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NURS 5334 - Final Exam Study Guide-latest-2024/2025 Latest Updated Version || Rated A+

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NURS 5334 - Final Exam Study Guide-latest-2024/2025 Latest Updated Version || Rated A+

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NURS 5334
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NURS 5334

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@PROFDOCDIGITALLIBRARIES


NURS 5334 - Final Exam Study Guide-latest-2024/2025
Latest Updated Version || Rated A+

Final Exam Blueprint


Prescribing Basics: 2 questions

Prescriptive authority regulated by the state BON in each state.

Tall man lettering to highlight dissimilaries with look-alike names

*Prescription contains… Physicians Name, Address, and telephone number are required to be included in
PR
the prescription. DEA number (two letters, five numbers) if the prescription is for controlled substance,
Patient name and DOB (also may include address and weight), Date Rx is written (expires 1 year after
date issued), Name of drug and strength- avoid trailing zeroes, use leading zeroes, Directions with
indications/route of administration and frequency, write out number of refills, quantity of drug,
signature, NPI number (9 or 11 numbers), sign as A-PNP or role recognized by the BON
O
Drug schedules – one is most addictive, up to schedule 5.

1) heroin, LSD, marijuana.
FD
2) oxycodone, hydrocodone, methamphetamines.

3) codeine, ketamine, testosterone.

4) Xanax, valium, ambien, tramadol.
O
5) antidiarrheal, antitussives, Lomotil, lyrica.

*calculation question
C

Pharmacology Principles: 3 questions

Pharmacodynamics – effect of drugs on body. Works by receptors. Usually proteins that interact with
drugs.

Agonist – produce receptor stimulation, conformational change every time they bind.

Partial agonist – properties between agonists and antagonists. Submaximal effect. Stimulate only some
of the receptors.

Antagonist – affinity for receptor but NO intrinsic activity. Affinity allows antagonist to bind to receptors,
but lack of intrinsic activity prevents receptor activation. Blocks action of drugs (example Narcan).

Therapeutic range – between minimum effective concentration and toxic concentration. Working
effectivity with no toxicity or adverse effects. Wider therapeutic range is better! Easiest to control.
1

,@PROFDOCDIGITALLIBRARIES


Bioavailability – percentage of dose of drug that survives first pass through liver and reaches blood




PR
O
FD
O
C



2

,@PROFDOCDIGITALLIBRARIES




stream.

Half life – time required for amount of drug to decline by 50%. Shorter half life admin more frequently.
4.5-5 half lives to get to steady state and to eliminate from body.

PR
O
FD
O
C



3

, @PROFDOCDIGITALLIBRARIES




Pharmacokinetics – what body does to drug. Absorption, distribution, metabolism, elimination. (ADME)

Parenteral (bypass first pass), then oral, then lungs, then skin, eye and ears for best absorption.

Distribution affected by lipid/water solubility, PH, protein binding, size of molecule.
Protein binding – unbound drug is free drug which is active. When 2 highly bound drugs are given it
increases the level of one of the drugs, leading to toxicity. IE warfarin and phenytoin are both highly
protein bound. Low plasma protein result in more free drug. May be in elderly, so decrease dose of
medication. T3 and T4 both highly protein bound. 1% of drug is powerful.

Distribution – BBB (only lipid soluble will pass) – these such as narcotics, only work because they do
cross BBB. Some meds we do not want to pass. Placental barrier (many drugs can pass) so be careful
with drugs in pregnancy.

Metabolism – liver. Chemical change of a drug structure to enhance excretion, inactivate drug, increase
therapeutic action, activate prodrug, increase or decrease toxicity.
PR

Substrate – agent that is metabolized by an enzyme into a metabolite and product and eventually
excreted.

*Inhibitors – compete with other drugs for a particular enzyme affecting the metabolism (decreases) of
the substrate and decreases the excretion of the substrate and increasing the circulating drug. Need to
O
decrease dose of substrate if start on an inhibitor. INH increases substrate.

*Inducer – competes with other drugs for a particular enzyme affecting metabolism of the substrate
FD
(increases) decreasing the efficacy of the drug. Need to increase dose of substrate if start on an inducer.
IND decreases substrate.

Renal excretion – passive glomerular filtration, active tubular secretion, tubular reabsorption.

Pharmacogenomics: 1 question
O
Pharmacogenomics- the study of the influence of hereditary factors on the response of individual
organism to drugs, and the study of variations of DNA and RNA characteristics as related to drug
response.
C
Pharmacogenetic tests mentioned on drug labels can be classified as “test required”, “test
recommended”, and “information only”. Currently there are 4 drugs requiring to have pharmacogenetic
testing performed before they are prescribed: Cetuximab, Trastuzumab, Maraviroc, and Dasatinib.

No genetic testing is required by the FDA for the initiation of medications such as warfarin,
carbamazepine, valproic avid and abacavir are currently in place, such tests are recommended prior to
initial dosing.

BBW initiated in December 2007- on carbamazepine label – testing recommended for HLA-B 1502 in
patient with Asian ancestry due to high risk of developing SJS or toxic epidermal necrolysis (TEN).



Drugs across the lifespan: 3 questions


4

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