In pharmacology, bioavailability is used to describe the fraction of an administered dose of unchanged drug that reaches the systemic circulation, one of the principal pharmacokinetic properties of drugs. Pharmacology (from Greek grc φάρμακον pharmakon, "drug" and grc -λογία -logia) is the study of how Drugs Systemic circulation is the portion of the Cardiovascular system which carries Oxygenated Blood away from the heart to the Body, and returns Pharmacokinetics (in Greek: “pharmacon” meaning drug and “kinetikos” meaning putting in motion the study of time dependency sometimes abbreviated as “PK” is a Medication, also referred to as medicine, can be loosely defined as any substance intended for use in the diagnosis cure mitigation treatment or prevention of disease By definition, when a medication is administered intravenously, its bioavailability is 100%. Intravenous therapy or IV therapy is the giving of Liquid substances directly into a Vein. However, when a medication is administered via other routes (such as orally), its bioavailability decreases (due to incomplete absorption and first-pass metabolism). In Pharmacology and Toxicology, a route The first-pass effect (also known as first-pass metabolism or presystemic metabolism) is a phenomenon of Drug metabolism whereby the Concentration Bioavailability is one of the essential tools in pharmacokinetics, as bioavailability must be considered when calculating dosages for non-intravenous routes of administration.

Contents 1 Definition 2 Absolute bioavailability 3 Relative bioavailability 4 Factors influencing bioavailability 5 See also 6 References

Definition

Bioavailability is a measurement of the extent of a therapeutically active drug that reaches the systemic circulation and is available at the site of action. ^[1]

It is expressed as the letter F.

Absolute bioavailability

Absolute bioavailability compares the bioavailability (estimated as area under the curve, or AUC) of the active drug in systemic circulation following non-intravenous administration (i. Intravenous therapy or IV therapy is the giving of Liquid substances directly into a Vein. In Pharmacology and Toxicology, a route e. , after oral, rectal, transdermal, subcutaneous administration), with the bioavailability of the same drug following intravenous administration. It is the fraction of the drug absorbed through non-intravenous administration compared with the corresponding intravenous administration of the same drug. The comparison must be dose normalized if different doses are used; consequently, each AUC is corrected by dividing the corresponding dose administered.

In order to determine absolute bioavailability of a drug, a pharmacokinetic study must be done to obtain a plasma drug concentration vs time plot for the drug after both intravenous (IV) and non-intravenous administration. Pharmacokinetics (in Greek: “pharmacon” meaning drug and “kinetikos” meaning putting in motion the study of time dependency sometimes abbreviated as “PK” is a The absolute bioavailability is the dose-corrected area under curve (AUC) non-intravenous divided by AUC intravenous. The European Space Agency 's INTErnational Gamma-Ray Astrophysics Laboratory ( INTEGRAL) is detecting some of the most energetic radiation that comes from space For example, the formula for calculating F for a drug administered by the oral route (po) is given below.

Therefore, a drug given by the intravenous route will have an absolute bioavailability of 1 (F=1) while drugs given by other routes usually have an absolute bioavailability of less than one.

Relative bioavailability

This measures the bioavailability (estimated as area under the curve, or AUC) of a certain drug when compared with another formulation of the same drug, usually an established standard, or through administration via a different route. When the standard consists of intravenously administered drug, this is known as absolute bioavailability.

Factors influencing bioavailability

The absolute bioavailability of a drug, when administered by an extravascular route, is usually less than one (i. e. F<1). Various physiological factors reduce the availability of drugs prior to their entry into the systemic circulation,

Such factors may include, but are not limited to:

• Physical properties of the drug (hydrophobicity, pKa, solubility)
  
• The drug formulation (immediate release, excipients used, manufacturing methods, modified release - delayed release, extended release, sustained release, etc. )
  
• If the drug is administered in a fed or fasted state
  
• Gastric emptying rate
  
• Circadean differences
  
• Enzyme induction/inhibition by other drugs/foods:
  
  • Interactions with other drugs (e. g. antacids, alcohol, nicotine)
    
  • Interactions with other foods (e. g. grapefruit juice, pomello, cranberry juice)
    
• Transporters: Substrate of an efflux transporter? (e. g. P-glycoprotein)
  
• Health of the GI tract
  
• Enzyme induction/inhibition by other drugs/foods:
  
  • Enzyme induction (increase rate of metabolism). e. g. Phenytoin (antiepileptic) induces CYP1A2, CYP2C9, CYP2C19 and CYP3A4
    
  • Enzyme inhibition (decrease rate of metabolism). e. g. grapefruit juice inhibits CYP3A --> higher nifedipine concentrations
    
• Individual Variation in Metabolic Differences
  
  • Age: In general, drugs metabolized more slowly in fetal, neonatal, and geriatric populations
    
  • Phenotypic differences, enterohepatic circulation, diet, gender.
    
• Disease state
  
  • e. g. hepatic insufficiency, poor renal function
    

Each of these factors may vary from patient to patient (inter-individual variation), and indeed in the same patient over time (intra-individual variation). Whether a drug is taken with or without food will affect absorption, other drugs taken concurrently may alter absorption and first-pass metabolism, intestinal motility alters the dissolution of the drug and may affect the degree of chemical degradation of the drug by intestinal microflora. Disease states affecting liver metabolism or gastrointestinal function will also have an effect.

Relative bioavailability is extremely sensitive to drug formulation. Relative bioavailability is one of the measures used to assess bioequivalence between two drug products, as it is the Test/Reference ratio of AUC. Bioequivalence is a term in Pharmacokinetics used to assess the expected in vivo biological equivalence of two proprietary preparations of a drug The maximum concentration of drug in plasma or serum (Cmax) is also usually used to assess bioequivalence.

See also

• ADME-Tox
• Lipinski's Rule of 5
• Biopharmaceutics Classification System
• Caco-2

http://www.nottingham.ac.uk/nursing/sonet/rlos/bioproc/metabolism/default.html

References

1. ^ Shargel, L. ADME is an Acronym in Pharmacokinetics and Pharmacology for '''a'''bsorption, '''d'''istribution, '''m'''etabolism Lipinski's Rule of Five is a Rule of thumb to evaluate Druglikeness, or determine if a Chemical compound with a certain pharmacological or The Biopharmaceutics Classification System is a guidance for predicting the intestinal Drug absorption provided by the U The Caco-2 cell line is an immortalized line of heterogenous human epithelial colorectal Adenocarcinoma cells developed by the Sloan-Kettering ; Yu, A. B. (1999). Applied biopharmaceutics & pharmacokinetics (4th ed. ). New York: McGraw-Hill. ISBN 0-8385-0278-4

© 2009 citizendia.org; parts available under the terms of GNU Free Documentation License, from http://en.wikipedia.org
Dapyx Software network: MP3 Explorer | Ebook Manager | Zenithic