 minutes using USP apparatus I or II in a volume of < 900 ml buffer solutions.

7 BCS Class Boundaries: ObjectivesDissolution(Product)Solubility (Drug)Permeability(Drug)Rapid dissolution - ensure that in vivo dissolution is not likely to be the rate determining stepHigh solubility- ensure that solubilityis not likely to limit dissolution and, therefore, absorptionHigh permeability - ensure that drugis completely absorbed during the limitedtransit time through the small intestineBCS -Implications for drug developmentЖApplication in early drug development and then in the management of product change through its life cycleЖAids fundamental understanding of the biopharmaceutical and physical properties of the drugЖAids discriminatory dissolution method developmentЖCan help guide the development of in-vitro/in-vivo correlationsЖCan be used to obtain a biowaiverЖDevelopment of

8 Poorly soluble drugsThis CLASSIFICATION is associated with drug dissolution and absorption model, which identifies the key parameters controlling drug absorption as a set of dimensionless numbers vizBCS defines 3 numbers (no units) An ~ absorption number Do ~ dose number Dn ~ dissolution number ABSGIGIeffTTTRPAn Effective permeabilityRadius of GIResidence time in GITime required forcomplete absorptionAbsorption NumberA function of GI Permeability to Drug Substance SWaterCVDDoHighest Dose Unit250 mLSolubility Dose NumberA function of solubility of drug substanceSolubility mg/mL DISSGIGISTTTCrDDn 23 Diffusivity5x10-6 cm2 mg/cm3 Particle Radius mResidence time in GI 180 minTime required forcomplete dissolutionDissolution

9 NumberA function of drug release from formulationIVIVC expectations for immediate release products based on BCSC lass Solubility Permeability Absorption rate control IVIVC expectations for Immediate release product IHighHighGastric emptyingIVIVC expected, if dissolution rate is slower than gastric emptying rate, otherwise limited or no correlationsIILowHighDissolutionIVIVC expected, if in vitro dissolution rate is similar to in vivo dissolution rate, unless dose is very (permeability) is rate determining and limited or no IVIVC with by caseLimited or no IVIVC is expected.

10 High Solubility Low Solubility High Permeability Class 1 Abacavir Acetaminophen Acyclovirb AmilorideS,I Amitryptyline S,I Antipyrine Atropine Buspironec Caffeine Captopril ChloroquineS,I Chlorpheniramine Cyclophosphamide Desipramine Diazepam Diltiazem S,I Diphenhydramine Disopyramide Doxepin Doxycycline Enalapril Ephedrine Ergonovine Ethambutol Ethinyl Estradiol FluoxetineI Glucose ImipramineI Ketorolac Ketoprofen Labetolol LevodopaS Levofloxacin S LidocaineI Lomefloxacin Meperidine Metoprolol Metronidazole MidazolamS,I Minocycline Misoprostol Nifedipine S Phenobarbital Phenylalanine Prednisolone PrimaquineS Promazine Propranolol I QuinidineS,I Rosiglitazone Salicylic acid Theophylline Valproic acid Verapamil I Zidovudine Class 2 Amiodarone I AtorvastatinS, I AzithromycinS ,I Carbamazepine S,I Carvedilol Chlorpromazine I CisaprideS Ciprofloxacin S Cyclosporine S, I Danazol Dapsone Diclofenac Diflunisal Digoxin S Erythromycin S,I Flurbiprofen Glipizide GlyburideS,I Griseofulvin Ibuprofen Indinavir S Indomethacin Itraconazole S.


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