High-dose cefepime therapy is recommended for febrile neutropenia.
Safety issues have been raised in a recent meta-analysis reporting
an increased risk of mortality during cefepime therapy. Cefepime-related
neurological toxicity has been associated with overdosing due
to severe renal dysfunction. This study aimed to investigate
the association between cefepime plasma concentrations and neurological
toxicity in febrile neutropenic patients. Cefepime trough concentrations
(by high-performance liquid chromatography) were retrospectively
analyzed for 30 adult febrile neutropenic patients receiving
the recommended high-dose regimen (6 g/day for a glomerular
filtration rate [GFR] of >50 ml/min). The dose adjustment
to renal function was evaluated by the ratio of the cefepime
daily dose per 100 ml/min of glomerular filtration. The association
between cefepime plasma concentrations and neurological toxicity
was assessed on the basis of consistent neurological symptoms
and/or signs (by NCI criteria). The median cefepime concentration
was 8.7 mg/liter (range, 2.1 to 38 mg/liter) at a median of
4 days (range, 2 to 15 days) after the start of therapy. Neurological
toxicity (altered mental status, hallucinations, or myoclonia)
was attributed to cefepime in 6/30 (20%) patients (median GFR,
45 ml/min; range, 41 to 65 ml/min) receiving a median dose of
13.2 g/day per 100 ml/min GFR (range, 9.2 to 14.3 g/day per
100 ml/min GFR). Cefepime discontinuation resulted in complete
neurological recovery for five patients and improvement for
one patient. A multivariate logistic regression model confirmed
high cefepime concentrations as an independent predictor of
neurological toxicity, with a 50% probability threshold at
22
mg/liter (
P = 0.05). High cefepime plasma concentrations are
associated with neurological toxicity in febrile neutropenic
patients with mild renal dysfunction. Careful adherence to normalized
dosing per 100 ml/min GFR is crucial. Monitoring of plasma concentrations
may contribute to preventing neurological toxicity of high-dose
therapy for this life-threatening condition.
Antimicrobial Agents and Chemotherapy, October 2010, p. 4360-4367, Vol. 54, No. 10
0066-4804/10/$12.00+0 doi:10.1128/AAC.01595-08
No comments:
Post a Comment