Week 1 Flashcards
Pharmacokinetics -
What the body does to the drug
Absorption:
The movement of a drug from its site of administration into the blood
Distribution:
The movement of drugs throughout the body
Metabolism:
Transformation of a drug by enzymes into metabolites
Excretion:
Drug removal from the body
Pharmacodynamics -
What the drug does to the body; Study of the relationship between the drug and a target cell or receptor to produce a therapeutic effect in a patient
Pharmacogenomics -
Study of the genetic attributes of an individual that lead to variable responses to drugs
Pharmacoeconomics -
Description and analysis of the cost of drug therapy to healthcare systems and society
Drug:
any chemical that produces a measurable biological response
Pharmacology:
the study of drugs and their actions
Pharmacotherapeutics:
the use of drugs to diagnose, prevent, or treat disease or to prevent pregnancy
Prodrugs:
Inactive compounds that rely on metabolism to become active
Bioavailability:
percentage of administered dose that enters the bloodstream
Efficacy:
index of the maximal response a drug can produce regardless of dose
Potency:
index of how much drug must be administered to elicit a desired response
ED50 =
amount of drug that produces the desired effect in 50% of the people taking it
LD50 =
amount of drug that produces toxicity in 50% of the people taking it
Therapeutic index:
Ratio of LD50 to ED50; Drugs with narrow therapeutic index have a very narrow range between the dose that is effective and the dose that is toxic
Genes:
a stretch of DNA which encodes for proteins and determines genetic characteristics.
Genotype:
an individual’s genetic makeup derived from mixing of genes from that individual’s parents
Phenotype:
physical characteristics of an individual based on expression of the genotype
Common Supplements
o Calcium o Echinacea o Fish Oil o Ginseng o Glucosamine and/or Chondroitin Sulphate o Garlic o Vitamin D o St. John’s Wort o Saw Palmetto o Ginkgo o Green Tea
Describe how ABSORPTION affects drug movement throughout the body.
i) Rate of absorption determines how soon effects will begin: ii) Route (e.g. IV, IM, PO, topical, rectal, inhaled, etc..) iii) Characteristic of pharmaceutical preparation (e.g. immediate versus extended release) iv) Most oral absorption occurs in the small intestine v) Amount of absorption determines intensity of effect: (1) Plasma drug levels (2) Bioavailability: percentage of administered dose that enters the bloodstream (a) 100% for parenteral administration (b) Ranges for oral administration (c) Low bioavailability = higher dose needed
Describe how DISTRIBUTION affects drug movement throughout the body.
i) Factors affecting distribution (1) Blood flow (2) Lipid/water solubility (3) pH (a) pH changes the charge of drugs depending on the pKa (4) Protein binding (a) Albumin (b) Can increase circulation, decrease metabolism and excretion (c) Needs to be unbound to have effect ii) Passage of drugs across membranes (1) Drugs may need to pass through membranes to get to site of action (a) Three ways: Channels and pores, Transport systems (P-glycoprotein), Direct penetration of the membrane (2) Medications that do NOT pass through the plasma membranes easily: (a) Polar molecules (b) Ions (c) Large molecules iii) Medications that DO pass through the plasma membranes easily: (1) Neutral molecules (2) Lipophilic (3) Small iv) Barriers to know about (1) Blood Brain Barrier (a) Capillary endothelial cells are surrounded by a sheath of glial tissue (b) Impermeable to water soluble drugs and ionized drugs (2) Placental Barrier (a) Lipid membrane that allows passage of drugs by simple diffusion (b) Smaller molecules cross most easily v) Transport systems (1) E.g. p-glycoprotein (P-gp) (a) Membrane bound transport system which moves drugs from across membranes (i) Member of ATP binding proteins (b) Affects level of substrate available for absorption/elimination (i) If an P-gp inhibitor is given, P-gp substrate levels will rise (c) Examples of P-gp substrates: carvedilol, diltiazem, digoxin (d) Examples of P-gp inhibitors: verapamil, quinidine, cyclosporine, ketoconazole (2) Protein Binding (a) Drugs can form reversible bonds with various proteins in the blood (i) Albumin 1. Most abundant and important 2. Large molecule that always remains in the bloodstream 3. Impacts drug distribution – if drug is bound to protein, it cannot leave the blood to get to its site of action (protein is too large) a. E.g. phenytoin
Describe how METABOLISM affects drug movement throughout the body.
i) Transformed into a molecule that is: (1) More easily excreted (a) Usually becomes more water soluble (less lipid soluble) (2) Increased or decreased therapeutic action (3) Increased or decreased toxicity ii) Phase I and Phase II Metabolism (1) Phase I metabolism: Oxidation, reduction, and hydrolysis (a) Cytochrome P450 (CYP 450) system (2) Phase II metabolism: Conjugation reactions (a) E.g. glucuronidation, sulfation iii) Prodrugs (1) Inactive compounds that rely on metabolism to become active (2) Example: codeine is not active as codeine, but is metabolized to morphine by CYP2D6 iv) First pass metabolism (1) When oral drugs are absorbed by the GI tract they are carried directly to the liver (a) Some drugs can be completely inactivated on first pass if liver is able to metabolize (2) For this reason some medications cannot be given orally (a) E.g. nitroglycerin v) Hepatic Dose Adjustments (1) For medications metabolized in the liver, may need to adjust the dose in patients with liver dysfunction. (2) Stages of liver disease: Child’s Pugh Score (a) Given points for ascites, encephalopathy, bilirubin, albumin, and prothrombin time (b) Higher points value = worsening liver function
Describe how EXCRETION affects drug movement throughout the body.
i) Most commonly occurs in the kidneys ii) Steps in renal excretion: (a) Glomerular filtration to passive and active tubular reabsorption to active tubular secretion iii) Renal function (1) Methods of assessing renal function: (a) Estimated glomerular filtration rate (eGFR) (b) Creatinine clearance (CrCl) iv) Renal dosing (1) If patient’s kidneys are not working properly, may need to adjust dose based on renal function to prevent toxicity.
Identify the importance of the CYP450 system in drug metabolism and how drug interactions and genetics can affect the metabolism of medications.
a) Cytochrome P450 (CYP450) enzymes i) Primarily found in the liver ii) Account for 70-80% of the enzymes involved in drug metabolism iii) Examples: (1) CYP3A4 – 50% of drug metabolism (2) CYP2D6 – 25% of drug metabolism (a) Selective serotonin reuptake inhibitors (SSRIs), Tricyclic antidepressants (TCAs), Beta blockers, codeine (3) CYP2C9 (a) Warfarin, antiepileptic drugs (phenytoin), glipizide
Recognize how changes in pharmacokinetics in PEDIATRIC patients may affect medication therapy.
i) Children are NOT just small adults ii) Absorption (1) Normal pH around age 2 (2) Normal motility around 6-8 months iii) Distribution (1) Decreased protein binding (2) Adult values between 7 – 12 years (3) More lipid soluble meds may cross BBB iv) Metabolism (1) Increased metabolic rate and clearance for first 2 years (2) Decreased metabolic rate and clearance until puberty v) Elimination (1) Kidney matures around 6 – 12 months
Recognize how changes in pharmacokinetics in GERIATRIC patients may affect medication therapy.
i) absorption (1) May have decreased acid secretion, increased gastric pH, decreased first pass effect leading to increased bioavailability (2) Medications (a) Proton pump inhibitors (b) H2 receptor antagonists (3) Drug interactions (a) Drug-drug (e.g. sucralfate) (b) Drug-food (e.g. tetracyclines with milk) (c) Drug-disease state (e.g. s/p bariatric surgery) ii) distribution (1) Decrease in lean body mass (a) Impact drug volume of distribution (i) Fat soluble medications: duration of action frequently prolonged (e.g. benzodiazepines) (ii) Water soluble drugs: e.g. acyclovir dosed based on ideal or adjusted body weight (2) Decreased blood flow and tissue perfusion (3) Decrease in serum albumin and protein binding iii) Metabolism (1) Changes in hepatic function with aging (a) Decreased hepatic blood flow (especially in heart failure, etc..) (b) Decreased ability to recover from injury (alcohol, hepatitis, etc..) (c) Decreased CYP450 activity with decreasing hepatic function iv) Elimination/Excretion (1) Decreased renal function associated with aging (a) Age-related decrease in creatinine clearance (b) Estimates for renal function based on various equations (i) E.g. eGFR, Cockcroft-Gault (c) Drugs doses and recommendations based on renal function to avoid toxicity
Recognize how changes in pharmacokinetics in PREGNANT patients may affect medication therapy.
i) Most drugs taken by pregnant women will cross the placenta and expose the developing embryo and fetus to pharmacologic and teratogenic effects ii) Critical factors include: (1) Properties of the drug (2) Rate and amount that crosses placenta (3) Duration of exposure (4) Distribution characteristics in fetal tissues (5) Stage of placental and fetal development iii) Pregnancy Categories (1) Pregnancy categories are being taken away – in future will just have a description of risks/studies
Define Half-life
time required for the amount of drug in the body to decrease by 50%
What is half-life dependent on?
(1) Clearance (2) Volume of distribution (3) Steady state
