Generic Name

Gentamicin

Mechanism

• Inhibits Protein Synthesis by binding to the 30S ribosomal subunit, causing misreading of mRNA and premature chain termination.
• Produces a *bactericidal* effect that is both time‑dependent (microbial kill increases with drug concentration > MIC) and concentration‑dependent (higher peaks → more bacterial clearance).

> Key Point: Gentamicin’s unique property is a *post‑inhibitory effect*—bacteria continue to be killed for a period after drug levels fall below the MIC.

---

Pharmacokinetics

> Toxicity Link: Nephro‑ and ototoxicity correlate with *area‑under‑curve (AUC)* and *peak concentrations*.

--
•

Indications

• Life‑threatening infections caused by gram‑negative organisms:
• *Pseudomonas aeruginosa* (lung, bloodstream, wound)
• *Escherichia coli*, *Klebsiella*, *Proteus*, *Enterobacter* species
• Septicemia, peritonitis, osteomyelitis, meningitis (with proper CSF penetration).
• Combination therapy with β‑lactams or carbapenems for severe polymicrobial infections.
• Treatment of *Acinetobacter* species when susceptible.

---

Contraindications

• Absolute Contraindications
• Known hypersensitivity to gentamicin or other aminoglycosides.
• Pregnant women (category C) – avoid near term.
• Warnings
• *Nephrotoxicity*: dose‑dependent tubulointerstitial damage.
• *Ototoxicity*: cochlear and vestibular dysfunction, dose‑dependent.
• *Neuromuscular blockade*: potentiates neuromuscular blocking agents.
• *Cardiovascular*: may cause arrhythmias in susceptible patients.
• Precaution
• Renal impairment: use renal‑dose adjustments.

---

Dosing

• Peak Levels: 5–10 µg/mL (for serious infections).
• Trough Levels: <2 µg/mL (ideally <0.5 µg/mL for high‑risk patients).
• TDM (therapeutic drug monitoring) is mandatory to adjust dose and schedule.

--
•

Adverse Effects

• Common
• Nephrotoxicity (azotemia, proteinuria).
• Ototoxicity (tinnitus, hearing loss).
• Hypotension (rare, but possible).
• Rash or mild hypersensitivity reactions.
• Serious
• Sensorineural hearing loss (irreversible, often dose‑related).
• Vestibular symptoms: vertigo, imbalance.
• Renal failure (acute tubular necrosis).
• Neuromuscular blockade: respiratory depressant effect.
• Rash → anaphylaxis (rare).

---

Monitoring

--
•

Clinical Pearls

• Single‑Daily Dosing Is Key: Once‑daily (q24 h) dosing maximizes peak levels while allowing troughs to fall below 2 µg/mL, reducing toxicity without compromising efficacy.
• Use TDM Early: Aim to draw trough levels 30 min before the next dose on day 3–5 to avoid accumulation in renal impairment.
• Renal Index Formula:
• *Dose (mg) = 7.5 mg/kg × (CrCl/120) (for CrCl 30–120 mL/min).*
• Never forget to convert to renal dose if CrCl <30 mL/min—use a loading dose of 5 mg/kg followed by lower maintenance doses or intermittent dosing (q48 h).
• Ototoxicity Prevention: Combine gentamicin with a non‑aminoglycoside (e.g., β‑lactam) and avoid concurrent loop diuretics or other ototoxic agents.
• Nephrotoxicity Monitoring: Track serum creatinine after each dose until plateau; a ≥30% rise warrants dose readjustment or discontinuation.
• Pregnancy Note: Animal studies show fetal harm; use only if benefits outweigh risks and alternative agents are unsuitable.
• Use in Sepsis: Pair with a β‑lactam or carbapenem; avoid monotherapy in MDR gram‑negative infections unless susceptibility confirmed.

--
• References
• Tripathi K. *Goodman & Gilman’s The Pharmacological Basis of Therapeutics.* 13th ed.
• WHO Drug Information, 2024.
• American Society for Clinical Pharmacology & Therapeutics (ASCPT) guidance on aminoglycoside monitoring.