NR565 / NR 565 Advanced Pharmacology Care of the Fundamentals Midterm Exam | Chamberlain University (2026/2027) | Verified Questions and Answers with Rationales | Get HighScore | Instant Download

GET HIGHSCORE on the NR565 Advanced Pharmacology Care of the Fundamentals Midterm Exam (Weeks 1-4) at Chamberlain University with this comprehensive test bank featuring verified questions and answers with detailed rationales. The NR565 midterm exam is non-cumulative, consisting of 100 multiple-choice questions with a 120-minute time allotment (1.2 minutes per question), covering content from Weeks 1 through 4 of the course . The exam will be available from Wednesday of Week 4 at 12:01 am MT until Saturday of Week 4 at 11:59 pm MT . This resource covers the four key content areas: Week 1 (Foundations in Pharmacology), Week 2 (Pharmacotherapy for Cardiovascular Conditions), Week 3 (Pharmacotherapy for Pain), and Week 4 (Pharmacotherapy for Musculoskeletal and Rheumatologic Conditions) . MASTER FOUNDATIONS IN PHARMACOLOGY (WEEK 1 - CHAPTERS 1-10) Pharmacokinetics (What the Body Does to the Drug) : The study of drug movement from administration until elimination, consisting of four phases: Absorption (how drug enters bloodstream - IV gives 100% bioavailability, oral drugs experience first-pass effect in liver), Distribution (how drug spreads to tissues - influenced by protein binding, blood flow, and body composition), Metabolism (biotransformation primarily in liver via CYP450 enzymes), and Excretion (elimination primarily via kidneys) . First-Pass Effect: The initial metabolism of an orally administered drug in the liver before reaching systemic circulation. Drugs administered via parenteral routes (IV, IM, SubQ) bypass first-pass effect and are 100% bioavailable . Half-Life: The time required for half of a drug to be eliminated from the body . Steady State: The point at which the amount of drug going into the body equals the amount being eliminated . Loading Dose vs Maintenance Dose: Loading doses rapidly achieve therapeutic levels; maintenance doses sustain therapeutic levels over time . Pharmacodynamics (What the Drug Does to the Body) : The study of drug mechanisms of action, including three primary mechanisms: Receptor interactions (agonists activate receptors, antagonists block receptors), Enzyme interactions (drugs enhance or inhibit enzyme activity), and Nonselective interactions (drugs chemically alter cellular structures, such as chemotherapy) . Efficacy: The maximal response a drug can produce; high-efficacy agonists produce maximum response while occupying a relatively low proportion of receptors . Potency: The amount of drug required to produce a given effect (related to dose, not clinical effectiveness). Therapeutic Index: The ratio between toxic and therapeutic doses; narrow therapeutic index drugs require monitoring . CYP450 Enzyme System: Critical for drug metabolism; variations affect drug levels and response . CYP450 Inhibitors: Medications that slow metabolism of other drugs, potentially leading to toxicity. Examples include Valproate, Isoniazid, Sulfonamides, Amiodarone, Chloramphenicol, Ketoconazole, Grapefruit juice, Quinidine (mnemonic: VISACKGQ) . CYP450 Inducers: Medications that accelerate metabolism of other drugs, potentially reducing effectiveness. Examples include Carbamazepine, Rifampin, Alcohol, Phenytoin, Griseofulvin, Phenobarbital, Sulfonylureas (mnemonic: CRAPGPS) . Poor Metabolizer Phenotype: Occurs when both alleles of CYP2D or CYP2C19 carry inactivating mutations. Medications are metabolized slower, leading to increased risk of side effects or therapeutic failure . Drug Interactions : Additive: Combined effect equals sum of individual effects. Synergistic: Combined effect is greater than sum of individual effects (e.g., lisinopril + HCTZ for hypertension) . Antagonistic: Combined effect is less than desired effect of one or both drugs (e.g., antacids reducing absorption of thyroid medications or antibiotics) . Grapefruit Juice Interaction: Decreases metabolism of several drugs including buspirone, nifedipine, and statins . Warfarin Interaction: Leafy dark greens (containing Vitamin K) counter the anticoagulant effect of warfarin . Prescriptive Authority and Legal Considerations : Practice Authority refers to the NP's ability to practice without physician oversight, whereas Prescriptive Authority refers to the NP's authority to prescribe medications independently . Prescriptive authority is regulated by state health professional boards (Nursing, Medicine, or Pharmacy) as determined by each state . Full Practice Authority: NPs have autonomy to evaluate, diagnose, order/interpret tests, initiate treatments, and prescribe medications including controlled substances without physician oversight . Reduced Practice Authority: NPs are limited in at least one element; state requires formal collaborative agreement (e.g., physician involvement for 5 years before independent practice) . Restricted Practice Authority: NPs require supervision, delegation, or team management by an outside health discipline (typically physician on site) . Limited prescriptive authority creates barriers to quality, affordable, and accessible patient care including longer wait times and restricted outreach to rural areas . Prescribing Considerations and Responsibilities : Key considerations include: documented provider-patient relationship, thorough history and physical, discussions of risks/side effects, drug monitoring/titration plan, avoidance of prescribing for self/family/friends, and consideration of cost, guidelines, interactions, allergies, hepatic/renal function, and special populations . The FDA regulates whether drugs are safe and effective for proposed use and whether benefits outweigh risks . Eight Rights of Medication Administration: Right Patient, Right Medication, Right Dose, Right Route, Right Time, Right Reason, Right Response, Right Documentation . Medication Non-Adherence: Factors include multiple chronic disorders, multiple prescriptions, multiple daily doses, difficult packaging, multiple prescribers, regimen changes, cognitive/physical impairment, living alone, recent hospital discharge, low literacy, inability to pay, and side effects . Special Populations - Geriatrics : Pharmacokinetic Changes in Older Adults: Increased gastric pH, decreased absorptive surface area, decreased splanchnic blood flow, decreased GI motility, delayed gastric emptying (absorption); increased body fat, decreased lean body mass, decreased total body water, decreased serum albumin, decreased cardiac output (distribution); decreased renal blood flow, decreased GFR, decreased tubular secretion, decreased number of nephrons (excretion) . Beers Criteria: Guidelines updated annually to help prescribers avoid medications that are or can be harmful to older adults; applicable in all healthcare settings except hospice and palliative care . Polypharmacy: Greatly increases risk for interactions, some with life-threatening consequences. Crucial to ask patients about all drugs including OTC and herbal preparations . Special Populations - Pediatrics : Neonates have slow and erratic IM absorption due to low blood flow in muscles first few days of life . Delayed gastric emptying in infancy increases oral drug absorption . Medications to avoid in pediatric patients: glucocorticoids, tetracyclines (tooth discoloration), sulfonamides (kernicterus), fluoroquinolones, aspirin (severe intoxication risk from acute overdose) . Neonate and infant drug dosing is based on weight or body surface area (BSA) . Transdermal absorption is more rapid and complete in infants due to thin skin and great blood flow . Special Populations - Pregnancy : Physiological changes during pregnancy that impact pharmacokinetics: increased glomerular filtration rate (increased drug excretion), increased hepatic metabolism, decreased tone and motility of bowel (increased drug absorption) . Examples of teratogenic medications: antiepileptic drugs, tetracyclines, fluoroquinolones, large doses of Vitamin A, some anticoagulants, and diethylstilbestrol (DES) . MASTER PHARMACOTHERAPY FOR CARDIOVASCULAR CONDITIONS (WEEK 2) Hypertension Management : Antihypertensive drug classes: ACE inhibitors, ARBs, beta-blockers (cardioselective vs non-selective), calcium channel blockers (dihydropyridine vs non-dihydropyridine), diuretics (loop, thiazide, potassium-sparing) . ACE inhibitors and ARBs are preferred in patients with CKD or heart failure . ACE inhibitors and ARBs are contraindicated in pregnancy due to teratogenic effects . Heart Failure Pharmacotherapy : Medications include: ACE inhibitors, ARBs, beta-blockers, diuretics, digoxin, sacubitril/valsartan, spironolactone . Digoxin: Cardiac glycoside that increases myocardial contractility; reduces symptoms and hospitalizations in HF but does NOT prolong life. Benefits derive from increased contractility and neurohormonal effects . Hyperlipidemia Management : Statins: First-line lipid-lowering therapy; can be prescribed for patients 10 years old . ASCVD Risk Score: Used under 2018 ACC/AHA guidelines to determine patient's absolute risk for developing clinical coronary disease over the next 10 years. Mode of intervention is determined by individual's degree of risk . Ezetimibe (Zetia) : Non-statin lipid-lowering agent that inhibits cholesterol absorption in the small intestine . Anticoagulation Management : Warfarin: Anticoagulant requiring INR monitoring (target range 2-3 for most indications) . DOACs (Direct Oral Anticoagulants): Apixaban, rivaroxaban, dabigatran, edoxaban . Quinidine and Digoxin Interaction: Quinidine can double digoxin levels by displacing digoxin from plasma albumin and decreasing elimination