Pharm Principles (325E1)

Question 1

3 phases of drug action

Answer 1

every drug every time
1: pharmaceutic (only for oral)
2: pharmacokinetic (iv drugs enter here)
3: pharmacodynamic

Question 2

Phases of drug action: pharmaceutic (1)

Answer 2

drug dissolves to be used and absorbed in blood and body (dissolution) all oral drugs and only occurs w/ oral drugs

Question 3

Phases of drug action: pharmacokinetic (2)

Answer 3

drug moving through the body and what the body does to the body (4 processes: absorption, distribution, metabolism, excretion)

Question 4

Phases of drug action: pharmacodynamic

Answer 4

what the drug does to the body (MOA, intended effect, therapeutic action)

Question 5

pharmacokinetic (2): absorption

Answer 5

the drug goes into the small intestines and then into the blood

Question 6

pharmacokinetic (2): distribution

Answer 6

drug has already been absorbed into the blood and now it leaves the blood stream and goes to the site of action and exerts it effort

Question 7

pharmacokinetic (2): metabolism / biotransformation

Answer 7

after the drug has been excreted, it is broken down by liver to go from lipid soluble to water soluble so it can be removed from the body method by which drugs are inactivated

Question 8

pharmacokinetic (2): excretion

Answer 8

kidneys excrete water soluble form of drug (some drugs can be excretede from liver)

Question 9

drugs must have what type of solubility to pass through the cellular membrane

Answer 9

lipid soluble (water soluble need a transport mechanism to cross)

Question 10

if we give an drug PO/orally, what does it have to go through

Answer 10

first pass effect

Question 11

what drugs are 100% bioavailable

Answer 11

IV drugs (PO drugs have a varying of

Question 12

PO meds bio availability

Answer 12

the amount of drug left after the first pass effect (ex: if first pass is 20%, then the drugs bio avail is 80%)

Question 13

when would you expect to see a high first pass %

Answer 13

if a drug is taken in a high amount (dose) or is taken often

Question 14

high first pass % would give what type of bio availability %

Answer 14

low

Question 15

the first pass effect alters

Answer 15

the amount of a drug that is absorbed

Question 16

first pass effect

Answer 16

PO meds that are absorbed in the SI have to go through the liver to be turned into its active form before they can enter circulation and this determines their bio availability

Question 17

routes of absorption (ROA)

Answer 17

enteral
parenteral
topical

Question 18

enteric coated (EC) meds

Answer 18

intended to break down in the small intestine and not the stomach (still goes through first pass)

Question 19

ROA: enteral

Answer 19

by way of the GI tract (oral/gastric mucosa, SI, rectum aka po meds & rectal)

Question 20

PO meds break down starts in the “” and are absorbed in the “” and it does or does not go through first pass?

Answer 20

stomach ; small intestine ; does

Question 21

what routes of enteral meds do not go through first pass and why

Answer 21

SL, buccal and rectal bc all sites contain highly vascularized tissue

Question 22

why can you not make a PO drug rectal

Answer 22

no first pass effect due to the bio availability so it by passes the liver

Question 23

ROA: parenteral

Answer 23

SQ, IM, IV, intrathecal (into spinal canal), epidural (space around the spinal cord)

Question 24

do parenteral drugs go through first pass effect

Answer 24

no

Question 25

what route of parental drug is fastest

Answer 25

IV bc there are no barriers to absorption (they are often irreversible)

Question 26

ROA: topical (transdermal)

Answer 26

application of meds to body surfaces, has a slower onset & more prolonged interaction

Question 27

do topical drugs go through first pass effect

Answer 27

"not concerned with first pass effect because it will act very localized"

Question 28

where does the best drug distribution occur

Answer 28

in areas that are highly vascularized w/ good blood flow (decreased blood flow = decreased distribution)

Question 29

condition that decrease blood flow

Answer 29

peripheral vascular disease, abscesses, tumors

Question 30

blood brain barrior

Answer 30

cells in the capillary wall in the brain with very tight junctions that prevent drug passages (prevents drugs from going to the brain as a preventive mechanism)

Question 31

what drugs can't pass the blood brain barrier

Answer 31

only drugs that have transport systems or are "extremely" lipid soluble

Question 32

what drugs can pass the blood brain barrier

Answer 32

alcohol, glucose (the brains source of energy)

Question 33

what is a main consideration when giving drugs to infants

Answer 33

the blood brain barrier is not fully developed so more drugs can pass through

Question 34

protein binding effect

Answer 34

temporary storage of drug molecule that allows drug to be available for a longer period of time, drugs bind to albumin but can rapidly be unbound

Question 35

what type of drug, bounded or unbounded, is considered active and free exert effects

Answer 35

unbound (free)

Question 36

what is the goal of protein binding

Answer 36

maintain a steady free drug concentration "steady state"

Question 37

what affects protein binding

Answer 37

the amount of protein in the blood

Question 38

what is the primary plasma protein

Answer 38

albumin (it circulates constantly)

Question 39

hypo albuminemia

Answer 39

**malnutrition or liver disease** more free drug is available for distribution to tissue site leading to possibility of overdose and drug toxicity

Question 40

example of protein binding: warfarin/coumadin

Answer 40

this is a blood thinner that is 97-99% protein bound so if a pt has low albumin a person is at greater risk for bleeding due to higher effect of drug exerted

Question 41

besides low albumin, what else is a risk factor for toxicity of protein bound drugs

Answer 41

if a person is taking multiple protein bound drugs at the same time bc all the drugs are fighting for the albumin in the body

Question 42

a drug goes through metabolism (biotransformed) and is inactivated, what is it now called

Answer 42

metabolite

Question 43

what is the major site for drug metabolism

Answer 43

the liver by cytochrome P-450 enzymes

Question 44

what organ(s) failure can lead to drug toxicity

Answer 44

the liver bc they don't get metabolised, the kidneys bc the drug doesn't get excreted

Question 45

how many drugs use the CYP450 system

Answer 45

about 1/2 of all drugs ; since so many use it, it creates drug - drug interactions

Question 46

clinical significance of CYP450 inhibitor

Answer 46

can be a substrate, inducer or inhibitor

Question 47

if a drug uses CYP450 system as a substrates

Answer 47

the drug uses the system for metabolism (it initiates the drug)

Question 48

if a drug uses CYP450 system as an inducer

Answer 48

the system increases the breakdown and elimination of the drug to lower the drugs therapeutic effect

Question 49

if a drug uses CYP450 system as an inhibitor

Answer 49

the system decreases the breakdown and elimination of the drug to increase the amount of drug in the body and increase the therapeutic effect **risk for toxicity**

Question 50

example of CYP450 inhibitor

Answer 50

grapefruit -> drinking or eating grapefruit with a CYP450 drug increases the amount of the drug in the body leading to toxicity

Question 51

teaching point for grapefruit consumption and medications

Answer 51

don't take medications w/ grapefruit juice and avoid eating grapefruit or drinking it for 2-4 hours after taking me

Question 52

what is the major site of excretion

Answer 52

the kidney through gglomerular filtration, tubular secretion, and tubular reabsorption **all need to be working for the drug to be excreted**

Question 53

reabsorption from the kidneys

Answer 53

some drugs are reabsorbed through the kidney tubules, if low amounts of a drug is reabsorbed, need high dose to maintain levels

Question 54

what are the renal labs

Answer 54

BUN, creatinine, GFR (main one)

Question 55

what does half life determine

Answer 55

dosing of a drug and how often it should be given

Question 56

what process from phase 2 does half life effect

Answer 56

elimination (it takes 5 half lives for 97% of a drug to be eliminated)

Question 57

serum half life (T 1/2)

Answer 57

the time required for the serum concentration of a drug to decrease by 50%

Question 58

example for T 1/2: if half life is 1 week, how long will it take for the drug to be gone from the body

Answer 58

5 weeks

Question 59

how many half livees for a "steady state" to occur

Answer 59

4-5

Question 60

goal of steady state

Answer 60

when intake of a drug is equal to the amount of drug metabolized and excreted (the state when the BP meds will have BP always under control)

Question 61

around the clock dosing (ATC)

Answer 61

goal is to maintain 50% concentration in the body (how we treat pain and dose antibiotics)

Question 62

drug onset

Answer 62

time it takes for drug to elicit therapeutic response (latent period)

Question 63

drug peak

Answer 63

time it takes for drug to reach its maximum therapeutic effect (when 10mg of morphine feels like 10mg of morphine)

Question 64

drug duration

Answer 64

time drug concentration is sufficient to elicit a therapeutic response (consistent 5mg)

Question 65

how do drug create a response in phase 3

Answer 65

increase, decrease, replace, inhibit, destroy, protect, or irritate

Question 66

what are non desired effects of a drug

Answer 66

side effects (ex: metaproterenol is a broncho dilator so it dilates the bronchial passage but it also increases HR & palpitations beyond normal range)

Question 67

receptors

Answer 67

proteins located on cell surface that are chemicals (hormones or neurotransmitters) in the body that interact with drugs to produce effects (creates drug receptor complex)

Question 68

what does the drug receptor complex initiate

Answer 68

a physiochemical reaction by means of agonist (stimulates) or antagonist (inhibits)

Question 69

agonist

Answer 69

a drug that has the ability to initiate a desired therapeutic effect by binding to a receptor

Question 70

antagonsit

Answer 70

a drug that produces it action not be stimulating receptors but by preventing or blocking or inhibiting other natural substances (ligands) from binding and causing a response

Question 71

do all drugs responses involve receptors

Answer 71

no, some drugs act through simple physical or chemical interactions with small molecules (ex: antacids work by neutralizing gastric acidity through direct chemical interaction)

Question 72

therapeutic index

Answer 72

the measure of relative safety of a drug

Question 73

narrow therapeutic index (NTI)

Answer 73

a ratio of lowest concentration at which clinical toxicity commonly occurs (if safe range is 10, toxic at 10.1)

Question 74

black box warning

Answer 74

required by FDA for drugs that are especially dangerous (the strongest safety warning a drug can carry and still remain on the market)

Question 75

examples of NTI drugs

Answer 75

theophyllin, digoxin, phenobarital, lithium, coumadin

Question 76

where must the black box warning appear prominently

Answer 76

on the package insert, product label and any magazine or advertising

Question 77

med errors are a major cause of what

Answer 77

morbidity and mortality

Question 78

high alert medications

Answer 78

most likely to cause serious harm and death

Question 79

examples of high alert meds

Answer 79

insulin, heparin, opioids, IV KCL, neuromuscular blocking agents, chemo drugs

Question 80

what are the types of drug interactions

Answer 80

drug - drug (most concerning w/ NTI) drug - food drug - herb drug - disease

Question 81

how to minimize drug interactions

Answer 81

lower # of drugs a person is on, reconcile meds, monitor

Question 82

drug interactions that increase therapeutic effect: additive effects

Answer 82

2 drugs taken w/ similar MOA (they become stronger together)

Question 83

drug interactions that increase therapeutic effect: synergism/potentiation

Answer 83

2 drugs w/ different MOA but result in a combined drug effect greater than that of either drug alone (still will become stronger together)

Question 84

drug interactions that increase therapeutic effect: activation

Answer 84

activation of drug - metabolizing enzymes in the liver which decreases metabolism rate of the drug

Question 85

drug interactions that increase therapeutic effect: displacement

Answer 85

displacement of one drug from plasma protein binding sties by a second drug which increases effect of displaced drug

Question 86

drug interactions that decrease therapeutic effect: antidote

Answer 86

drug given to a antagonize (stop) the toxic effects of another drug

Question 87

drug interactions that decrease therapeutic effect: decrease intestinal absorption

Answer 87

applied for PO meds bc some people cannot break down for effect

Question 88

drug interactions that decrease therapeutic effect: activation

Answer 88

activation of drug metabolizing enzymes in the liver -> enzymes inducers (get the drug out quicker)

Question 89

pharmacokinetic consequences in older adults

Answer 89

-decreased production of CYP 450 enzymes -increase risk for drug interactions

Question 90

changes in older adults

Answer 90

-hepatic: drugs metabolize slower -cardiac/circ: impaired, slows distri. -GI: decreases absorption of PO meds -Renal: drugs excreted less completely