Term
| what is the most important limited factor in the movement of drugs in the body? |
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Definition
| the lipid:water partition coefficient |
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Term
| what happens to the solubilty of an amount of HA (a weak acid with pKa: 4.4) at pH 1.4? 7.4? |
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Definition
| at 1.4, the majority will be in the non-ionized form (HA) and will therefore be more lipid soluble. At 7.4, H+ and A- will be preferred and will be less soluble |
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Term
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Definition
isolating a drug into a certain environment where its ionization status is favored. this will prevent drugs from going back into cell compartments where they are no longer needed
fetal plasma is slightly more acidic than a mothers, therefore, ion trapping can happen across the placenta |
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Term
| how is glucose usually transferred into muscles cells? |
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Definition
| usually by facilitated diffusion which does not require energy, it simply goes down it conc gradient. glucose is brought into a muscle cell by insulin-sensitive transported protein GLUT4 |
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Term
| SLC superfamily of transporters |
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Definition
| includes organic anion transport proteins (OATP). transports ionic and non-ionic and xenobiotics into cells. relies on facilitated transport or secondary active sym or anti-porters |
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Term
| ABC superfamily of transporters |
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Definition
includes p-glycoprotein and transports xenobiotics out of cell against their gradients to keep cells safe. relies on ATP hydrolysis to do this.
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Term
| difference between enterally and parentally administered drugs? |
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Definition
| enterally is via alimentary system (mouth and rectal), parentally is injection |
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Term
| why is absorption in small intestine always more successful than stomach absorption? |
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Definition
| because there is 200 m2 of surface area in the duodenum and even it its present in the ionized form, it's still many time more effective than the stomach |
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Term
| problems with rectal adminstration of drugs? |
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Definition
| 50% of drug will bypass liver, and absorption is irregular and incomplete, and it can irritate the rectal mucosa |
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Term
| why choose parental adminstration of a drug? |
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Definition
patient is combatitive, you absolutely need the drug delivered in active for and cannot have the body perform that task for you., you need to deliver a large volume
IV administration delivers 100% bioavailability, but can cause infections and pain. intramuscular and subQ can be delivered almost anywhere, but transfer of drug is limited to capillary permeability vs. the size of the drug |
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Term
| why do drugs take long to reach interstitial fluid in the brain? |
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Definition
allthought capillaries in most endothelial tissue are highly permeable, the blood brain barrier is formed by tight juctions between capillary cells thus restricting the passage of substances to the CNS.
sinusoidal capillaries of the liver and spleen have larger openings that allow passage of red blood cells adn seum proteins |
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Term
| what is the order of distribution of a drug starting from the blood? |
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Definition
it first quickly enteres vessel rich groups of organs (first phase), then muscles, skin, and fat (second phase).
a final redistribution of the drugs is possible following initial distribution, but this usually dignifies the begining of termination of effect (i.e., anesthesia, where maximum effect on brain has been reached, the effect was short lived, and not the drug is being redirected to start clearing it from the system) |
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Term
| drug binding to inert plasma proteins |
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Definition
only free unbound drugs and produce effects, but some being plasma proteins specifically, but reversibly. this takes these drugs out of bioavailability.
these extent of bound and unbound drugs is usually help pretty constant (known as steady state.) is bound plasma-protein drug complexes began being eliminated from the system, circulating plasma-protein drug complexes will start dissociating to maintain the steady state.
albumin mainly sequesters acidic drugs
a-1 acid glycoprotein mainly sequesters basic drugs |
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Term
| tissue reservoirs for drugs? |
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Definition
bones often can obsorb heavy metals and tetracycline and incorperate them into their crystal lattice.
fat hoards lipid soluble drugs |
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Term
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Definition
many enzymes exist that transform drugs into metabolites. these metabolites may be the active form of the drug, may make a hydrophobic molecule hydrophilic so that it can be excreted, and have been transformed into a percursor before becoming another metabolite
the liver is the primary organ for biotransformation bc:
-has large blood flow
-high conc of enzymes
-high conc of transporters including SLC type and ABC type and MRP2 type |
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Term
| some major phase 1 metabolizing enzymes? phase 2? |
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Definition
phase 1: CYPS, FMOs, EHs
phase 2: UGT (UDP-gluconyltransferase)
all are located in ER of the cell (often hepatocyte) and this is good because the ER is a distinct lipid-bilayer in the cell so when lipid soluble molecules enter the cytosol through the PM, they become embedded in the ER to be acted on by phase 1 enzymes. once a phase one enzyme acts, another molecule like a phase 2 (UGT) can modify the metabolite |
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Term
| what do you call the phase 1 modification of a molecule to an active metabolite? |
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Definition
| usually phase 1 metabolism of a molecule leads to inactivation of a molecule through hydrolysis of an ester or amide linkage. a molecule becomes a PRODRUG if the metabolism results in the bioactivation of the drug. |
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Term
| main purpose of CYP family? |
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Definition
| Phase 1 microsomal drug oxidations. can do this because they carry a heme group |
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Term
| main purpose of UGT family |
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Definition
a transferase (like all phase 2s) which adds a functional group to a metabolite (usually leading to hydrophilicity and are excrete in urine and feces)
urudine diphsophate-glucosyntransferases (UGT) is the most common of the phase 2 enzymes and has highest concentration in GI tract and liver
addes glucuronic acid leading to excretion. normal flora in ileum can cleave off this acid and cause the substrate metabolite to go back into circulation.
can lead to drug-drug interactions bc UGTs are inducible and can be inhibited |
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Term
| what do GSTs and SULTs do? |
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Definition
phase two enzymes
SULT makes a metabolite a reactive electrophile
GST addes a glutathione to reactive electrophiles therefore protecting it from reaction
Glutathione (usually stored as GSH) can cause oxidative damage to a cell if its conc falls too low. Falling levels of GSH has been associated with cancer, AIDS, spsis, trauma, and burns |
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Term
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Definition
a certain percentage of absorbed drugs taken orally will end up in the liver during the first pass, become metabolized, and not be biologically available. This will happen a few more times until all the agents have been eliminated.
IV drug administration ensures 100% bioavailability |
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Term
| explain one method of hastening the treatment of drug-poisoning. |
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Definition
acidify or make alkaline a patient's urine. The more drug you can ionize, the fast it will clear.
ie. alkalation with sodium bicarbonate to rid of weak acids
acidification with ammonium chloride to rid of weak bases |
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Term
| explain renal excretion of drugs |
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Definition
only drugs that are not bound to plasma proteins can be filtered with water by the glomerulus. High plasma protein binding means low filtration and excretion of the drug. as more unbound drugs are passively diffused into the proximal tubule for elimination, more bound drugs unbind to maintain the steady state.
nonionized drugs are capabably of being reabsorbed if reabsorption of Na ions is causing a gradient. The nonionized drugs will be carried back to circulation in the water. |
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Term
| how to genetics explain some people's intolerance to certain drugs? |
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Definition
their phenotype is such that they have pharmacogenetic differences in the expression of xenobiotic metabolizing enzymes. the difference has to appear in >1% of the population
often this is the case of SNPs |
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Term
| properties of a good drug? |
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Definition
| can reach target, exert effect, be metabolized and excreted |
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Term
| factors affecting drug's abilty to exert desired effect? |
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Definition
| structural features, solubilities, chirality, charge, size, try of bond it can form (weak? irreverslble?) |
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Term
| what affects extend of drug action? |
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Definition
-a drug interacting with receptors that serve functions common to most cells - widespread effects
-a drug working on receptors that are only unique to a few cell types
-a drug interacting with a receptor that serve a vital function may be difficult to dangerous to use |
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Term
| what can lead to supersensitivity of a receptor? |
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Definition
constant and chronic administration of a receptor antagoist
the denervation of a preganglionic fiber that indices postganglionic neuronal supersensitivity |
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Term
What is:
EC50
Emax
Kd
Bmax |
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Definition
EC50=conc at which 50% of the maximal response is seens
Emax=the dose at which no futher increase in response can be seen
Kd=conc of free drug at which 50% of all binding sites are filled
Bmax=the total conc of binding sites |
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Term
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Definition
| that ability of a drug bound to its receptor to activate downstream effector mechanism |
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Term
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Definition
| a quantitative measure of the effects of a drug at |
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Term
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Definition
| a measure of drug concentration needed to ellicit an effect. A more potent drug will require a lower conc of itself to elicit the same effect as another drug |
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Term
| a physiological antagonist |
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Definition
an agonist and an antagonist acting at two independent sites and inducing independent, but opposite, effects
i.e. insulin lowers blood glucose by stimulating cells to take up glucose, glucoagon increases blood glucose by promoting hepatic glycogenolysis and gluconeogenesis |
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Term
| define the therapeutic indexes |
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Definition
| the LD50/ED50. drugs are often defined by the width of their therpeutic window. in a narrow window, sligh changes in systemic conc can lead to signifcan changes in pharmacodynamic response |
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Term
| what is the formula for drug clearance? |
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Definition
CL= rate of elimination
drug conc in fluid measured |
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Term
| how do you calculate the volume distribution, Vd? |
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Definition
Vd= dose/Cp <--conc in plasma.
therefore, if the concentration in plasma is very low, we make an apparent assumption that most of the dose is taken up into the extravascular tissues
operates under an assumption of first order kinetics where any drug that has been eliminated from the plasma per unit time depended on the conc of drug remaining in the plasma |
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Term
| what is the half-life formula |
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Definition
| half life = (0.693 x Vd)/CL |
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Term
| what is the calculation of dosing rate? |
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Definition
rate of drug elimination must be equal to the rate of drug adminstration
dosing rate = CL x Css
by the 4-5th half life, steady state will be achieved |
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Term
| what first effects bioavailability? |
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Definition
bioavailability is abbreviated by F (the fraction reaching systemic circulation).
it is effected by inital dose and the amount of first pass hepatic metabolism
the efficiency of first pass hepatic clearance is determined by its intrinsic value, CL, and the flow rate of the blood to it, Q
if the extraction rate of the liver is .33, then the bioavailability is .67 right off the bat
increased blood flow will slow down the liver intrinsic metabolism |
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Term
| when wanting to continue a patient on a medicine, what must one do prior to discharge |
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Definition
calculate the absolute and variable bioactivites of the drugs they were taking.
the formula is set up like is
F = 100 x AUCa x doseb
AUCb x dose a
a and b can be brand vs. generic, or IV vs. oral
looking for bioequivalence |
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Term
explain saturable elimination
what does it assimilate graphically |
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Definition
it seems to follow michaelis-menten kinetics (ie. Km is equal to 50% of receptor binding, a definate Vmax exists)
it is risky to increase a dose in a saturation index is near. even increasing it a small bit could lead to a large jump in plasma conc. if dosing rate exceeds elimination capacity, toxicity can ensue
these are ZERO-ORDER kinetics and include ethanol, aspirin, and phenytoin |
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Term
| recommendations for dosage increase |
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Definition
stay low and go slow
increase no more than 50%, and don't do it until 4-5 halflives |
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Term
| what is a maintenance dose |
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Definition
an adjusted formula which allows for the state-state dose to factor in the rate of loss
dosing rate = CL x Css
F
(F doesn't matter for IV infusions) |
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Term
| considerations to make if drug absorption seems to be lower than expected |
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Definition
-patient's compliance might be low
-patient could have organ impairments
-plasma protein binding could be fluxuating
-if it (Cp) goes up, Vd does down and vice versa
-patient may be obese
-skeletal muscle mass differences |
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Term
| what is an idiosynchratic drug response? |
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Definition
unpredictable, manifested as ultra sensitivity to a low dose, or extreme insensitivity to high doses
can result from genetic polymorphisms |
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Term
| what are cumulative effects? |
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Definition
| results of chronic exposures to therpeutic conc of drugs as well as low conc or other natural and synthetic material in environment |
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Term
| some causes of hepatotoxicity |
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Definition
| alcoholism, acetaminophen tox, viral infections, steatosis (fatty liver) |
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Term
| some causes of nephrotoxicity |
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Definition
| NSAIDS (sometimes in combination with acetaminophen), ACE inhibitors, cyclosporine |
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Term
| what is an additive effect? |
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Definition
| the compounding of two drugs. each performs their single dose effect, but you will ultimately have two doses |
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Term
| what is a synergistic/potentiation effect? |
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Definition
| one drug magnifies the negative quality of another. the resultant effect exceeds any of the individual drug's possible effects |
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Term
| actions patients take that alter the absorption of drugs |
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Definition
alteration of gastic pH what they swallow their pill with. ginger ale is acidic, milk is basic, this could have good or bad consequences
sequestration of drug tetracycline binds to antacids, so if they're taken at the same time, you're going to get poor absorption
alteration of gastic motility slowing it down slows down reabsorption
inhibition or induction of Pgp transporters they are meant to keep out absorption |
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Term
Strong inducers of CYP3A4 and Pgp: |
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Definition
| Carbamazepine (antiepileptic drug) Phenobarbital (antiepileptic drug) Phenytoin (antiepileptic drug) Rifampin (antibiotic) St. John’s wort (herbal remedy) |
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Term
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Definition
potentially lead to carcinogenicity - cigarette smoke and other hydocarbons are inducers of this family
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Term
Moderate-to-strong CYP3A4 inhibitors |
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Definition
Cimetidine (reduces stomach acidity) Erythromycin and Clarithromycin (macrolide antibiotics) Ketoconazole and Itraconazole (antifungals) Ritonavir (protease inhibitor; one of the most potent CYP3A4 inhibitors) Atazanavir (protease inhibitor); also inhibits UGT1A1 Grapefruit juice |
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Term
| urinary acidifiers will have what effect on the clearance of drugs? |
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Definition
| they will decrease the clearence of acid drugs and increase the clearance of basic drugs (this is because of ion trapping) |
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