Term
Distinguish between semisynthetic and synthetic drugs. |
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Definition
semi - altered natural cmpds
synthetic - entirely made by chemists |
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Term
What does the ending "-mab" indicate about that drug? |
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Definition
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Term
Distinguish between proprietary and non-propietary drugs. |
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Definition
proprietary - trade name; original drug-->$$ to make and market; patent protection for 17 yrs
non-proprietary - generic name; less $$, must achieve 80-120% blood levels as original |
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Term
Which drugs end with -olol? |
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Definition
beta-adrenergic antagonist |
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Term
Which drugs end with -caine? |
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Definition
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Term
Which drugs end with -dipine? |
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Definition
Ca2+ channel antagonists of the dihydropyridine type |
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Term
Which drugs end with -tidine? |
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Definition
histamine2 receptor antagonists |
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Term
Which drugs end with -prazole? |
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Definition
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Term
Which drugs end with -zosin? |
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Definition
alpha1 receptor antagonists |
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Term
Which drugs end with -pril? |
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Definition
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Term
Describe the implications for the 5 schedules for prescribing practice under the Controlled Substance Act. |
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Definition
1 - no acceptable medical use; but okay to use in research
2 - has acceptable medical use; abuse = severe dependency; oral ppx orders are not accaptable unless it's an emergency
3 - acceptable medical use; abuse = moderate dependency; <5 refills before 6 mo.
4 - acceptable med. use; abuse = limited dependency; <5 refills in 6 mo.
5 - acceptable med. use; may even be obtained at descretion of pharmacist w/o prescription; unlimited refills |
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Term
How is the regulation of herbal products different to that of ppx drugs? |
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Definition
burden of proof that herbal product is unsafe is upon FDA and composition is not standardized due to variability in botanical components
ppx drugs must be proven safe prior to marketing |
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Term
What are the approaces to drug discovery? |
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Definition
ID new drug target---> design based on desired function---> screen known products---> chemical modification to activate drug |
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Term
Distinguish between forward and reverse pharmacology processes. |
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Definition
forward: compound discovered--->usefu mechanism determined
reverse: molecular target ID'ed---> desired drug designed for target |
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Term
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Definition
median lethal dose: fatal to 50% of animals
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Term
Define the term "no effect dose." |
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Definition
max dose without toxic effect |
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Term
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Definition
max tolerated dose: mild-sublethal toxic effects |
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Term
What dose is usually administered to humans in Phase 1 clin. trials? |
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Definition
1/100th - 1/10th of no effect dose |
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Term
Distinguis b/t requirements and purposes of the 4 phases of drug development. |
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Definition
Phase 1 CT - IND (investigational new drug) application filed with FDA; 20-100 healthy volunteers; to assess safety and pharmacodynamics
Phase 2 CT - 100-200 pts; assess efficacy and adverse drug reactions
Phase 3 CT - 1000-6000 pts; assess efficacy and adverse rxns against current standard; NDA (new drug applcation) filed upon completion
Phase 4 CT - post marketing surveillance |
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Term
Which phases of drug development exclude pregnant women? |
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Definition
Phase 1-3; categories A - X ---> no risk shown - risk outwieghs benefit |
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Term
Which measures have been introduced to ensure clinical trials in children? |
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Definition
FDA Modernization Act '97 - patent extension incentive
Pediatric Rule '98 - demands studies be done |
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Term
Are the elderly inclided in clinical trials? |
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Definition
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Term
Describe the way in which the following factors determines the rate of passive diffusion across lipid membranes.
1. degree of ionization
2. lipid solubility
3. concentration gradient |
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Definition
1. less ionized---> more lipid soluble---> faster diffusion
2. more lipid soluble---> faster diffusion
3. greater concentration gradient of non-ionized form---> faster diffusion
(weak acids: when pH<pKa; weak bases: when pH>pKa) |
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Term
Describe the "First Pass" effect disadvantage of oral drug admin. |
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Definition
1st pass effect = loss of drug as it's metabolized within gut wall and liver---> less reaches systemic circulation |
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Term
What is the disdvantage of IV drug admin in terms of solubility? |
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Definition
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Term
What is the major advatnage to subcutaneous drug admin. in terms of rate of absorption? |
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Definition
can CONTROL rate of absorption by:
- altering blood flow (epinephrine; cold/heat)
- altering vehicle (oil vs. aqueous) |
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Term
What is a major advantage of inhalation drug admin. in terms of rate of absorption? |
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Definition
very rapid absorption but hard to control dosage size |
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Term
What is the purpose of intrathecal (sbarachnoid) admin? |
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Definition
to enusre entry into CSF and CNS; e.g. spinal anesthesia |
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Term
How does drug absorption vary in the SI compared to the stomach? |
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Definition
in SI:
- largest SA for absorption
- pH progressively more alkaline
- longer transit time |
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Term
List ways in which drug absorption from parenteral (non-GI) sites can be retarded or enhanced. |
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Definition
- blood flow---> reduction = slower absorption = longer duration of action (e.g. epinephrine-->vasocinstriction of local capillaries)
- pH---> causes non-ionized form to be prevalent---> poorly water soluble and percipitates out---> slower absorption |
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Term
Define the following terms relating to solid dosage forms and describe their significance.
- disintegration
- dissolution (How can this be prolonged?) |
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Definition
- disintegration: break-down into smaller solid particles---> increase SA
- dissolution: entry into aqueous GI medium---> availability for absorption (rate limiting)
prolonged by coating with water-insoluble material (e.g. wax) or embeddin in matrix |
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Term
List the various body compartments and aproximate percentage body weight of fluid in each. |
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Definition
total body water: 60%
ECF: 20% (4% plasma; 16% in ISF)
ICF: 40% |
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Term
How do plasma binding proteins affect drug absorption? |
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Definition
enhances it cause plasma protein binding keeps conc. of free drug low so that more of it gets absorbed to systemic circulation |
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Term
Describe the concept of "reversibility" of the plasma protein binding of drugs. |
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Definition
plasma proteins can serve as drug "depot" cause as more free drug leaves circulation, more drug dissociates from bound to unbound form within plasma |
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Term
What is the relationship between plasma protein saturation and toxicity? |
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Definition
increase in drug concentration beyond plasma protein-binding capacity (i.e. beyond saturation)---> increase in [free drug]---> more diffusion into tissues (site of receptors and drug action)---> toxicity! |
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Term
Which types of drugs typically cross the adult BBB? What are exceptions? |
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Definition
highly lipid soluble
exceptions:
- infant BBB - relatively permeable to water-soluble drugs;
- inflammation alters permeability
- active transport possible through choroid plexus
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Term
Describe the role of P-glycoprotein (MDR1). |
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Definition
ATP-binding membrane protein that actively transports proteins and lipids across cell membranes |
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Term
What are "targeted drugs?" |
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Definition
Drugs that are designed to achieve have highest concentration at site of action. |
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Term
Describe the role of OATP1B1. |
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Definition
organic anion transporter polypeptide that enhances hepatic uptake during first pass effect |
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Term
What is the relationship b/t the redistribution of drugs and blood flow? |
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Definition
drugs usually redistribute according to blood flow---> more rapidly perfused organs are usually the first to recieve drug;
subsequent distribution to less rapidly perfused organs (muscle and adipose)---> drug storage and lower drug concentration available for rest of the organs (decreased duration of action!) |
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Term
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Definition
vol. of fluid that is required to contain drug at same concentration as plasma |
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Term
What volume of fluid constitutes renal plasma flow and undergoes glomerular filtration in a 70kg person? |
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Definition
125 ml/min (1/5th of renal plasma flow--> 650 ml/min) |
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Term
Compare the renal clearance of lipid-soluble and insoluble drugs |
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Definition
lipid-soluble drugs are passively reabsorbed---> slow excretion
lipid-insoluble---> not reabsorbed (cause of charge), rapidly excreted |
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Term
How does alteration of the urine pH with sodium bicarb affect the excretion of weak acids or bases? |
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Definition
sodium bicarb: increases pH---> favors ionized form of weak acids; non-ionized form of weak bases----> enhanced secretion of weak acids
ammonium chloride: decreases pH---> favores non-ionized form of weak acids; ionized form of weak bases---> enhanced secretion of weak bases
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Term
Describe the role of transporters in renal clearance of a drug. |
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Definition
if transporter has higher affinity for drug than plasma protein, drug preferentially binds transporter and is excreted |
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Term
Which factors alter active secretion/reabsorption versus passive reabsorption? |
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Definition
active - diseased tubules; competition for transport sites
passive - pH alterations |
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Term
What is the equation for renal clearance? |
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Definition
Clr = U x V/Cp x T
units: mg/ml and min |
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Term
What size and polarity drugs usually undergo active billiary excretion? |
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Definition
large (>300 Daltons); polar drugs |
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Term
Describe the process of enterohepatic cycling. |
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Definition
drugs excreted into from liver bile---> reabsorbed at duodenum---> returned to liver via portal circulation with small amt released to systemic circulation (drug reservoire action) |
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Term
What is the major route of excretion of volatile chemicals with low solubility coefficients? |
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Definition
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Term
Which organ is predominantly responsible for biotransformation and what is the significance of this process? |
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Definition
liver (SER)
biotransformation---> drug transformed to less pharmacologically active, more polar form----> more readily secreted via kidneys and bile---> less toxicity |
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Term
Describe the general mechanism of action of CYP on drug oxidation. |
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Definition
drug binds oxygenated CYP---> complex is reduced---> undergoes internal rearrangement----> re-oxidized----> oxidized drug dissociates |
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Term
Which Phase 1 reactions involve intestinal anaerobic bacteria? |
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Definition
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Term
Which tissue is primarily responsible for hydrolysis Phase 1 rxns? |
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Definition
many diff types of tissues |
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Term
Where do conjugatio reaction (Phase 2) typically occur? |
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Definition
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Term
What is the purpose of conjugation reactions? |
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Definition
increase water solubility for enhanced excretion |
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Term
How does age influece biotransformation? |
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Definition
newborn: drug metabolizing enzymes not yet fully developed---> very slow biotransformation
elderly: drug metabolzing enzymed decreased due to decreased liver function---> v. slow biotransformation |
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Term
What is the equation for liver extraction ratio? |
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Definition
Ca-Cv/Ca
(fraction of arterial drug content that is extracted during single passage through liver) |
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Term
Distinguish between substrate-limited and enzyme-limited drugs. |
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Definition
substrate-limited drugs: high extraction ratio---> rate of metabolism is sensitive to hepatic blood flow
enzyme-limited drugs: low extraction ratio---> rate of metabolism is not sensitive to hepatic flow
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Term
Compare the effect of plasma binding to the rate of metabolism of a drug with a high extraction ratio to that of one with a low extraction ratio. |
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Definition
high extraction ratio--->free drug efficiently taken up by liver---> shifts plasma equilibrium to unbound (so plasma protein binding has little effect on rate of metabolism.
low extraction ratio---> no shift in equilibrium because of amount of limited enzyme available to metabolize drug (so rate of metabolism is limited by plasma protein binding) |
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Term
Define "therapeutic range." |
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Definition
range b/t maximum effective concentration (Cpe) and minimum effective concentration (Cpm) of drug |
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Term
Describe the first-order process of elimination. |
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Definition
first-order:
rate of elimination is proportional to plasma concentration (Cp), which is proportional to the drug amount (A); i.e. constant fraction of drug is eliminated per unit time
assumption: drug has equilibriated into its volume of distribution |
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Term
What does the slope of the lnCp vs. time curve of 1st-order elimination represent? |
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Definition
Ke - fraction of drug eliminated per unit time |
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Term
In the case of a 2-compartment model, how is Cp obtained from the LnCp vs. time graph? |
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Definition
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Term
Describe zero-order kinetics. |
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Definition
elimination occurs at constant rate regardless of Cp; cause elimination proccesses are saturated |
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Term
Equation for total body clearance (Clt.b.)? |
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Definition
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Term
What is Ka of first-order absorption? |
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Definition
the fraction of drug that is absorpbed per unit time; stays constant |
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Term
What causes the shape of the Cp vs. time curve of an orally administered drug? |
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Definition
positive slope---> rate of absorption is relatively greater than rate of elimination
negative slope--> vice versa |
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Term
How does a slower Ka affect the shape of the absorption curve? |
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Definition
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Term
How does a smaller dose affect the shape of the absorption curve? |
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Definition
lower Cp, but occurs just as fast |
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Term
How does a fixed Ka but lower Ke affect the shape of the absorption curve? |
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Definition
greater Cp, longer duration of drug action |
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Term
Equation for bioavailability? |
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Definition
bioavail. = AUCoral/AUCIV |
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Term
Equation for steady-state plasma concentration following maintenance therapy? |
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Definition
Amount(Ass) = rate of administration (Kad)/(rate of elimination (Ke)
assume zero-order kinetics for Kad
Cpss = Ass/Vd = (Kad/Ke)/Vd = Kad/clearance |
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Term
How many t1/2's are typically required to reach 90% steady state plasma drug conc.? |
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Definition
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Term
Equation for maintenance dose? |
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Definition
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Term
Equation for loading dose (dose given to achieve CpE rapidly)? |
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Definition
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Term
What effect does halving both the dose and dosage interval have on the steady state level of the drug? |
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Definition
steady state level ---> unchanged, but less fluctuation around that level |
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Term
Equation for Cpss following IV infusion? |
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Definition
Cpss = infusion rate/total clearance |
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Term
How does altered drug structure affect affinity for its receptor? |
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Definition
alters affinity for a receptor but NOT it's pharmacological efficacy |
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Term
Describe the relationship btween competitor concentration and affinity and the rightward shift of the concentration binding relationship for the given drug. |
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Definition
higher concentration or higher affinity---> greater rightward shift, higher Kd |
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Term
What is the relationship between the % receptors bound by a given drug and the concentration and affinity of competitor added? |
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Definition
higher concentration or higher affinity---> less of the given drug bound at a given concentration
[image]
affinity of C > of B
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Term
Is there a limit to the increase of binding of a drug to receptors that can be produced by modulators? |
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Definition
Yes, binding of drug will not increase beyond 100% bound no matter how much additional modulator is present. |
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Term
Is there a limit to the leftward shift of concentration binding relationship of drug to receptors that can be produced by a modulator? |
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Definition
No. Extent of leftward shift depends on modulator concentration and modulator affinity. |
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Term
Describe the maximum response possible through drug-receptor interaction? |
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Definition
100% receptors bound and activated by drug |
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Term
What is pharmacological efficacy? |
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Definition
ability of drug to bind and induce maximum response; can range through 0-100%
antagonists have pharm. efficacy = 0%
partial agonists = <100%
full agonists = 100% |
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Term
What is the relationship between drug affinity to a receptor and its pharm. efficacy? |
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Definition
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Term
Describe the action of an inverse agonist. |
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Definition
reduces the activity of a receptor below its basal activity |
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Term
Distinguis between Kd and EC50. |
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Definition
Kd = [drug] required to bind 50% of receptors; measure of affinity
EC50 = [drug] required to produce 50% maximal response; measure of potency |
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Term
What is the relationship between affinity and potency?
Why is EC50 slightly < Kd? |
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Definition
potency reflects affinity; higher affinity ----> higher potency
EC50<Kd because drug binds "spare" receptors contribute amplification that allows 50% max response before binding 50% receptors |
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Term
How does competition affect Kd and EC50? |
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Definition
increases Kd causing an apparent decrease in affinity; increases EC50--->rightward shift of % response vs. [drug] curve |
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Term
How does the [antagonist] and antagonist affinity affect the potency of an agonist? |
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Definition
higher [antagonist] and/or higher antag. affinity---> higher agonist EC50---> lower potency |
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Term
What effects do antagonists have on agonist efficacy? |
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Definition
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Term
How do modulators alter effect of an agonist? |
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Definition
increase affinity of effector binding site so that drugs or other molecules may bind more easily to that binding site |
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Term
What is the effect of modulators on EC50 of agonists? |
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Definition
decreases EC50---> increased agonist potency |
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Term
What is the relationship between [modulators] and modulator affinity and agonist EC50? |
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Definition
higher [modulator] and/or increased modulator affinity---> lower EC50 (more dramatic leftward shift of concentration-response curve) |
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Term
Is the extent to which modulators shift the concentration response relationship to the left limited? |
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Definition
Yes. Beyond maximal saturation of receptor modulation sites, EC50 will not be reduced regardless of further increase in modulators. |
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Term
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Definition
dose required to produce desired effect in 50% of patients |
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Term
Are A and B equally efficacious? Equally potent?
[image]
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Definition
equally efficacious because can obtain desired effect in 100% of patients at some concentration.
NOT equally potent. A is more potent than B cause of lower ED50. |
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Term
Define variabe response to a drug. |
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Definition
for given [drug] at site of action or dose of drug given, response induced by drug declines with repeated dosing or maintained [drug] |
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Term
Define cellular tolerance. Is this a response to agonists or antagonists or to both? |
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Definition
decrease in response to drug over milliseconds due to presence of constant drug concentration at site of action.
produced by agonists |
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Term
List the two mechanisms of cellular tolerance. |
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Definition
1. receptor internalization
2. receptor desensitization (effector uncoupling)--> binding occurs but response is diminished |
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Term
Describe metabolic (dispositional) tolerance. Is this response produced by agonists, antagonists, modulators, or all 3?
What is the mechanism of metabolic tolerance? |
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Definition
tolerance to drug due to repeated dosing over several days
produced by all 3
mechanism: induction of metabolizing enzymes |
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Term
What is the relationship b/t drug concentration and response in the case of metabolic tolerance? |
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Definition
As conc. increases with each repeated dose, response decreases due to induction of metabolic enzymes
but decrease in response is LIMITED by saturation of these enzymes |
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Term
What is the relationship b/t drug concentration and response in the case of cellular tolerance? |
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Definition
internalization causes response to decrease while drug concentration stays constant
decrease in response is LIMITED by limit to decrease in receptor internalization |
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Term
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Definition
drug dose that produces toxicity in 50% of patients |
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Term
What is the relationship between the safety of a drug and the difference between ED50 and TD50? |
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Definition
the greater the difference between ED50 and TD50 (i.e. ED50<<<TD50), the safer the drug |
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Term
What does therapeutic index measure and how is it determined? |
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Definition
measures safety
= LD50/ED50
higher number---> safer drug |
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Term
What is the standard safety margin? |
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Definition
= TD1/ED99
(dose that's toxic to 1% of patients/dose that's therapeutic to 99% of patients) |
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