Monitoring

Serum creatinine (Scr)

• Baseline
• Once weekly (more frequently if renal function changing or if concurrent nephrotoxic drugs)
• If creatinine changes (increase in Scr of ≥ 40 µmol/L, or 50% of baseline), draw vancomycin trough level to assess need for dosing change

Complete blood count with differential

• baseline
• once weekly

Peak (post) vancomycin levels are NOT RECOMMENDED

Vancomycin trough level

• Order only if patient meets inclusion criteria.

• Draw levels during daytime hours; no need to do in evening/overnight.  Avoid weekend levels if possible.

• Vancomycin trough levels should be deferred until after culture & susceptibility results are available and it is confirmed that ongoing vancomycin therapy is needed.  Early vancomycin target concentrations can be achieved with weight & renal function based dosing (see vancomycin dosing) and risk of toxicity is low with maximum of 2-3 days of empiric vancomycin therapy.

• Collect serum specimen 30 minutes or less before next dose

Pediatrics:

• first level at steady state - pre 5th dose is recommended if normal renal function; pre-3rd can be used in neonates, patients with GFR < 80mL/min/1.73m², and/or on concomitant nephrotoxins, or in patients considered at high risk of acute renal failure
• subsequent levels every 5-7 days

Adults:

• first level at steady state (see Vanco SS calculator) and after at least 2 maintenance doses (~ 30 hours if normal renal function, e.g. prior to 4th dose if q12h or prior to 5th dose if q8h)
• vancomycin clearance is enhanced in obesity. For morbidly obese patients (≥ 190% IBW or BMI ≥ 40kg/m²) consider drawing first level sooner (e.g. before 2^nd or 3^rd dose)
• subsequent levels every 7-10 days (may need more frequently if renal function changing or concurrent nephrotoxic drugs)

Intermittent hemodialysis (IHD) with high flux filters:

• Draw serum vancomycin level before 3rd maintenance dose (draw prior to/at the start of dialysis run). Subsequently, draw levels weekly for the duration of therapy. Additional levels may be ordered as clinically indicated.

Area under the curve (AUC)

• Recent US guidelines have recommended AUC (or AUC:MIC assuming MIC =1) monitoring.  In AHS, this method of monitoring is strongly discouraged because:
  • of the need for more levels, more calculations  and/or use of expensive Bayesian prediction software programs.
  • the evidence supporting AUC/MIC monitoring is generally retrospective and of low quality. 
• Numerous clinical studies have found high correlation between AUC and trough, therefore the use of the easier to use trough level method of monitoring continues to be recommended in AHS