Pharmacokinetics (Wolff)

Question 1

What are the four basic pharmacokinetic processes?

(Mnemonic)

Answer 1

ADME

A-absorption (GI and blood)

D-Distribution (Blood)

M-Metabolism (liver, kidney, action sites, other)

E-Excretion (bile and urine out of body)

Question 2

What factors affect Absorption

Answer 2

rate of dissolution

surface area

blood flow

lipid solubility

pH partitioning

Question 3

Pros and Cons of oral administration

Answer 3

Pros: convenient, slow uniform absorption, safe, economical

Cons: destruction by low pH, poor absorption of large and charged particles, bind with GI contents, irritate intestines

Question 4

Pros and Cons of Rectal administration

Answer 4

Pros: limited first pass metabolism, useful if oral route precluded

Cons: irregular absorption, irritation of rectal mucosa

Question 5

Pros and Cons of sublingual/buccal administration

Answer 5

Pros: rapid absorption, avoids first pass metabolism

Cons: only small amounts absorbed at a time

Question 6

Pros and Cons of IV administration

Answer 6

Pros: Most direct, bypasses barriers to absorption, suitable for large volumes, easy to adjust dosage

Cons: painful, immediate adverse effects, not suitable for oily substances/suspensions

Question 7

Pros and Cons of IM administration

Answer 7

Pros: quick and easy, possible rapid absorption, may use as depot, good for oily substances/suspensions

Cons: painful, bleeding, nerve injury

Question 8

Pros and Cons of Sub.Q. administration

Answer 8

Pros: Quick and easy, rapid aborption, good for suspensions and pellets

Cons: painful, cannot give large amounts

Question 9

Pros and cons of inhalation administration

Answer 9

Pros: vollatile/aerosolized, rapid absorption, selivery to lungs may minimize systemic effects

Cons: variable systemic distribution

Question 10

Pros and Cons of topical administration

Answer 10

Pros: application to specific surface for local effect

Cons: irritation

Question 11

Pros and Cons of transdermal administration

Answer 11

Pros: controlled permeation through skin

Cons: irritation

Question 12

Three ways for drugs to cross cell membranes

Answer 12

1. facillitated diffusion (rare)
2. Active transport (p-glycoprotein, gets drugs out of cells)
3. direct penetration through simple diffusion (most common)

Question 13

Which will cross the cell membrane better, polar or nonpolar drugs?

Answer 13

Nonpolar drugs readily dissolve in nonpolar substances and easily cross the cell membrane

Question 14

What is an example of a polar drug?

Answer 14

Quaternary ammonium compounds have fixed charges and cannot readily cross the cell membrane

Question 15

When are weak acids and weak bases able to cross cell membranes ?

Answer 15

only when in their unionized forms

Question 16

Define the following:

Ka

S

F

Amount Absorbed

Answer 16

Ka=rate constant for absorption

S=salt factor

F=bioavailability, AUC route used/AUCiv

Amount absorbed=SxFxDose

Question 17

If F=AUCroute used/AUCiv, what is AUC?

Answer 17

AUC is the area under the curve

where F equals the fraction of oral dose that enters the plasma

Question 18

Equation for concentration in plasma (Cp)

Equation for Volume of Distribution (Vd)

Answer 18

Cp=SxFxDose/Vd

Vd=amount of drug in body/plasma concentration

Question 19

What factors affect drug distribution?

Answer 19

ability of drugs to enter cells

blood flow to tissues

ability of drugs to exit the vascular suystem

Question 20

Explain the significance of protein binding of drugs

Answer 20

Drugs are only bioactive if they are free (a=fraction unbound)

there is a finite number of protein binding sites in teh plasma, thus new addition of drugs can displace the bound drug

this can be a concern if the drug has a small therapeutic window, example: if drug is normally 90% bound and added drug displaces it so that now 80% is bound, the (a) doubled, from 10% to 20%

Question 21

The BBB is a barrier to which category of drugs?

Answer 21

ionized or polar drugs unless they have a transporter

Question 22

What is the primary site of biotransformation (metabolism)?

Answer 22

the liver which may activate pro-drugs but primarily INACTIVATES drugs

this is crucial for the renal elimination of lipophilic drugs which must be made more polar so they can be trapped in the renal tubular fluid

Question 23

What are the two phases of metabolism?

Answer 23

Phase I: oxidation, reduction, hydrolysis

Phase II: conjugation

Question 24

What occurs in Phase I of metabolism?

Answer 24

Products are made more polar by introducing or unmasking functional groups

oxidative proceses involve enzymes from SER and cytochrome p450

Question 25

What is the function of CYP inducers

Answer 25

increase the enzyme levels, speed up metabolism of other drugs metabolized by same enzyme, lower plasma levels below MEC

examples: phenobarbitol, carbamazepine, ethanol, cig. smoke

Question 26

Whatis the function of CYP inhibitors?

Answer 26

Inhibit enzymes

slows the metabolism of any other drug metabolzied but the same enzyme and can lead to toxic levels

examples: erthromycin, ketconazole, metronidazole, grapefruit juice

Question 27

How does grapefruit juice inhibit the cytochrome p450?

Answer 27

Inhibits CYP3A4 enzyme in the intestinal epithelial cells thus increasing the bioavailability of other drugs metabolized by the same enzyme

Question 28

What is the purpose of Phase II in metabolism?

Answer 28

Conjugation occurs to make the drug more water soluble and more excreable since the molecule is highly polar via glucoronidation or sulfation

Acetylation and methylation can also occur to make drugs less water soluble and to inactivate drug

Question 29

What is the difference between glucuronidation and sulfation in the Phase II reaction of metabolsim?

Answer 29

glucuronidation is the major route of metabolism for drugs and endogenous compounds and occurs in the ER, can be induced

Sulfation occurs in the cytoplasm

Question 30

What happens with oral administered drugs that effect their bioavailbility?

Answer 30

They undergo first pass metabolism which can greatly decrease the bioavailability of orally administered drugs

Question 31

How are drugs eliminated?

Answer 31

renal (major)

bile, sweat, breath and breast milk (minor)

Question 32

Describe the steps in renal drug excretion

Answer 32

1. Glomerular filtration of small drugs filter out, protein bound drugs do not filter out
2. Passive tubular reabsorption occurs of lipid soluble drugs and unionized weak acids/bases
3. Active tubular secretion leads to elimination of protein bound drugs when they temporarily dosplace from protein near basolateral membranes of PCT

Question 33

What are some factors that modify renal drug excretion?

Answer 33

pH dependent ionization

competiton for active tubular transport

age-GFR decreases with increasing age

Question 34

What is the excretion rate?

Answer 34

mass eliminated per unit time; with first order kinetics, this increases as the plasma concentration increases

Question 35

What is clearance?

what is total clearance?

Answer 35

the plasma volume from which all of the solute is removed per unit time (flow rate)

with first order kinetics, this remains constant as plasma concentrations change

Total clearance=renal clearance+hepatic clearance+other clearance

Question 36

What is the Cockcroft-Gault eGFR equation

Answer 36

quick estmiate of creatinine clearance (eGFR) from a serum measurement of creatinine concentration

eGFR=[(140-age)xBW(kgs)/72xScr]

if female, multiply by 0.85

Question 37

Why are adverse drug reactions 7x more likely in elderly patients?

Answer 37

drug accumulation due to declining renal function

greater severity of illness

use of drugs with a low therapeutic index

poor pt compliance

polypharmacy

presence of multiple pathologies

inadequate supervision

Question 38

What are some of the consequences of drug-drug interactions?

Answer 38

synergy/potentiation leading to increased therapeutic and increased adverse effects

antagonism leading to therapeutic effects decreasing and decrease in adverse effects

creates a unique drug response (may be unpredictable)

Question 39

Common adverse drug effects

Answer 39

constipation

skin rash

diarrhea

dizziness

drowsiness

dry mouth

headache

insomnia

Question 40

What are some of the various mechanisms of drug-drug interactions?

Answer 40

directly chemical/physical

pharmacokinetic (altered ADME, issues with p-glycoprotein like MDR1)

Pharmacodynamic interactions (same receptor, different sites)

combined toxicity

Question 41

Drug allergies and hypersensitivies require what event to occur?

What are common drug allergies?

Answer 41

Require prior sensitization and are not dose-dependent

penicillins have the most serious reactions, other common allergies are NSAIDs and sulfonamides

Question 42

What drug will cause apnea of long duration if you lack plasma esterase?

Answer 42

Succinylcholine

Question 43

What drug will cause hereditary methemoglibinemia if you lack NADH methemoglobin reductase?

Answer 43

Nitrites, sulfonamides, preimaquine, etc

Question 44

What drug will cause increased toxicity if you have low liver actyl transferase?

Answer 44

Isoniazid and others

Question 45

What drug will cause drug induced anemia (favism) if you lack G6P dehydrogenase?

Answer 45

Primaquine and others

Question 46

what drug will cause acute intermittent porphyria if you lack porphobilinogen deaminase?

Answer 46

barbituates, estrogens, sulfonamides, chlorquine

Question 47

What is an example of food affecting drug absorption?

Answer 47

Ca in diet can lead to precipitation of tetracyclines in the GI tract

Question 48

What is an example of food/herbs affecting drug metabolism?

Answer 48

grapefruit juice is a CYP inhibitor and St. John’s Wort is a CYP inducer

Question 49

What is an example of food affecting drug toxicity?

Answer 49

tyramine in wine, cheese and sausages cannot be metabolizd in the presence of MAO inhibitors leading to hyperadrenergic crisis

Question 50

What is an example of food affecting drug action?

Answer 50

Na in diet can impact the actions of Li in bipolar disorder

Question 51

How can food interfere with timing of drug administration?

Answer 51

food can mitigate GI upste but interfere with absorption of drugs in stomach

Question 52

What are some issues with drug-herb interactions

Answer 52

Don’t always know the MOA of interaction so it is difficult to predict how they will influence drug; may cause diuresis, but still unpredictable

Question 53

What are some heaptotoxic drugs?

Answer 53

lipid-lowering drugs

antiseizures drugs

tuberculosis drugs

antiretroviral drugs

oral hypoglycemics

antifungals

immunosuppresants

acetaminphen

Question 54

What drugs can cause QT prolongation?

Answer 54

Tergenadine with erythromycin or ketoconazole

QT prolongation can lead to Torsades and vfib

Question 55

Drugs are responsible for how many major fetal structural abnormalities?

Answer 55

<1%

must see characteristic malformations during a specific window of vulnerability with a dose dependent response

Question 56

What are some examples of drug induced carcinogenesis

Answer 56

hard to evaluate, can take years for cancer to crop up.

cancer chemotherapy drugs assx with greatest carcinogenic potential (Tamoxifen for breast cancer, can cause uterine cancer)

DES was used to prevent SAb in high risk women but female fetuses exposed had increased incidence of vaginal and uterine cancers

Question 57

ADME in neonates and infants (increased total body water)

Answer 57

Absorption: increased or decreased in GI decreased from IM injection

Distribution: low albumin-high levels of free drugs, BBB not developed, so drugs can enter brain

Metabolism: decresed, so must adjust dose downward

Excretion: decreased, so must adjust dose downward for drugs

Question 58

ADME for geratrics (decrease in water, decrease in lean body mass, increase in body fat)

Answer 58

A: no changes, tends to decrease from GI

D: influenced by body comp., albumin levels also fall

M: tends to decrease but varies

E: decreases progressively from early adulthood

Question 59

ADME for children over age one

Answer 59

ADE: similar to adults

M: much faster than adults, peaks at age 2

Question 60

What is the placebo effect?

Answer 60

measurable, observable, or felt improvement that is not attributable to treatment

1/3 of all pt will respond to placebo and response may exceed that of some drugs

for pain, =75% of patients will respond to placebo

Question 61

Physiological changes in pregnancy that affect drug therapy

Answer 61

decreased bowel tone and motility increases time for drug absorption

increased hepatic metabolism

RGF doubles thus increases GFR

(does all of this balance out such that pregnant people do not need changed doses?)

Question 62

What type of drugs cross the placenta?

Answer 62

All drugs can cross the placenta, with lipid soluble drugs cross most readily

Question 63

What are adverse drug reactions during pregnancy?

Answer 63

teratogenesis

dependence-producing drugs

drugs that change uterine tone

Question 64

How to handle breastfeeding and drug adminstration

Answer 64

dose immediately after breastfeeding and avoid drugs with a long halflife

Question 65

What are zero order kinetics

Answer 65

• constant amount eliminated per unit
• the drug elimination process is saturated
• consequently, the amount of drug eliminated is independent of the drug concentration
• can be written as dCp/dt=k, where it is the rate of change in plasma concentration; k is a constant in units of amount per time
• example: ethanol-rate of metabolism is rapidly saturated so it is effectively zero

Question 66

What are first order kinetics?

Answer 66

• constant fraction is eliminated per unit time
• drug elimination process is not saturated
• the mass of drug eliminated is directly related to the drug concentration
• can be written dCp/dt=kCp where it is the rate of change in plama concentration, k= fractional rate constant in unites of time, Cp equals the plasma concentration of the drug
• This is the more typical form of drug elimination

Question 67

With first order kinetics, each half life backwards does what to the concentration?

Answer 67

doubles it

Question 68

Know these equations

Answer 68

kel=Cl/Vd

Cl=kelxVd

kel=first order eliminatino rate constant

Cl=clearance

Vd=is the apparent volume of distribution

Question 69

Calculating clearance

Answer 69

Cl=SxFxDose/t/Cp

Cl=clearance

S= salt factor

F=bioavailability

t=dosing interval in hours

Cp=plasma concentration

Question 70

Capicty-Limited reactions

Answer 70

• display zero order kinetics initially
• displays first order kinetics as the drug concentration falls
• would be seen with most drugs at high enough concentrations
• plasma concentration vs. time has a hockey stick appearance

Question 71

Capacity Limited Elimination equation

Answer 71

rate of elimination=Vmax x C/Km + C

Vmax=max eliminatino capacity

C=plasma concentration

Km=drug concentration at which rate of elimination is 50% of Vmax

Question 72

How to calculate Cpss

Answer 72

Cpss=dosing rate/Cl

=SxFxD/t X 1/kelxVd

Question 73

What is a loading dose?

Answer 73

dose needed to rapidly achieve therapeutic drug concentrations for drugs with a very long half life (digoxin)

leading dose=Cpss x Vd/(SxF)