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NU 578 Unit 1 Study Guide (2026/2027) (PDF) | Advanced Nursing | University of South Alabama

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INSTANT PDF DOWNLOAD. This focused NU 578 Unit 1 Study Guide is designed for graduate nursing students at the University of South Alabama. It provides a clear, exam-oriented summary of key concepts and foundational material introduced in Unit 1, supporting efficient review and confident exam preparation. The guide highlights essential lecture content, reinforces understanding of core principles, and helps students identify weak areas early in the course. Ideal for structured study, unit assessments, and last-minute review. What’s included: Focused coverage of NU 578 – Unit 1 topics Key concepts and targeted exam review Clear, concise summaries aligned with course objectives High-quality, printable PDF format Immediate digital access after download Course: NU 578 – Advanced Nursing Unit: 1 Institution: University of South Alabama Format: PDF Access: Instant download NU 578 unit 1, NU 578 study guide, advanced nursing unit exam, University of South Alabama nursing, NU 578 notes, graduate nursing study guide, advanced nursing exam review, NU 578 unit notes, nursing unit study guide, NU 578 PDF download, advanced nursing notes, graduate nursing exam prep, USA nursing program, nursing coursework PDF, NU 578 exam review, advanced nursing study guide

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NU 578
Unit 1 Study Guide
Key Concepts & Exam Review
University of South Alabama.



This document provides a focused
study guide
It summarizes key concepts, lecture highlights, and
exam-relevant material to support efficient last-
minute review. The guide is structured to help students reinforce
understanding, identify weak areas, and prepare confidently for
the assessment.

, NU 578 Unit 1 Study Guide
Pharmacokinetics (PK)
 CYP450 characteristics, induction, inhibition pg 17 - 18
 CYP450 is an enzyme present in the liver that is responsible for the majority of drug
metabolism. It is a group of 12 closely related enzyme families. CYP1,2,3 metabolize
drugs while the rest metabolize endogenous compounds.
 Metabolism is defined as the enzymatic alteration of a drug structure.
 Induction
 Drugs that increase the rate of drug metabolism are called P450 inducers.
 Inducers act of the liver to stimulate enzyme synthesis. This is called the process of
induction.
 By increasing the rate of metabolism, the amount of active drug is decreased and
plasma drug levels fall. Dosing adjustments may be required to achieve a
therapeutic plasma level.
 Inhibition
 Inhibitors act on the liver through a process known as inhibition.
 By slowing the rate of metabolism, inhibition can cause an increase in active drug
accumulation. This can lead to an increase in adverse drug reactions (ADRs) and
toxicity.

 P-glycoprotein (PGP) pg 14
 Transporter of drugs out of cells, including the intestinal epithelium, placenta, BBB, liver,
and kidney tubules

 Pediatric/Infant populations and PK effects pg 18, 20
 The liver does not develop to its full capacity to metabolize drugs until around 1 year of
age. Infants are especially susceptible to injury prior to hepatic maturation.
 BBB not fully developed in infants so CNS is sensitive. Neurotoxicity is a risk.
 Plasma proteins are lower for the first year so distribution of drugs may be affected.
 Absorption may not normalize until age 2.

 Geriatric populations and PK effects pg 18, ppt
 The ability of older adults to metabolize and absorb drugs is decreased. Drug dosages
may need to be reduced to prevent toxicity.
 Distribution is affected by increase body fact and less lean body mass, decreased TBW,
and decreased serum albumin.
 Progressive decline in renal function and resulting drug accumulation is the most
common cause of ADRs in elderly.

 Effects of renal function of drug persistence in the body pg 19-20
 The kidneys account for the majority of drug excretion.
 Excretion is defined as the removal of drugs from the body.
 Drugs move from bloodstream to kidneys for excretion via active transport.
 Factors that affect renal excretion include:
 pH-dependent ionization

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