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NR 601 Antimicrobial Therapy & Antihelminthics Reviewer

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Antimicrobial Therapy & Antihelminthics Reviewer Reference: Rosenthal & Burchum, 2026; CDC, 2024 o Five generations; increasing gram- Chapter 72: Basic Principles of Antimicrobial Therapy • Selective Toxicity = ability of drug to kill/inhibit microbes without harming host. • Classification: o By susceptible organism: antibacterial, antifungal, antiviral. o By MOA: inhibit cell wall synthesis, protein synthesis, nucleic acids, etc. • Bactericidal vs. Bacteriostatic: o Cidal → kills bacteria. o Static → slows growth, relies on host immunity. • Resistance: o Microbe may ↓ drug uptake, ↑ drug inactivation, alter drug target sites, or pump drug out (efflux). o Big issue: MRSA, VRE, multidrug- resistant TB. • Superinfection: o New infection during treatment of another. Example: C. difficile after broad-spectrum antibiotics. • Prophylaxis: o Given to prevent infection (e.g., before surgery, recurrent UTIs, immunocompromised pts). Chapter 73: Penicillins (PCNs) • MOA: Weaken bacterial cell wall → lysis. • Bactericidal, time-dependent. • Resistance: Beta-lactamase production, altered PBPs (penicillin-binding proteins). • Types: o Narrow-spectrum PCN G, V (strep, syphilis). o Broad-spectrum aminopenicillins (amoxicillin, ampicillin). o Antistaphylococcal (nafcillin, oxacillin, dicloxacillin). o Antipseudomonal (piperacillin/tazobactam). • Allergy: Rashes → anaphylaxis. Cross- reactivity with cephalosporins. Chapter 74: Other Cell Wall Drugs • Cephalosporins: negative activity and beta- lactamase resistance. o 1st gen (cefazolin) → staph/strep. o 3rd gen (ceftriaxone) → meningitis, gonorrhea. o 5th gen (ceftaroline) → MRSA. • Carbapenems (imipenem): Ultra broad spectrum, resistant to most beta-lactamases. • Vancomycin: o Not a beta-lactam, but inhibits cell wall synthesis. o Used for MRSA, C. diff (oral). o Risks: nephrotoxicity, ototoxicity, “red man syndrome.” Chapter 75: Bacteriostatic Inhibitors of Protein Synthesis • Tetracyclines (doxycycline): Broad spectrum, used for acne, atypicals (chlamydia, Lyme). o Risks: teeth discoloration (avoid <8 yrs), photosensitivity, GI upset. • Macrolides (azithromycin, erythromycin): o Used for strep throat in PCN allergy, atypical pneumonia. o Risks: QT prolongation, GI upset, CYP3A4 interactions. • Clindamycin: o Effective for anaerobes. o High risk of C. diff infection

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, Antimicrobial Therapy & Antihelminthics Reviewer
Reference: Rosenthal & Burchum, 2026; CDC, 2024
o Five generations; increasing gram-
Chapter 72: Basic Principles of negative activity and beta-
lactamase resistance.
Antimicrobial Therapy
o 1st gen (cefazolin) → staph/strep.
• Selective Toxicity = ability of drug to
kill/inhibit microbes without harming o 3rd gen (ceftriaxone) →
host. meningitis, gonorrhea.
• Classification: o 5th gen (ceftaroline) → MRSA.
o By susceptible organism: • Carbapenems (imipenem): Ultra broad
antibacterial, antifungal, antiviral. spectrum, resistant to most beta-
o By MOA: inhibit cell wall lactamases.
synthesis, protein synthesis, nucleic • Vancomycin:
acids, etc. o Not a beta-lactam, but inhibits cell
• Bactericidal vs. Bacteriostatic: wall synthesis.
o Cidal → kills bacteria. o Used for MRSA, C. diff (oral).
o Static → slows growth, relies on o Risks: nephrotoxicity, ototoxicity,
host immunity. “red man syndrome.”
• Resistance:
o Microbe may ↓ drug uptake, ↑ drug Chapter 75: Bacteriostatic Inhibitors of
inactivation, alter drug target sites, Protein Synthesis
or pump drug out (efflux). • Tetracyclines (doxycycline): Broad
o Big issue: MRSA, VRE, spectrum, used for acne, atypicals
multidrug- resistant TB. (chlamydia, Lyme).
• Superinfection: o Risks: teeth discoloration (avoid <8
o New infection during treatment of yrs), photosensitivity, GI upset.
another. Example: C. difficile • Macrolides (azithromycin,
after broad-spectrum antibiotics. erythromycin):
• Prophylaxis: o Used for strep throat in PCN
o Given to prevent infection allergy, atypical pneumonia.
(e.g., before surgery, recurrent o Risks: QT prolongation, GI upset,
UTIs, CYP3A4 interactions.
immunocompromised pts). • Clindamycin:
o Effective for anaerobes.
Chapter 73: Penicillins (PCNs) o High risk of C. diff infection.
• MOA: Weaken bacterial cell wall → lysis.
• Bactericidal, time-dependent. Chapter 76: Aminoglycosides (Bactericidal
• Resistance: Beta-lactamase production,
altered PBPs (penicillin-binding proteins).
Protein Synthesis Inhibitors)
• Gentamicin, Amikacin, Tobramycin.
• Types:
• MOA: Cause misreading of mRNA →
o Narrow-spectrum PCN G, V
defective proteins → bacterial death.
(strep, syphilis).
• Uses: Serious gram-negative infections.
o Broad-spectrum aminopenicillins
• Risks: Ototoxicity, nephrotoxicity,
(amoxicillin, ampicillin). neuromuscular blockade.
o Antistaphylococcal • Monitor drug levels (narrow therapeutic
(nafcillin, oxacillin, index).
dicloxacillin).
o Antipseudomonal
(piperacillin/tazobactam). Chapter 77: Sulfonamides & Trimethoprim
• Allergy: Rashes → anaphylaxis. Cross- • MOA: Inhibit folic acid synthesis
reactivity with cephalosporins. (bacteria need to make their own).


Chapter 74: Other Cell Wall Drugs
• Cephalosporins:

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