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Pharmacology Exam #1 Study Guide

Intro To Pharm/Med Errors/Drug Atlas

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1) Rights of medication administration

  1. Right drug - must check the name of the drug 3 times - at the medical administration record, while drawing up the medication, and again at bedside before giving it to the patient. Don’t forget to ask the patient if they have any allergies or have had a prior allergic reaction to that medication in the past.

  2. Right dose - become familiar with the dosing, or cross reference with a book or the EHR

  3. Right time - some drugs need to reach a therapeutic level to be able to work well on the receptor. Just because it is scheduled for 2 pm does not mean that it needs to be given at that time - if the toxicity level is too high, then it should not be given as it can harm the patient. Toxicity can be checked with labs for example. 

  4. Right route - know that it is the right route for the patient. 

    1. For example - if a patient has been ordered a PO medication but they have AMS/fatigue/dysphagia/etc then the route might need to be changed. ((i think call pharmacy to see if there is another route that the drug can be given and then if there is - call provider and ask to change the order)) 

  5. Right patient - use 2 identifiers such as name and DOB, double check their ID band. Make sure to check the med order against their ID band by scanning it and making sure that they match. 

  6. Right documentation - We document the date, time, route, dose, site of administration. 

  7. Right reason or indication - We need ro know why the meds are being given.

    1. For example - if a patient has a headache and the provider orders Tylenol, but then they develop a fever - the Tylenol can only be given for the headache and the provider must be notified about the fever as they will need to determine what the underlying cause of it is. 

  8. Right response - ensure the patient is responding well to the medication - in terms of the therapeutic effects (is the patient’s problem improving with the medication), in terms of the side effects and adverse effects (are they experiencing any and how severe are they?) 

  9. Right to refuse - need to inform the patient that they are allowed to refuse the medication at any time-  but we need to ensure that they are sound of mind - meaning they are able to make the right decisions 

**there are 9 rights, other ones have been proposed but for the sake of the class and exam, we only need to know those.

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2) Pharmaceutics: understand how different forms of the medication affect its dissolution and absorption into the body


ENTERAL - mouth and GI

  • Drugs given orally, sublingual (however, this one goes directly into the  bloodstream since there are many blood vessels under the tongue and thus bypasses the ‘first pass effect’ - but because it is considered PO it is considered enteral), buccal, rectal and vaginal (but can also be considered topical). 

  • This will first undergo ‘first pass effect’ - meaning it will go though the liver to be metabolized (AKA break down the drug into its active components) so the drug can have its active effect on the target tissue. 

    • Another way to define it is the processing of that drug by the liver. 

  • Bioavailability is the amount of the drug that is available when it reaches the target tissue/organ after the first pass effect of an ENTERAL drug. 

    • Not all drugs have high bioavailability -for example Bactrim has 100% bioavailability, vancomycin has 0% bioavailability. 

  • This means that Bactim, when taking ENTERAL it will have 100% of the drug reaching the target tissue/organ after it has been metabolized by the liver. 

  • Vancomycin, when taking ENTERAL will have 0% reaching the drug after it has been processed by the liver. 


PARENTERAL - into the bloodstream 

  • Drugs given IV, IM, SUBQ, ID, intraarterial, intrathecal, intraarticular (directly into the joints)

  • These do not need to go through the liver (AKA no need for first pass effect) as it goes directly into the bloodstream

  • PARENTERAL drugs will always have 100% bioavailability since they are administered directly into the bloodstream 


TOPICAL - through the skin

  • Drugs to the skin including transdermal patches (PARENTERAL), ointments (messier but more effective), gels, creams (less effective because they are water based, but often preferred by patients), 


DISTRIBUTION - protein bound drugs 

  • Some medications are protein bound when they get into the bloodstream - meaning they use the proteins in your plasma to travel through the bloodstream and reach the target tissue/organs.

  • Albumin is the most abundant protein in plasma, it helps hold water within the blood vessels (if low, then water leaks and this leads to edema). 

  • When protein-bound drugs enter the bloodstream, they will mainly bind to albumin (as it is the most abundant) and be carried to the target tissue/organ. The remaining drug will stay in the bloodstream ready to be metabolized. 

  • Eventually as the free flowing drug in the body decreases (bc it has been metabolized) then some of the bound drug (to albumin) will unbind and get released into the bloodstream to continue being metabolized.

  • If a patient has low albumin levels, they will have extra medication in the bloodstream - meaning more effect which can lead to higher drug toxicity. 

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3) Remember which medications should not be crushed


Extended release - d/t being a higher dose and it dissolves slowly - this is used to reduce amount of time per day that medication is taken. 

Coated - meds can be coated for a purpose such as taste masking, protecting med from moisture, or facilitating swallowing. Enteric coated - the coating is designed to resist the acidic environment of the stomach and dissolve in the alkaline environment of the intestines - ensuring the medication is released at a specific location in the GI tract - this coating is used for meds that may cause irritation to the stomach lining or that need to be absorbed by the intestine for optimal effectiveness. Coated or enteric coated medication should not be crushed as they are designed to release the active ingredient in a controlled manner and crushing them will affect their safety and efficacy which can lead to pt having adverse effects or treatment failure. 

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4) In pharmacokinetics review the following concepts: absorption, distribution, metabolism, and excretion. Remember main organs in charged of metabolism and excretion as well, plasma proteins in distribution. 


Pharmacokinetics is the study of what the body does to the drug - the way the drug moves through the body, and the body’s effect to the drug. 


Absorption and distribution are both discussed above. 


Metabolism - the major site of drug metabolism is the liver


Excretion - the primary organ responsible for excretion of most drugs is the kidney

However, it is important to note that drugs can also be excreted through biliary or bowel excretion (this is not as important for the exam as kidney/renal)  

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5) Understand how different routes affect absorption and bioavailability


The different routes (oral, sublingual, IV, IM, ID, etc are all discussed above, as well as how bioavailability is affected with enteral vs parenteral). 

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6) Understand loading dose


**Loading dose - some drugs will need to be given a high dose first to be able to reach a therapeutic effect and then give maintenance (lower dose).

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7) Review Peak, trough, therapeutic window, therapeutic range, and toxicity table


Pharmacotherapeutics - using the drug to treat the patient, and the cellular changes that happen. 


Peak level is the highest blood level of a drug.

Trough level is the lowest blood level of a drug.

Therapeutic window - it is the dosage range between a minimum effective therapeutic concentration and the minimum toxic concentration.

Therapeutic range - the dosage range or blood plasma concentration usually expected to achieve the desired therapeutic effect.


Toxicity table:  Toxicity occurs if the peak blood level of the drug is too high.

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8) Different types of enteral routes


Please see above.

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9)  Understand what half-life is and how it affects drug administration


Half life is the time required for 50% of the drug to be removed from the body.

Knowing half life is important because this determines how often the medication needs to be given.

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10)  Teratogenic effect, carcinogenic effect

Teratogenic effect - When medications cause congenital disorders in developing embryo or fetus. This usually occurs in early pregnancy (first trimester). Example - needing to sign iPledge before starting Accutane.

Carcinogenic effect - It is when a medication directly causes cancer. Example - some chemotherapies.

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11)  What are the different drug categories in pregnancy? Which is the safest? Which is the ones that is most contraindicated?


Different drug categories:

Category A - Studies indicate no risk to human fetus. (SAFEST)

Category B - Studies indicate no risk to the animal fetus, information for humans is not available.

Category C - Adverse effects reported in the animal fetus, information for humans is not available.

Category D - Possible fetal risk in humans has been reported; however, in selected cases consideration of the potential benefit versus risk may warrant sue of these drugs in pregnant women.

Category X - Fetal abnormalities have been reported, and positive evidence of fetal risk in humans is available from animal and/or human studies. These drugs are not to be used in pregnant women. (MOSTCONTRAINDICATED)


Per new FDA rules - *discusses risk to pregnant woman and breastfeeding mother

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12)  What is a black box warning and the subcategories? Which one is worse?


Black-box warning is seen in meds where there is a reasonable possibility of serious adverse effects or death.

Schedule-I: HIGH abuse potential - no medical use - severe physical and psychological dependency potential. (HIGHEST WARNING - WORSE)

Schedule-II: HIGH abuse potential - accepted medical use - severe physical and psychological dependency potential.

Schedule-III: LESS THAN C-II abuse potential - accepted medical use - moderate to low physical and psychological dependency potential.

Schedule-IV: LESS THAN C-III abuse potential - accepted medical use - limited physical and psychological dependency potential.

Schedule-V: LESS THAN C-IV abuse potential - accepted medical use - limited physical and psychological dependency potential.

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13)  What are scheduled drugs and what does it mean?


Please see above. 

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14) Review medication errors and how to prevent them.

Medication errors -

Preventing - 

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15)  Reporting of medication errors

Reporting of medical errors - Report to prescriber and nursing management and document error per policy and protocols. BUT FIRST - ASSESS THAT THE PATIENT IS DOING WELL AFTER THE ERROR IS MADE.

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16) What is a medication reconciliation and why is it important?

what is it? Medication reconciliation is when the nurse verifies, clarifies, and reconciles the list of medications of a patient - including prescriptions, OTC medications, supplements, etc.

importance -Having an updated list is important in order to ensure that if the patient is having any symptoms that it may/may not be related to the things they are taking. it is also important for knowing any potential interactions if being prescribed a new medication.

when is it done - Upon admission, before patient is transferred to another unit

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17)  Older adult physiologic changes and pharmacokinetics

**** Their heart might not be working as well so they can have decreased cardiac output and blood flow and thus in absorption and distribution of meds.


Cardiovascular system

Decreased CO = decreased absorption and distribution

decreased blood flow = decreased absorption and distribution

GI

Increased pH = altered absorption

Decreased peristalsis = delayed gastric emptying

Hepatic

decreased enzyme production = decreased metabolism

*LESS PRODUCTION OF PROTEINS - DRUG BOUND PROTEINS ARE UNBOUND NOW WHICH LEADS TO INCREASED TOXICITY.

decreased blood flow = decreased metabolism

Renal

decreased blood flow = decreased excretion

decreased function = decreased excretion

decreased glomerular filtration rate = decreased excretion

*DECREASED GFR MEANS DRUGS ARE CLEARED LESS EFFECTIVELY.

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18)  Cultural assessment

  • Health benefits and practices - goal is to build trust with the patient

    •  Barriers to adequate health care for the culturally diverse U.S. patient population
      ◦Language, pride, and beliefs regarding medical practices
      ◦Medications may have a different meaning to different cultures.

  • Language spoken

    • Consider the use of an interpreter if needed.

  • Past uses of medicine

    • Historically - what have been their past use of medicine? 

  • Herbal treatments, folk remedies, and home remedies

    • Consider that others might have different ways of treatments and all of those things are important to consider when caring for them.

    • Ask: Tell me what you take at home? - that includes OTC drugs, supplements, teas, and any of the remedies mentioned above - they can affect the presentation of their symptoms of interfere with current medication.

  • Usual response to illness

  • Responsiveness to medical treatment

  • Religious practice and beliefs

    • Important for when considering treatment types for the patients and measures of care (like do they accept blood?)

  • Support from the patients cultural community

  • Dietary habits (certain foods can interact with meds) 

Patient Centered Care: Cultural Implications -

Cultural group - African

  • Common health benefits and alternative healers: Practice folk medicine, employ “root doctors” as healers (use herbs, roots, potions, and spells), spiritualists. Use herbs, oils, and roots.

  • Verbal and nonverbal communications; touch/time: Asking personal questions of someone met for the first time is seen as intrusive and not proper. Direct eye contact seen as rude and are present oriented.

  • Family: Have close, extended family ties; women play important key role in making health care decisions.

  • Biologic variations: Keloid formation, sickle cell anemia, lactose intolerance, skin color

Cultural group - Asian

  • Common health benefits and alternative healers: Believe in traditional medicine, hot and cold foods, herbs/teas/soups; use of acupuncturist, acupressurist, and herbalist. Tai Chi, QiGong (exercises)

  • Verbal and nonverbal communications; touch/time: High respect for others, especially individuals in positions of authority. Not usually comfortable with customs of shaking hands with those of opposite sex. Present oriented.

  • Family: Have close extended family ties; family’s more important than individual needs.

  • Biologic variations: Many drug interactions, lactose intolerance, skin color, thalassemia (inherited blood disorder where the body doesn’t make enough Hgb)


Cultural group - Hispanic

  • Common health benefits and alternative healers: View health as a result of good luck and living right; see illness as a result of doing a bad deed. Heat, cold, and herbs used as remedies. Use curandero, spiritualist.

  • Verbal and nonverbal communications; touch/time: Expressing negative feelings is seen as impolite. Avoiding eye contact is seen as respectful and attentive; touching acceptable between two persons in conversation.

  • Family: Have close extended family ties; all family members involved in healthcare decisions. Past cultural experiences in the family with illness and healing practices hold significant value. Strong adherence to cultural practices.

  • Biologic variations: Lactose intolerance, skin color.


Cultural group - Native American

  • Common health benefits and alternative healers: Believe in harmony with nature and ill spirits causing disease; use medicine man (spiritual healer)

  • Verbal and nonverbal communications; touch/time: Speak in low tone of voice, light touch of a person’s hands is preferred versus a firm handshake as a greeting. Present oriented.

  • Family: Have close extended family ties; emphasis on family.

  • Biologic variations: Lactose intolerance; skin color, cleft uvula problems.

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19) Review power Atlas of drug administration and major points discussed in class.

o   How to administer SubQ, Intradermal and IM drugs (Including z track technique) review needles used, amount of medication and angle to use for each. Understand which ones you draw back and why?

o   How to mix insulins (which one do you draw first and which one second)



Administering: Intramuscular (IM) medications

  • Needles used: 18-21 gauge

  • Amount of medication that can be given: 3 mL is the max

  • Angle used: 90 degrees

  • Special considerations:
    Technique: Z track technique - prevents med from leaking through the tissue as it can be irritating

    • PER BOOK - We insert the needle aspirate - if you see blood then do not inject, draw the needle and then go in again. (WHY? because you do not want to give the medication in the bloodstream, you want to give it intramuscularly).

    • PER CDC - you do not aspirate for self admin, or vaccines. 


Administering: Intradermal (ID) medications

  • Needles used: 25-27 gauge

  • Amount of medication that can be given: 0.1 mL max

  • Angle used: 15 degrees

  • Special considerations: N/A


Administering: Subcutaneous (SUBQ) medications

  • Needles used: 25-27 gauge

  • Amount of medication that can be given: 0.5-1 mL max

  • Angle used: 45 degrees, if patient has a lot of adipose tissue then 90 degrees

  • Special considerations:
    Examples are insulin and heparin. If injecting a blood thinner - DO NOT MASSAGE AREA as it can cause bruising.
    Location of medication is a nursing intervention - meaning it is up to the nurse.

Administering: Insulin

  • Use units when measuring amount of insulin, not mLs.

  • When drawing insulin - if using the same syringe - draw clear first then cloudy 

    • Check compatibility before mixing!!



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Analgesics/Sedatives/Anesthetics

20) Opioid analgesics discussed in class, mechanism of action (MOA), indications, side effects, reversal and nursing implications (Remember what to assess before and after and what to monitor for), what to do if RR is less than 10 and medication used to reverse it


  • What are they?

    • Analgesics - medications that relieve pain without losing consciousness.

    • Opioid drugs - synthetic drugs that bind to opiate receptors to relieve pain - VERY STRONG pain relievers. Used often to treat acute p/op pain, CA pain, and severe pain.

  • Types - Painkillers, opioid analgesics, adjuvant analgesic drugs (meds not primarily designed to control pain but can be used for this purpose).

  • Multimodal medications - use of more than one pharmacological class of analgesic medication targeting different receptors along the pain pathway with the goal of improving analgesia while reducing individual class-related side effects.

  • MOA

    • Opioid drugs - bind to opiate receptors to relieve pain.

      • They have 3 receptors (SEE PICTURE)

        • mu - most powerful when it comes to pain relief

        • kappa and delta will not have the same euphoric effect as mu

  • Indications:

    • Opioids - used for acute p/op pain, CA pain, and severe pain.

  • Side effects: Constipation is a common AE - try to prevent with adequate fluid and fiber intake.

    • OPIOID adverse effects: CNS depression (which leads to respiratory depression, it is the most serious AE), n/v, urinary retention, diaphoresis and flushing, pupil constriction (miosis), constipation, itching

  • Reversal: naloxone (Narcan) and naltrexone (ReVia)

    • Narcan - blocks opioid receptor completely, if suspect opioid overdose and pt has resp depression - we can give it. Pt will go into withdrawal which can be uncomfortable but at least they will be breathing.

  • Nursing implications: Before giving opioids, make sure you know VS.

    • Oral forms should be taken with food to minimize gastric upset.

    • Ensure safety measures, such as keeping side rails up.

    • Withhold dose and contact physician if decline in patient’s condition or VS, RR <10-12 bmp, may need Narcan.

    • Instruct patients to follow directions for administration carefully and to keep a record of their pain experience and response to treatments.

    • Change positions slowly to prevent orthostatic hypotension.

    • Assess bowel sounds before administration.

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21) What is an agonist, antagonist, and what is their effect usually?


Agonists

  • Bind to opioid pain receptor in the brain - cause analgesic response (reduction of pain sensation)

  • All come down to morphine -

Partial Agonist/Mixed Agonist/Agonist-Antagonist

  • Bind to pain receptor

  • Cause weaker neurologic response than full agonist

  • Can use these when trying to help a patient wean down if they are addicted to opioids

Antagonists

  • Reverse effects of these drugs in pain receptors (competitive antagonists)

  • Example - naloxone


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22) Non-pharmacologic pain control


  • Physical method like hot/cold therapy

  • Massage, touch

  • Therapeutic communication

  • Relaxation

  • Distraction

  • Coping skills training

  • Cognitive behavioral therapy

  • Transcutaneous electrical nerve stimulation (TENS) - uses low-voltage electrical currents to relieve pain. A TENS unit is a small device that delivers the current at or near your nerves to block or change your perception of pain 

  • Acupuncture

  • PT/Yoga/PEt therapy/ musci mindful meditation/ imagery


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23)  What is acetaminophen (Tylenol), mechanism of action, indications, side effects, main organ of concern, reversal agent, maximum daily dose, nursing implications (ie teaching and monitoring)


ACETAMINOPHEN (TYLENOL)

  • MOA: It blocks pain impulses peripherally by inhibiting prostaglandin synthesis in the CNS- AKA blocking signals that travel from the site of pain to your brain by interfering with the signals at the source before they reach the brain.

    • Acetaminophen has little to no real anti-inflammatory effects (it is considered an anti-inflammatory because it blocks prostaglandin - but it does not block the inflammatory cascade)

    • It provides analgesia and has antipyretic effect (reduce fever).

  • Indications:

    • Mild to moderate pain

    • Fever

    • Alternative to aspirin/NSAID products

    • Adjunct pain reliever

  • Side effects: Generally well tolerated.

    • Possible adverse effects include skin disorders, nausea, vomiting.

    • Less common - effects of blood disorders, nephrotoxicities, and hepatotoxicity (most serious).

  • Main organ of concern: Liver

  • Reversal agent (antidote): Acetylcysteine (Mucomyst)

  • Maximum daily dose: 3g a day

    • (if pt has liver disease don’t go over 2g/day)

  • Nursing implication (ie teaching and monitoring): (*Unclear if this is right*)

    • Assess the pain level to ensure acetaminophen is appropriate for their needs. Educate patient on purpose, effects, and proper usage. Monitor patient closely for any adverse reactions or side effects - including VS, liver function tests if necessary. 


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24) a) What are NSAIDs? 

They are large and chemically diverse group of drugs with the following properties:

  • Analgesic

  • Anti-inflammatory

  • Antipyreptic

  • Aspirin-platelet inhibition


b) Review main NSAIDs discussed in class in bold, mechanism of action, indications, main side effects and organs of concern, nursing implications and teaching to the patients, from the NSAIDs which ones work more on COX 2 and what is the benefit, and the main problem, signs of toxicity?


  • Main NSAIDS discussed in class

  • MOA: inhibiting leukotriene pathway, prostaglandin pathway, or both. Blocking chemical activity of COX

  • Which ones work more on COX2 and what is the benefit and main problem of this

    • One that works more on COX2 is Celebrex

    • Benefit of blocking COX2: it is only expressed in certain conditions like inflammatory responses (whereas COX1 is only expressed in almost all cells and it is always active)

    • Problem - then COX1 can become more enhanced

  • Indications: Mild to moderate headaches, myalgia, neuralgia, arthralgia, alleviation of p/op pain, relief of pain associated with arthritic disorders like RA, juvenile arthritis, ankylosing spondylitis, and osteoarthritis. Treatment of gout and hyperuricemia.

  • Main side effects:

    • GI: dyspepsia (discomfort in upper abdomen), heartburn, epigastric distress, nausea. GI bleeding (because of blocking blood flow to the gut - can cause GI bleeding GI upset), mucosal lesions.

    • Renal: reduction in creatinine clearance, acute tubular necrosis with renal failure(Kidney not getting enough blood flow leads to reduction in creatinine clearance - it is a reflection of glomerular filtration rate - if the kidney isn’t clearing it is not working)

    • CV: noncardiogenic pulmonary edema (the noncardiogenic pulmonary edema - not heart related but more so of the fluid accumulation and it is more than the heart can handle  - SUPER IMPROTANT - pts with cardiac history cannot be on a whole class of medications (NSAIDs) )

  • Organ of concern: GI, Renal, and CV

  • Signs of toxicity

  • Nursing implication and teaching to the patients: Assess for conditions that may be contraindications to therapy like GI lesions, peptic ulcer disease, bleeding disorders. labs like cardiac, renal, LFT, CBC, plt count). Educate patients about the various adverse effects of NSAIDs and inform them to notify their prescriber if the effects become severe or GI pain occurs. Inform that enteric-coated tablets should not be crushed or chewed.

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25) What is malignant hyperthermia and how would a patient with it present?


It is a genetic condition. Associated with administration of general anesthetics - symptoms will include

  • high temp

  • muscle rigidity (uncontrolled release of intracellular Ca which causes the muscles to contract)

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26) What is a neuromuscular blocking drug (NMBD)? What does it do?  (both types) . Does it provide analgesia or sedation? Can the patient breath on their own after receiving this medication? 

What is the nursing implication of this?


  • What does it do? They prevent nerve transmission in skeletal and smooth muscle, resulting in muscle paralysis.

  • Does it provide analgesia or sedation? No, they are strictly paralytic

  • Can the patient breathe on their own after receiving this medication? No, it causes muscle paralysis of the diaphragm and intercoastal muscles which are needed to breathe.

  • What is the nursing implication of this?

    • Always assess past history of surgeries and response to anesthesia.
      Assess past history of allergies, and medications.
      Assess use of alcohol, illicit drugs, and opioids.

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27) Succinylcholine MOA, side effects, indications, nursing implications and black box warning


Succinylcholine - a depolarizing neuromuscular blocking drug

  • MOA - binds to Ach receptors at neuromuscular joints, depolarizes receptors which cause Na channels to open = membrane polarizes (pt will have fasciculations followed by flaccid paralysis) = prevents repolarization from happening.

  • Side effects -

  • Indications - used mainly to facilitate controlled ventilation during surgical procedures - short acting (used with rapid sequence intubation). Also used to reduce muscle contraction in an area that needs surgery. Can also be used to diagnose MG.

  • Nursing Implications: Assess pass SHx and response to anesthesia, h/o allergies and meds, and use of alcohol, illicit drugs, and opioids. Assess VS, labwork, O2 stat, etc. Watch for sudden elevations in body temperature, which may indicate malignant hyperthermia.

  • Black box warning: Contraindicated in patients with personal or familial history of malignant hyperthermia and/or skeletal muscle myopathy. There have been rare reports of ventricular dysrhythmias and fatal cardiac arrest secondary to rhabdomyolysis with hyperkalemia, primarily in healthy-appearing pediatric patients who were subsequently found to have undiagnosed skeletal muscle myopathy, most frequently Duchenne’s muscular dystrophy. 

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28) General anesthetics, effects


General anesthetics - inhalation or IV

  • Block flow of Na+ into neurons, delay nerve impulses and reduce neural activity

    • Exact mechanism unknown but likely activate GABA receptors in the brain

  • They produce unconsciousness, lack of responsiveness to painful stimuli.

  • They can decrease metabolic rate, feeling cold, gut shuts down,

    • Some patients can be more sensitive to the anesthesia than others 

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29) Triptans (for migraines)- MOA


 Triptans - second line therapies for migraines (first is NSAIDS)

  • Examples Maxalt & Imitrex (Abortive treatment)

    • Stimulate 5-HT-1 cerebral arteries, causing vasoconstriction and reducing headache symptoms. They also reduce the production of inflammatory neuropeptides

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30)  Benzos (Diazepam, lorazepam)- MOA, indications, adverse effects, reversal agent, nursing implications. (Use for seizures too, especially status epilepticus)


Benzos (Diazepam, lorazepam) - most commonly prescribed sedative-hypnotic drug. Classified as either sedatives or hypnotic and antianxiety.

  • MOA - depress CNS activity in the brain. Facilitate the binding of the inhibitory neurotransmitter GABA at various receptors throughout the CNS = calming effect.

  • Indications: for sedation, sleep induction, skeletal muscle relaxation. Anxiety relief (if pt has severe anxiety attack which constitutes as an medical emergency - it acts quickly), treatment of acute seizures especially status epilepticus, treatment of alcohol withdrawal, agitation relief, balanced anesthesia, moderate/conscious sedation.

  • Adverse effects: Drowsy, dizziness, cognitive impairment, respiratory impairment (with overdose or drug interaction), lethargy, fall hazard for older patients, can have hangover effect the next day - daytime sleepiness.

  • Reversal agent: Flumazenil

    • Giving someone this medication can actually cause them to go into withdrawal which can lead to higher anxiety, seizure activity which can be dangerous. So in real life, we don’t use this anymore, we use supportive care.

  • Nursing implications: Monitor adverse effects, safety (side rails up, keep call light within reach, etc), most benzodiazepines cause REM rebound and a tired feeling the next day; use with caution in the elderly, instruct pts to avoid alcohol and CNS depressants.

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31) Salicylate toxicity: signs/symptoms

  • Toxicities of salicylate

    • Cardiovascular - increased HR

    • Pulmonary - bronchoconstriction 

    • Central nervous - tinnitus, HL, dimness of vision, HA, dizziness, mental confusion, lassitude, drowsiness 

    • GI - n/v/d

    • Metabolic: metabolic acidosis, sweating, thirst, hyperventilation, hypoglycemia or hyperglycemia

FYI - Salicylates are NSAIDS - example aspirin , inhibit COX1 and COX2. Do not give to children d/t risk of Reye’s syndrome.


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32)  Barbiturates (Phenobarbital mainly)- MOA, indications, adverse effects, nursing implications. Remember that this medication is an enzyme inducer. What does that mean?


Barbiturates (Phenobarbital mainly) - oldest sedating drug, can be very toxic very quickly.

  • MOA: They are potentiating GABA inhibition (meaning this promotes a calming effect of the nervous system), they are less selective than benzos which means can have more respiratory depression.

  • Indications: Sedatives (less likely), Anticonvulsants, Anesthesia for surgical procedures(more likely)

  • Adverse effects: Dependence, drowsiness, hypotension, respiratory depression, low plt count, hypersensitivity reaction like SJS, lack of restful sleep (interferes with REM sleep) which can lead to agitation and inability to deal with normal stress.

  • Toxicities: - at high doses it can have hypnotic effects and lower RR and can even lead to respiratory arrest. Overdose can produce CNS depression (sleep to coma and death)

  • Nursing implications -

**Remember, this medication is an enzyme inducer, what does this mean? This means that they stimulate the action of enzymes in the liver that are responsible for metabolism or breakdown of many drugs. By stimulating the action of these enzymes, they cause many drugs to be metabolized more quickly, which usually shortens their duration of action.

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Antiseizure/Parkinson/Anxiolytics



33) What are anticonvulsants or antiepileptic drugs? What is the goal of the therapy?


  • AEDs - they help prevent seizures while maintaining QOL. They work by stabilizing the electrical activity in the brain, thereby reducing the likelihood of abnormal excessive firing of neurons that can lead to seizures.

  • Patient might need a seizure regimen that consists of 1+ AED

  • Pts with true epilepsy it is a lifelong dx = meds forever


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34) a) Hydatoins family- Phenytoin (Dilantin) MOA, indications, adverse effects. Remember highly protein bound and what does this mean. Remember the therapeutic level. 

b)  Remember how is this drug different from Fosphenytoin, which one can be given IM and what happens if phenytoin is given IM or the IV infiltrates? How should this med be mixed and what tubing? How fast to give? Sign of toxicity. Remember teaching to the patient!


Hydatoins family - prototype drug is Dilantin

 Phenytoin (Dilantin)

  • MOA: Desensitize Na channels. It is a protein bound drug - meaning it is highly bound to protein (albumin). ((If patient has low albumin then this can lead to toxicity)).

  • Indications: Effective for most seizure types (except absence seizures), has anti-dysrhythmic properties. CAN BE GIVEN PO OR IV

  • Therapeutic effect (remember): Narrow therapeutic window of 10-20 mcg/mL. Toxicity happens over 20.

  • Adverse effects:

    • Can cause SJS. hyperglycemia, hypotension, v-fib, multiple blood dyscrasias (disorders) - assess for sore throat and fever! Can have androgen effect of excessive hair growth and development of acne.

    • IM - it can cause irritation in the skin leading to tissue necrosis.

    • IV: We can only give it with saline (as opposed to D5W - which is 5% dextrose with water) as it can precipitate and crystalize.

      • It needs to be a slow infusion as it can lower BP if given too quickly.

      • If it leaks into the nearby tissue, it can kill your hand (tissue necrosis) = purple glove

  • How should this med be mixed and what tubing?

    • Should be given with normal saline, mixed slowly and carefully to avoid precipitation.

    • Type of tubing - use line filter with pore size of 0.22 micrometers - this filter helps trap any potential particles or precipitates that may form during the mixing process, ensuring that only the dissolved medication reaches the patient's bloodstream.

  • How fast to give?

    • Depends, but slow infusion.

  • Signs of toxicity?


  • How is Phenytoin (Dilantin) different from Fosphenytoin?

    • Fosphenytoin (Celebryx) is a product of phenytoin. (NOT TO BE CONFUSED WITH CELEBREX WHICH IS AN NSAID)

      • It’s water soluble, meaning it can be given IV with D5W - which is 5% dextrose with water

      • Can be given IV at a faster rate

  • Which one can be given IM?

    • Only fosphenytoin 


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35)  Valproic acid- MOA, indications, adverse effects, therapeutic level, blood test needed to be done to monitor for adverse effects. Main organ of concern.

Valpiroic acid (Depakene)

  • MOA: desensitizes Na channels

  • Indications: Wide range of seizure types like focal, generalized, absence seizures. Also used for bipolar disorder.

  • Adverse effects: limited CNS depression, visual disturbances, ataxia, vertigo, headache. Additional ones include GI effects, hepatotoxicity, pancreatitis.

  • Therapeutic level: 50-100 mcg/mL

  • Blood test needed to monitor for AEs: Monitor LFTs at 2 month intervals

  • Main organ of concern: Liver- hepatic effects dysfunction possible in first 6 months 

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36)  Lamotrigine- MOA, indications, adverse effects (main one discussed in class).

Lamotrigine (Lamictal)

  • MOA: Blocks voltage gated Na channels in the nerve cells - which are essential for generating an electrical signal.

  • Indications: Focal and generalized seizures as well as bipolar disorder for mood stabilization.

    • No need for checking therapeutic levels as toxicity is rate with this med.

  • Adverse effect (main one discussed in class)- SJS

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37) Medication used for status epilepticus- Think Benzo. See above for MOA, side effects and reversal very important!


Status epilepticus - Continuous seizure activity >5 minutes without returning to baseline, can lead to a comma or death. Considered a medical emergency.

What meds are used: Benzodiazepines like diazepam (Valium)

  • Side effects - drowsiness, dizziness, respiratory depression

  • Reversal - Flumazenil (Romazicon)

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38) Parkinson disease, what is it, sign and symptoms and goals of pharmacological therapy.

PD

  • What is it? Chronic progressive degenerative disorder that affects the dopamine-producing neurons in the brain leading to low levels of dopamine. Since dopamine and Ach work in conjunction - when dopamine levels are decreased the Ach effects increase which is what causes the symptoms as the dopamine is no longer able to regulate the Ach.

  • Signs and symptoms: Loss of muscle control, tremors, bradykinesia, rigidity, postural instability, can lead to difficulty swallowing.

  • Goals of pharmacological therapy: Try to inhibit the breakdown of dopamine.

    • Carbidopa-Levodopa - prevents breakdown of catecholamines (dopamine) in the CNS, primarily in the brain, which leads to increase in dopamine levels.

    • Amantadine (Symmetrei) - causes release of dopamine. It was initially found as an antiviral agent for influenza but was seen that it causes a release in dopamine and thus used in the early diagnosis of PD to enhance dopamine on board.

    • BOTH DRUGS = Usually effective for a short period of time



      goal is to improve QOL and extend QOL - pt to be as independent as possible for as long as possible

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39)  Benztropine (Cogentin)- MOA, indications (remember avoid in elderly), side effects (Think anticholinergic)

Benztropine (Cogentin)

  • MOA: Anticholinergic drug used in the treatment of Parkinson’s disease and also of extrapyramidal symptoms from antipsychotic drug (block action of Ach).

  • Indications (remember avoid in elderly):  help with tardive dyskinesia and extrapyramidal symptoms - automatic involuntary movements that can occur with lip smacking (these can also occur with pts that are on anti psychotics but also with pts that have PD)  

    • Not a good medication for older patients, usually for younger patients with Parkinson's

  • Side effects (Think anticholinergic) - tachycardia, confusion, disorientation, toxic psychosis, urinary retention, dry throat, constipation, nausea, and vomiting

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40)  Review nursing implications for Parkinson meds.


Nursing implication

  • Perform a thorough assessment, nursing history, and medication history.

  • Include questions about the patient’s:

    • CNS

    • GI and GU tracts

    • psychologic and emotional status

      MAKE SURE U KNOW - goal is to improve QOL and extend QOL - pt to be as independent as possible for as long as possible

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41) Antipsychotics: adverse effects


Antipsychotics - Treat psychosis delirium schizophrenia (Block dopamine receptors in the brain)

  • Side effects are:

    • Neuroleptic malignant syndrome (NMS) - mental status change, rigidity, fever, and dysautonomia (can alter BP, HR, etc)

    • Myoglobinuria - excess amount of myoglobin in the urine (can indicate damage of the cell membranes of myocytes)

    • Extrapyramidal symptoms - sx include various motion disorders similar to those seen in PD

    • Tardive dyskinesia - repetitive, involuntary movements, such as grimacing and eye blinking.

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42) Lithium: therapeutic range


It has a very narrow therapeutic range (0.6-0.12 mmol/L - in labwork) - if toxicity occurs it can cause arrhythmias, epilepsy like seizures


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43) Side effects of SSRIs


Can feel too heightened (from my notes)

Anxiety, dizziness, drowsiness, headache, mild GI disturbance, sexual dysfunction, asthenia (weakness, lack of energy and strength), tremor (from the book).

If pt is on SSRI - concerned for suicide 

  • If pt was very depressed in the past but now they have a boost of energy with SSRIs, they can now have enough energy to plan to kill themselves 

Risk for serotonin syndrome (if toxicity)

  • Increased BP, HR

  • Delirium

  • Agitation

  • Sweating

  • Myoclonus (brief involuntary twitching or jerking of a muscle)

  • Hyperreflexia

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44)  Medication to treat extrapyramidal side effects.

Anticholinergic and antihistaminergic medications - the one mentioned in class was anticholinergic

Anticholinergic drug like Benztropine (Cogentin) 

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45)  How to prevent lithium toxicity-nursing teaching interventions


Lithium is a drug used to treat bipolar disorder - old drug choice for mania. 

It works by interfering with the Na ion transport as it uses the same pathway - the exact mechanism is unclear though. But we do need to keep an eye on the Na levels. 

It has a very narrow therapeutic range (0.6-0.12 mmol/L - in labwork) - if toxicity occurs it can cause arrhythmias, epilepsy like seizures

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*MOA- mechanism of action

* in the exam both brand and generic names will be used

* Good luck studying!!!

===

From her lectures

  • NMBD - depolarizing vs non-depolarizing 

Depolarizing - succinylcholine (for short acting short procedure) is the one we use, use with rapid sequence intubation 

  • Depolarizing succinylcholine - (non competitive) works by binding with Ach receptors at neuromuscular joints - cause Na channels to open membrane depolarizes- then pt will have fascilulations- then flaccid paralysis  - prevents repolarization from happening

Non depolarizing - most common, paralyzed for longer periods

  • They will compete with acetylcholine for cholinergic receptors at neuromuscular junctions, do not depolarize the muscle

  • Prevent depolarization from happening 

  • Drugs end with -urium


  • Xanax

  • commonly used anxiolytics - used for Generalized anxiety disorder - short term relief of anxiety symptoms

  • CNS depression is a common side effect


  • Ativan

    • used for seizure activity - first line AED

    • You can also use diazepam, midazolam to stop seizure activity



KA

Pharmacology Exam #1 Study Guide

Intro To Pharm/Med Errors/Drug Atlas

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1) Rights of medication administration

  1. Right drug - must check the name of the drug 3 times - at the medical administration record, while drawing up the medication, and again at bedside before giving it to the patient. Don’t forget to ask the patient if they have any allergies or have had a prior allergic reaction to that medication in the past.

  2. Right dose - become familiar with the dosing, or cross reference with a book or the EHR

  3. Right time - some drugs need to reach a therapeutic level to be able to work well on the receptor. Just because it is scheduled for 2 pm does not mean that it needs to be given at that time - if the toxicity level is too high, then it should not be given as it can harm the patient. Toxicity can be checked with labs for example. 

  4. Right route - know that it is the right route for the patient. 

    1. For example - if a patient has been ordered a PO medication but they have AMS/fatigue/dysphagia/etc then the route might need to be changed. ((i think call pharmacy to see if there is another route that the drug can be given and then if there is - call provider and ask to change the order)) 

  5. Right patient - use 2 identifiers such as name and DOB, double check their ID band. Make sure to check the med order against their ID band by scanning it and making sure that they match. 

  6. Right documentation - We document the date, time, route, dose, site of administration. 

  7. Right reason or indication - We need ro know why the meds are being given.

    1. For example - if a patient has a headache and the provider orders Tylenol, but then they develop a fever - the Tylenol can only be given for the headache and the provider must be notified about the fever as they will need to determine what the underlying cause of it is. 

  8. Right response - ensure the patient is responding well to the medication - in terms of the therapeutic effects (is the patient’s problem improving with the medication), in terms of the side effects and adverse effects (are they experiencing any and how severe are they?) 

  9. Right to refuse - need to inform the patient that they are allowed to refuse the medication at any time-  but we need to ensure that they are sound of mind - meaning they are able to make the right decisions 

**there are 9 rights, other ones have been proposed but for the sake of the class and exam, we only need to know those.

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2) Pharmaceutics: understand how different forms of the medication affect its dissolution and absorption into the body


ENTERAL - mouth and GI

  • Drugs given orally, sublingual (however, this one goes directly into the  bloodstream since there are many blood vessels under the tongue and thus bypasses the ‘first pass effect’ - but because it is considered PO it is considered enteral), buccal, rectal and vaginal (but can also be considered topical). 

  • This will first undergo ‘first pass effect’ - meaning it will go though the liver to be metabolized (AKA break down the drug into its active components) so the drug can have its active effect on the target tissue. 

    • Another way to define it is the processing of that drug by the liver. 

  • Bioavailability is the amount of the drug that is available when it reaches the target tissue/organ after the first pass effect of an ENTERAL drug. 

    • Not all drugs have high bioavailability -for example Bactrim has 100% bioavailability, vancomycin has 0% bioavailability. 

  • This means that Bactim, when taking ENTERAL it will have 100% of the drug reaching the target tissue/organ after it has been metabolized by the liver. 

  • Vancomycin, when taking ENTERAL will have 0% reaching the drug after it has been processed by the liver. 


PARENTERAL - into the bloodstream 

  • Drugs given IV, IM, SUBQ, ID, intraarterial, intrathecal, intraarticular (directly into the joints)

  • These do not need to go through the liver (AKA no need for first pass effect) as it goes directly into the bloodstream

  • PARENTERAL drugs will always have 100% bioavailability since they are administered directly into the bloodstream 


TOPICAL - through the skin

  • Drugs to the skin including transdermal patches (PARENTERAL), ointments (messier but more effective), gels, creams (less effective because they are water based, but often preferred by patients), 


DISTRIBUTION - protein bound drugs 

  • Some medications are protein bound when they get into the bloodstream - meaning they use the proteins in your plasma to travel through the bloodstream and reach the target tissue/organs.

  • Albumin is the most abundant protein in plasma, it helps hold water within the blood vessels (if low, then water leaks and this leads to edema). 

  • When protein-bound drugs enter the bloodstream, they will mainly bind to albumin (as it is the most abundant) and be carried to the target tissue/organ. The remaining drug will stay in the bloodstream ready to be metabolized. 

  • Eventually as the free flowing drug in the body decreases (bc it has been metabolized) then some of the bound drug (to albumin) will unbind and get released into the bloodstream to continue being metabolized.

  • If a patient has low albumin levels, they will have extra medication in the bloodstream - meaning more effect which can lead to higher drug toxicity. 

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3) Remember which medications should not be crushed


Extended release - d/t being a higher dose and it dissolves slowly - this is used to reduce amount of time per day that medication is taken. 

Coated - meds can be coated for a purpose such as taste masking, protecting med from moisture, or facilitating swallowing. Enteric coated - the coating is designed to resist the acidic environment of the stomach and dissolve in the alkaline environment of the intestines - ensuring the medication is released at a specific location in the GI tract - this coating is used for meds that may cause irritation to the stomach lining or that need to be absorbed by the intestine for optimal effectiveness. Coated or enteric coated medication should not be crushed as they are designed to release the active ingredient in a controlled manner and crushing them will affect their safety and efficacy which can lead to pt having adverse effects or treatment failure. 

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4) In pharmacokinetics review the following concepts: absorption, distribution, metabolism, and excretion. Remember main organs in charged of metabolism and excretion as well, plasma proteins in distribution. 


Pharmacokinetics is the study of what the body does to the drug - the way the drug moves through the body, and the body’s effect to the drug. 


Absorption and distribution are both discussed above. 


Metabolism - the major site of drug metabolism is the liver


Excretion - the primary organ responsible for excretion of most drugs is the kidney

However, it is important to note that drugs can also be excreted through biliary or bowel excretion (this is not as important for the exam as kidney/renal)  

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5) Understand how different routes affect absorption and bioavailability


The different routes (oral, sublingual, IV, IM, ID, etc are all discussed above, as well as how bioavailability is affected with enteral vs parenteral). 

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6) Understand loading dose


**Loading dose - some drugs will need to be given a high dose first to be able to reach a therapeutic effect and then give maintenance (lower dose).

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7) Review Peak, trough, therapeutic window, therapeutic range, and toxicity table


Pharmacotherapeutics - using the drug to treat the patient, and the cellular changes that happen. 


Peak level is the highest blood level of a drug.

Trough level is the lowest blood level of a drug.

Therapeutic window - it is the dosage range between a minimum effective therapeutic concentration and the minimum toxic concentration.

Therapeutic range - the dosage range or blood plasma concentration usually expected to achieve the desired therapeutic effect.


Toxicity table:  Toxicity occurs if the peak blood level of the drug is too high.

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8) Different types of enteral routes


Please see above.

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9)  Understand what half-life is and how it affects drug administration


Half life is the time required for 50% of the drug to be removed from the body.

Knowing half life is important because this determines how often the medication needs to be given.

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10)  Teratogenic effect, carcinogenic effect

Teratogenic effect - When medications cause congenital disorders in developing embryo or fetus. This usually occurs in early pregnancy (first trimester). Example - needing to sign iPledge before starting Accutane.

Carcinogenic effect - It is when a medication directly causes cancer. Example - some chemotherapies.

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11)  What are the different drug categories in pregnancy? Which is the safest? Which is the ones that is most contraindicated?


Different drug categories:

Category A - Studies indicate no risk to human fetus. (SAFEST)

Category B - Studies indicate no risk to the animal fetus, information for humans is not available.

Category C - Adverse effects reported in the animal fetus, information for humans is not available.

Category D - Possible fetal risk in humans has been reported; however, in selected cases consideration of the potential benefit versus risk may warrant sue of these drugs in pregnant women.

Category X - Fetal abnormalities have been reported, and positive evidence of fetal risk in humans is available from animal and/or human studies. These drugs are not to be used in pregnant women. (MOSTCONTRAINDICATED)


Per new FDA rules - *discusses risk to pregnant woman and breastfeeding mother

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12)  What is a black box warning and the subcategories? Which one is worse?


Black-box warning is seen in meds where there is a reasonable possibility of serious adverse effects or death.

Schedule-I: HIGH abuse potential - no medical use - severe physical and psychological dependency potential. (HIGHEST WARNING - WORSE)

Schedule-II: HIGH abuse potential - accepted medical use - severe physical and psychological dependency potential.

Schedule-III: LESS THAN C-II abuse potential - accepted medical use - moderate to low physical and psychological dependency potential.

Schedule-IV: LESS THAN C-III abuse potential - accepted medical use - limited physical and psychological dependency potential.

Schedule-V: LESS THAN C-IV abuse potential - accepted medical use - limited physical and psychological dependency potential.

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13)  What are scheduled drugs and what does it mean?


Please see above. 

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14) Review medication errors and how to prevent them.

Medication errors -

Preventing - 

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15)  Reporting of medication errors

Reporting of medical errors - Report to prescriber and nursing management and document error per policy and protocols. BUT FIRST - ASSESS THAT THE PATIENT IS DOING WELL AFTER THE ERROR IS MADE.

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16) What is a medication reconciliation and why is it important?

what is it? Medication reconciliation is when the nurse verifies, clarifies, and reconciles the list of medications of a patient - including prescriptions, OTC medications, supplements, etc.

importance -Having an updated list is important in order to ensure that if the patient is having any symptoms that it may/may not be related to the things they are taking. it is also important for knowing any potential interactions if being prescribed a new medication.

when is it done - Upon admission, before patient is transferred to another unit

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17)  Older adult physiologic changes and pharmacokinetics

**** Their heart might not be working as well so they can have decreased cardiac output and blood flow and thus in absorption and distribution of meds.


Cardiovascular system

Decreased CO = decreased absorption and distribution

decreased blood flow = decreased absorption and distribution

GI

Increased pH = altered absorption

Decreased peristalsis = delayed gastric emptying

Hepatic

decreased enzyme production = decreased metabolism

*LESS PRODUCTION OF PROTEINS - DRUG BOUND PROTEINS ARE UNBOUND NOW WHICH LEADS TO INCREASED TOXICITY.

decreased blood flow = decreased metabolism

Renal

decreased blood flow = decreased excretion

decreased function = decreased excretion

decreased glomerular filtration rate = decreased excretion

*DECREASED GFR MEANS DRUGS ARE CLEARED LESS EFFECTIVELY.

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18)  Cultural assessment

  • Health benefits and practices - goal is to build trust with the patient

    •  Barriers to adequate health care for the culturally diverse U.S. patient population
      ◦Language, pride, and beliefs regarding medical practices
      ◦Medications may have a different meaning to different cultures.

  • Language spoken

    • Consider the use of an interpreter if needed.

  • Past uses of medicine

    • Historically - what have been their past use of medicine? 

  • Herbal treatments, folk remedies, and home remedies

    • Consider that others might have different ways of treatments and all of those things are important to consider when caring for them.

    • Ask: Tell me what you take at home? - that includes OTC drugs, supplements, teas, and any of the remedies mentioned above - they can affect the presentation of their symptoms of interfere with current medication.

  • Usual response to illness

  • Responsiveness to medical treatment

  • Religious practice and beliefs

    • Important for when considering treatment types for the patients and measures of care (like do they accept blood?)

  • Support from the patients cultural community

  • Dietary habits (certain foods can interact with meds) 

Patient Centered Care: Cultural Implications -

Cultural group - African

  • Common health benefits and alternative healers: Practice folk medicine, employ “root doctors” as healers (use herbs, roots, potions, and spells), spiritualists. Use herbs, oils, and roots.

  • Verbal and nonverbal communications; touch/time: Asking personal questions of someone met for the first time is seen as intrusive and not proper. Direct eye contact seen as rude and are present oriented.

  • Family: Have close, extended family ties; women play important key role in making health care decisions.

  • Biologic variations: Keloid formation, sickle cell anemia, lactose intolerance, skin color

Cultural group - Asian

  • Common health benefits and alternative healers: Believe in traditional medicine, hot and cold foods, herbs/teas/soups; use of acupuncturist, acupressurist, and herbalist. Tai Chi, QiGong (exercises)

  • Verbal and nonverbal communications; touch/time: High respect for others, especially individuals in positions of authority. Not usually comfortable with customs of shaking hands with those of opposite sex. Present oriented.

  • Family: Have close extended family ties; family’s more important than individual needs.

  • Biologic variations: Many drug interactions, lactose intolerance, skin color, thalassemia (inherited blood disorder where the body doesn’t make enough Hgb)


Cultural group - Hispanic

  • Common health benefits and alternative healers: View health as a result of good luck and living right; see illness as a result of doing a bad deed. Heat, cold, and herbs used as remedies. Use curandero, spiritualist.

  • Verbal and nonverbal communications; touch/time: Expressing negative feelings is seen as impolite. Avoiding eye contact is seen as respectful and attentive; touching acceptable between two persons in conversation.

  • Family: Have close extended family ties; all family members involved in healthcare decisions. Past cultural experiences in the family with illness and healing practices hold significant value. Strong adherence to cultural practices.

  • Biologic variations: Lactose intolerance, skin color.


Cultural group - Native American

  • Common health benefits and alternative healers: Believe in harmony with nature and ill spirits causing disease; use medicine man (spiritual healer)

  • Verbal and nonverbal communications; touch/time: Speak in low tone of voice, light touch of a person’s hands is preferred versus a firm handshake as a greeting. Present oriented.

  • Family: Have close extended family ties; emphasis on family.

  • Biologic variations: Lactose intolerance; skin color, cleft uvula problems.

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19) Review power Atlas of drug administration and major points discussed in class.

o   How to administer SubQ, Intradermal and IM drugs (Including z track technique) review needles used, amount of medication and angle to use for each. Understand which ones you draw back and why?

o   How to mix insulins (which one do you draw first and which one second)



Administering: Intramuscular (IM) medications

  • Needles used: 18-21 gauge

  • Amount of medication that can be given: 3 mL is the max

  • Angle used: 90 degrees

  • Special considerations:
    Technique: Z track technique - prevents med from leaking through the tissue as it can be irritating

    • PER BOOK - We insert the needle aspirate - if you see blood then do not inject, draw the needle and then go in again. (WHY? because you do not want to give the medication in the bloodstream, you want to give it intramuscularly).

    • PER CDC - you do not aspirate for self admin, or vaccines. 


Administering: Intradermal (ID) medications

  • Needles used: 25-27 gauge

  • Amount of medication that can be given: 0.1 mL max

  • Angle used: 15 degrees

  • Special considerations: N/A


Administering: Subcutaneous (SUBQ) medications

  • Needles used: 25-27 gauge

  • Amount of medication that can be given: 0.5-1 mL max

  • Angle used: 45 degrees, if patient has a lot of adipose tissue then 90 degrees

  • Special considerations:
    Examples are insulin and heparin. If injecting a blood thinner - DO NOT MASSAGE AREA as it can cause bruising.
    Location of medication is a nursing intervention - meaning it is up to the nurse.

Administering: Insulin

  • Use units when measuring amount of insulin, not mLs.

  • When drawing insulin - if using the same syringe - draw clear first then cloudy 

    • Check compatibility before mixing!!



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Analgesics/Sedatives/Anesthetics

20) Opioid analgesics discussed in class, mechanism of action (MOA), indications, side effects, reversal and nursing implications (Remember what to assess before and after and what to monitor for), what to do if RR is less than 10 and medication used to reverse it


  • What are they?

    • Analgesics - medications that relieve pain without losing consciousness.

    • Opioid drugs - synthetic drugs that bind to opiate receptors to relieve pain - VERY STRONG pain relievers. Used often to treat acute p/op pain, CA pain, and severe pain.

  • Types - Painkillers, opioid analgesics, adjuvant analgesic drugs (meds not primarily designed to control pain but can be used for this purpose).

  • Multimodal medications - use of more than one pharmacological class of analgesic medication targeting different receptors along the pain pathway with the goal of improving analgesia while reducing individual class-related side effects.

  • MOA

    • Opioid drugs - bind to opiate receptors to relieve pain.

      • They have 3 receptors (SEE PICTURE)

        • mu - most powerful when it comes to pain relief

        • kappa and delta will not have the same euphoric effect as mu

  • Indications:

    • Opioids - used for acute p/op pain, CA pain, and severe pain.

  • Side effects: Constipation is a common AE - try to prevent with adequate fluid and fiber intake.

    • OPIOID adverse effects: CNS depression (which leads to respiratory depression, it is the most serious AE), n/v, urinary retention, diaphoresis and flushing, pupil constriction (miosis), constipation, itching

  • Reversal: naloxone (Narcan) and naltrexone (ReVia)

    • Narcan - blocks opioid receptor completely, if suspect opioid overdose and pt has resp depression - we can give it. Pt will go into withdrawal which can be uncomfortable but at least they will be breathing.

  • Nursing implications: Before giving opioids, make sure you know VS.

    • Oral forms should be taken with food to minimize gastric upset.

    • Ensure safety measures, such as keeping side rails up.

    • Withhold dose and contact physician if decline in patient’s condition or VS, RR <10-12 bmp, may need Narcan.

    • Instruct patients to follow directions for administration carefully and to keep a record of their pain experience and response to treatments.

    • Change positions slowly to prevent orthostatic hypotension.

    • Assess bowel sounds before administration.

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21) What is an agonist, antagonist, and what is their effect usually?


Agonists

  • Bind to opioid pain receptor in the brain - cause analgesic response (reduction of pain sensation)

  • All come down to morphine -

Partial Agonist/Mixed Agonist/Agonist-Antagonist

  • Bind to pain receptor

  • Cause weaker neurologic response than full agonist

  • Can use these when trying to help a patient wean down if they are addicted to opioids

Antagonists

  • Reverse effects of these drugs in pain receptors (competitive antagonists)

  • Example - naloxone


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22) Non-pharmacologic pain control


  • Physical method like hot/cold therapy

  • Massage, touch

  • Therapeutic communication

  • Relaxation

  • Distraction

  • Coping skills training

  • Cognitive behavioral therapy

  • Transcutaneous electrical nerve stimulation (TENS) - uses low-voltage electrical currents to relieve pain. A TENS unit is a small device that delivers the current at or near your nerves to block or change your perception of pain 

  • Acupuncture

  • PT/Yoga/PEt therapy/ musci mindful meditation/ imagery


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23)  What is acetaminophen (Tylenol), mechanism of action, indications, side effects, main organ of concern, reversal agent, maximum daily dose, nursing implications (ie teaching and monitoring)


ACETAMINOPHEN (TYLENOL)

  • MOA: It blocks pain impulses peripherally by inhibiting prostaglandin synthesis in the CNS- AKA blocking signals that travel from the site of pain to your brain by interfering with the signals at the source before they reach the brain.

    • Acetaminophen has little to no real anti-inflammatory effects (it is considered an anti-inflammatory because it blocks prostaglandin - but it does not block the inflammatory cascade)

    • It provides analgesia and has antipyretic effect (reduce fever).

  • Indications:

    • Mild to moderate pain

    • Fever

    • Alternative to aspirin/NSAID products

    • Adjunct pain reliever

  • Side effects: Generally well tolerated.

    • Possible adverse effects include skin disorders, nausea, vomiting.

    • Less common - effects of blood disorders, nephrotoxicities, and hepatotoxicity (most serious).

  • Main organ of concern: Liver

  • Reversal agent (antidote): Acetylcysteine (Mucomyst)

  • Maximum daily dose: 3g a day

    • (if pt has liver disease don’t go over 2g/day)

  • Nursing implication (ie teaching and monitoring): (*Unclear if this is right*)

    • Assess the pain level to ensure acetaminophen is appropriate for their needs. Educate patient on purpose, effects, and proper usage. Monitor patient closely for any adverse reactions or side effects - including VS, liver function tests if necessary. 


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24) a) What are NSAIDs? 

They are large and chemically diverse group of drugs with the following properties:

  • Analgesic

  • Anti-inflammatory

  • Antipyreptic

  • Aspirin-platelet inhibition


b) Review main NSAIDs discussed in class in bold, mechanism of action, indications, main side effects and organs of concern, nursing implications and teaching to the patients, from the NSAIDs which ones work more on COX 2 and what is the benefit, and the main problem, signs of toxicity?


  • Main NSAIDS discussed in class

  • MOA: inhibiting leukotriene pathway, prostaglandin pathway, or both. Blocking chemical activity of COX

  • Which ones work more on COX2 and what is the benefit and main problem of this

    • One that works more on COX2 is Celebrex

    • Benefit of blocking COX2: it is only expressed in certain conditions like inflammatory responses (whereas COX1 is only expressed in almost all cells and it is always active)

    • Problem - then COX1 can become more enhanced

  • Indications: Mild to moderate headaches, myalgia, neuralgia, arthralgia, alleviation of p/op pain, relief of pain associated with arthritic disorders like RA, juvenile arthritis, ankylosing spondylitis, and osteoarthritis. Treatment of gout and hyperuricemia.

  • Main side effects:

    • GI: dyspepsia (discomfort in upper abdomen), heartburn, epigastric distress, nausea. GI bleeding (because of blocking blood flow to the gut - can cause GI bleeding GI upset), mucosal lesions.

    • Renal: reduction in creatinine clearance, acute tubular necrosis with renal failure(Kidney not getting enough blood flow leads to reduction in creatinine clearance - it is a reflection of glomerular filtration rate - if the kidney isn’t clearing it is not working)

    • CV: noncardiogenic pulmonary edema (the noncardiogenic pulmonary edema - not heart related but more so of the fluid accumulation and it is more than the heart can handle  - SUPER IMPROTANT - pts with cardiac history cannot be on a whole class of medications (NSAIDs) )

  • Organ of concern: GI, Renal, and CV

  • Signs of toxicity

  • Nursing implication and teaching to the patients: Assess for conditions that may be contraindications to therapy like GI lesions, peptic ulcer disease, bleeding disorders. labs like cardiac, renal, LFT, CBC, plt count). Educate patients about the various adverse effects of NSAIDs and inform them to notify their prescriber if the effects become severe or GI pain occurs. Inform that enteric-coated tablets should not be crushed or chewed.

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25) What is malignant hyperthermia and how would a patient with it present?


It is a genetic condition. Associated with administration of general anesthetics - symptoms will include

  • high temp

  • muscle rigidity (uncontrolled release of intracellular Ca which causes the muscles to contract)

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26) What is a neuromuscular blocking drug (NMBD)? What does it do?  (both types) . Does it provide analgesia or sedation? Can the patient breath on their own after receiving this medication? 

What is the nursing implication of this?


  • What does it do? They prevent nerve transmission in skeletal and smooth muscle, resulting in muscle paralysis.

  • Does it provide analgesia or sedation? No, they are strictly paralytic

  • Can the patient breathe on their own after receiving this medication? No, it causes muscle paralysis of the diaphragm and intercoastal muscles which are needed to breathe.

  • What is the nursing implication of this?

    • Always assess past history of surgeries and response to anesthesia.
      Assess past history of allergies, and medications.
      Assess use of alcohol, illicit drugs, and opioids.

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27) Succinylcholine MOA, side effects, indications, nursing implications and black box warning


Succinylcholine - a depolarizing neuromuscular blocking drug

  • MOA - binds to Ach receptors at neuromuscular joints, depolarizes receptors which cause Na channels to open = membrane polarizes (pt will have fasciculations followed by flaccid paralysis) = prevents repolarization from happening.

  • Side effects -

  • Indications - used mainly to facilitate controlled ventilation during surgical procedures - short acting (used with rapid sequence intubation). Also used to reduce muscle contraction in an area that needs surgery. Can also be used to diagnose MG.

  • Nursing Implications: Assess pass SHx and response to anesthesia, h/o allergies and meds, and use of alcohol, illicit drugs, and opioids. Assess VS, labwork, O2 stat, etc. Watch for sudden elevations in body temperature, which may indicate malignant hyperthermia.

  • Black box warning: Contraindicated in patients with personal or familial history of malignant hyperthermia and/or skeletal muscle myopathy. There have been rare reports of ventricular dysrhythmias and fatal cardiac arrest secondary to rhabdomyolysis with hyperkalemia, primarily in healthy-appearing pediatric patients who were subsequently found to have undiagnosed skeletal muscle myopathy, most frequently Duchenne’s muscular dystrophy. 

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28) General anesthetics, effects


General anesthetics - inhalation or IV

  • Block flow of Na+ into neurons, delay nerve impulses and reduce neural activity

    • Exact mechanism unknown but likely activate GABA receptors in the brain

  • They produce unconsciousness, lack of responsiveness to painful stimuli.

  • They can decrease metabolic rate, feeling cold, gut shuts down,

    • Some patients can be more sensitive to the anesthesia than others 

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29) Triptans (for migraines)- MOA


 Triptans - second line therapies for migraines (first is NSAIDS)

  • Examples Maxalt & Imitrex (Abortive treatment)

    • Stimulate 5-HT-1 cerebral arteries, causing vasoconstriction and reducing headache symptoms. They also reduce the production of inflammatory neuropeptides

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30)  Benzos (Diazepam, lorazepam)- MOA, indications, adverse effects, reversal agent, nursing implications. (Use for seizures too, especially status epilepticus)


Benzos (Diazepam, lorazepam) - most commonly prescribed sedative-hypnotic drug. Classified as either sedatives or hypnotic and antianxiety.

  • MOA - depress CNS activity in the brain. Facilitate the binding of the inhibitory neurotransmitter GABA at various receptors throughout the CNS = calming effect.

  • Indications: for sedation, sleep induction, skeletal muscle relaxation. Anxiety relief (if pt has severe anxiety attack which constitutes as an medical emergency - it acts quickly), treatment of acute seizures especially status epilepticus, treatment of alcohol withdrawal, agitation relief, balanced anesthesia, moderate/conscious sedation.

  • Adverse effects: Drowsy, dizziness, cognitive impairment, respiratory impairment (with overdose or drug interaction), lethargy, fall hazard for older patients, can have hangover effect the next day - daytime sleepiness.

  • Reversal agent: Flumazenil

    • Giving someone this medication can actually cause them to go into withdrawal which can lead to higher anxiety, seizure activity which can be dangerous. So in real life, we don’t use this anymore, we use supportive care.

  • Nursing implications: Monitor adverse effects, safety (side rails up, keep call light within reach, etc), most benzodiazepines cause REM rebound and a tired feeling the next day; use with caution in the elderly, instruct pts to avoid alcohol and CNS depressants.

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31) Salicylate toxicity: signs/symptoms

  • Toxicities of salicylate

    • Cardiovascular - increased HR

    • Pulmonary - bronchoconstriction 

    • Central nervous - tinnitus, HL, dimness of vision, HA, dizziness, mental confusion, lassitude, drowsiness 

    • GI - n/v/d

    • Metabolic: metabolic acidosis, sweating, thirst, hyperventilation, hypoglycemia or hyperglycemia

FYI - Salicylates are NSAIDS - example aspirin , inhibit COX1 and COX2. Do not give to children d/t risk of Reye’s syndrome.


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32)  Barbiturates (Phenobarbital mainly)- MOA, indications, adverse effects, nursing implications. Remember that this medication is an enzyme inducer. What does that mean?


Barbiturates (Phenobarbital mainly) - oldest sedating drug, can be very toxic very quickly.

  • MOA: They are potentiating GABA inhibition (meaning this promotes a calming effect of the nervous system), they are less selective than benzos which means can have more respiratory depression.

  • Indications: Sedatives (less likely), Anticonvulsants, Anesthesia for surgical procedures(more likely)

  • Adverse effects: Dependence, drowsiness, hypotension, respiratory depression, low plt count, hypersensitivity reaction like SJS, lack of restful sleep (interferes with REM sleep) which can lead to agitation and inability to deal with normal stress.

  • Toxicities: - at high doses it can have hypnotic effects and lower RR and can even lead to respiratory arrest. Overdose can produce CNS depression (sleep to coma and death)

  • Nursing implications -

**Remember, this medication is an enzyme inducer, what does this mean? This means that they stimulate the action of enzymes in the liver that are responsible for metabolism or breakdown of many drugs. By stimulating the action of these enzymes, they cause many drugs to be metabolized more quickly, which usually shortens their duration of action.

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Antiseizure/Parkinson/Anxiolytics



33) What are anticonvulsants or antiepileptic drugs? What is the goal of the therapy?


  • AEDs - they help prevent seizures while maintaining QOL. They work by stabilizing the electrical activity in the brain, thereby reducing the likelihood of abnormal excessive firing of neurons that can lead to seizures.

  • Patient might need a seizure regimen that consists of 1+ AED

  • Pts with true epilepsy it is a lifelong dx = meds forever


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34) a) Hydatoins family- Phenytoin (Dilantin) MOA, indications, adverse effects. Remember highly protein bound and what does this mean. Remember the therapeutic level. 

b)  Remember how is this drug different from Fosphenytoin, which one can be given IM and what happens if phenytoin is given IM or the IV infiltrates? How should this med be mixed and what tubing? How fast to give? Sign of toxicity. Remember teaching to the patient!


Hydatoins family - prototype drug is Dilantin

 Phenytoin (Dilantin)

  • MOA: Desensitize Na channels. It is a protein bound drug - meaning it is highly bound to protein (albumin). ((If patient has low albumin then this can lead to toxicity)).

  • Indications: Effective for most seizure types (except absence seizures), has anti-dysrhythmic properties. CAN BE GIVEN PO OR IV

  • Therapeutic effect (remember): Narrow therapeutic window of 10-20 mcg/mL. Toxicity happens over 20.

  • Adverse effects:

    • Can cause SJS. hyperglycemia, hypotension, v-fib, multiple blood dyscrasias (disorders) - assess for sore throat and fever! Can have androgen effect of excessive hair growth and development of acne.

    • IM - it can cause irritation in the skin leading to tissue necrosis.

    • IV: We can only give it with saline (as opposed to D5W - which is 5% dextrose with water) as it can precipitate and crystalize.

      • It needs to be a slow infusion as it can lower BP if given too quickly.

      • If it leaks into the nearby tissue, it can kill your hand (tissue necrosis) = purple glove

  • How should this med be mixed and what tubing?

    • Should be given with normal saline, mixed slowly and carefully to avoid precipitation.

    • Type of tubing - use line filter with pore size of 0.22 micrometers - this filter helps trap any potential particles or precipitates that may form during the mixing process, ensuring that only the dissolved medication reaches the patient's bloodstream.

  • How fast to give?

    • Depends, but slow infusion.

  • Signs of toxicity?


  • How is Phenytoin (Dilantin) different from Fosphenytoin?

    • Fosphenytoin (Celebryx) is a product of phenytoin. (NOT TO BE CONFUSED WITH CELEBREX WHICH IS AN NSAID)

      • It’s water soluble, meaning it can be given IV with D5W - which is 5% dextrose with water

      • Can be given IV at a faster rate

  • Which one can be given IM?

    • Only fosphenytoin 


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35)  Valproic acid- MOA, indications, adverse effects, therapeutic level, blood test needed to be done to monitor for adverse effects. Main organ of concern.

Valpiroic acid (Depakene)

  • MOA: desensitizes Na channels

  • Indications: Wide range of seizure types like focal, generalized, absence seizures. Also used for bipolar disorder.

  • Adverse effects: limited CNS depression, visual disturbances, ataxia, vertigo, headache. Additional ones include GI effects, hepatotoxicity, pancreatitis.

  • Therapeutic level: 50-100 mcg/mL

  • Blood test needed to monitor for AEs: Monitor LFTs at 2 month intervals

  • Main organ of concern: Liver- hepatic effects dysfunction possible in first 6 months 

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36)  Lamotrigine- MOA, indications, adverse effects (main one discussed in class).

Lamotrigine (Lamictal)

  • MOA: Blocks voltage gated Na channels in the nerve cells - which are essential for generating an electrical signal.

  • Indications: Focal and generalized seizures as well as bipolar disorder for mood stabilization.

    • No need for checking therapeutic levels as toxicity is rate with this med.

  • Adverse effect (main one discussed in class)- SJS

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37) Medication used for status epilepticus- Think Benzo. See above for MOA, side effects and reversal very important!


Status epilepticus - Continuous seizure activity >5 minutes without returning to baseline, can lead to a comma or death. Considered a medical emergency.

What meds are used: Benzodiazepines like diazepam (Valium)

  • Side effects - drowsiness, dizziness, respiratory depression

  • Reversal - Flumazenil (Romazicon)

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38) Parkinson disease, what is it, sign and symptoms and goals of pharmacological therapy.

PD

  • What is it? Chronic progressive degenerative disorder that affects the dopamine-producing neurons in the brain leading to low levels of dopamine. Since dopamine and Ach work in conjunction - when dopamine levels are decreased the Ach effects increase which is what causes the symptoms as the dopamine is no longer able to regulate the Ach.

  • Signs and symptoms: Loss of muscle control, tremors, bradykinesia, rigidity, postural instability, can lead to difficulty swallowing.

  • Goals of pharmacological therapy: Try to inhibit the breakdown of dopamine.

    • Carbidopa-Levodopa - prevents breakdown of catecholamines (dopamine) in the CNS, primarily in the brain, which leads to increase in dopamine levels.

    • Amantadine (Symmetrei) - causes release of dopamine. It was initially found as an antiviral agent for influenza but was seen that it causes a release in dopamine and thus used in the early diagnosis of PD to enhance dopamine on board.

    • BOTH DRUGS = Usually effective for a short period of time



      goal is to improve QOL and extend QOL - pt to be as independent as possible for as long as possible

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39)  Benztropine (Cogentin)- MOA, indications (remember avoid in elderly), side effects (Think anticholinergic)

Benztropine (Cogentin)

  • MOA: Anticholinergic drug used in the treatment of Parkinson’s disease and also of extrapyramidal symptoms from antipsychotic drug (block action of Ach).

  • Indications (remember avoid in elderly):  help with tardive dyskinesia and extrapyramidal symptoms - automatic involuntary movements that can occur with lip smacking (these can also occur with pts that are on anti psychotics but also with pts that have PD)  

    • Not a good medication for older patients, usually for younger patients with Parkinson's

  • Side effects (Think anticholinergic) - tachycardia, confusion, disorientation, toxic psychosis, urinary retention, dry throat, constipation, nausea, and vomiting

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40)  Review nursing implications for Parkinson meds.


Nursing implication

  • Perform a thorough assessment, nursing history, and medication history.

  • Include questions about the patient’s:

    • CNS

    • GI and GU tracts

    • psychologic and emotional status

      MAKE SURE U KNOW - goal is to improve QOL and extend QOL - pt to be as independent as possible for as long as possible

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41) Antipsychotics: adverse effects


Antipsychotics - Treat psychosis delirium schizophrenia (Block dopamine receptors in the brain)

  • Side effects are:

    • Neuroleptic malignant syndrome (NMS) - mental status change, rigidity, fever, and dysautonomia (can alter BP, HR, etc)

    • Myoglobinuria - excess amount of myoglobin in the urine (can indicate damage of the cell membranes of myocytes)

    • Extrapyramidal symptoms - sx include various motion disorders similar to those seen in PD

    • Tardive dyskinesia - repetitive, involuntary movements, such as grimacing and eye blinking.

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42) Lithium: therapeutic range


It has a very narrow therapeutic range (0.6-0.12 mmol/L - in labwork) - if toxicity occurs it can cause arrhythmias, epilepsy like seizures


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43) Side effects of SSRIs


Can feel too heightened (from my notes)

Anxiety, dizziness, drowsiness, headache, mild GI disturbance, sexual dysfunction, asthenia (weakness, lack of energy and strength), tremor (from the book).

If pt is on SSRI - concerned for suicide 

  • If pt was very depressed in the past but now they have a boost of energy with SSRIs, they can now have enough energy to plan to kill themselves 

Risk for serotonin syndrome (if toxicity)

  • Increased BP, HR

  • Delirium

  • Agitation

  • Sweating

  • Myoclonus (brief involuntary twitching or jerking of a muscle)

  • Hyperreflexia

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44)  Medication to treat extrapyramidal side effects.

Anticholinergic and antihistaminergic medications - the one mentioned in class was anticholinergic

Anticholinergic drug like Benztropine (Cogentin) 

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45)  How to prevent lithium toxicity-nursing teaching interventions


Lithium is a drug used to treat bipolar disorder - old drug choice for mania. 

It works by interfering with the Na ion transport as it uses the same pathway - the exact mechanism is unclear though. But we do need to keep an eye on the Na levels. 

It has a very narrow therapeutic range (0.6-0.12 mmol/L - in labwork) - if toxicity occurs it can cause arrhythmias, epilepsy like seizures

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*MOA- mechanism of action

* in the exam both brand and generic names will be used

* Good luck studying!!!

===

From her lectures

  • NMBD - depolarizing vs non-depolarizing 

Depolarizing - succinylcholine (for short acting short procedure) is the one we use, use with rapid sequence intubation 

  • Depolarizing succinylcholine - (non competitive) works by binding with Ach receptors at neuromuscular joints - cause Na channels to open membrane depolarizes- then pt will have fascilulations- then flaccid paralysis  - prevents repolarization from happening

Non depolarizing - most common, paralyzed for longer periods

  • They will compete with acetylcholine for cholinergic receptors at neuromuscular junctions, do not depolarize the muscle

  • Prevent depolarization from happening 

  • Drugs end with -urium


  • Xanax

  • commonly used anxiolytics - used for Generalized anxiety disorder - short term relief of anxiety symptoms

  • CNS depression is a common side effect


  • Ativan

    • used for seizure activity - first line AED

    • You can also use diazepam, midazolam to stop seizure activity