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Reg Anesth Pain Med · Mar 2003
Case ReportsCentral nervous system toxicity following the administration of levobupivacaine for lumbar plexus block: A report of two cases.
- Dara S Breslin, Gavin Martin, David B Macleod, Francine D'ercole, and Stuart A Grant.
- Department of Anesthesiology, Duke University Medical Center, Durham, NC, USA. bres1002@mc.duke.edu
- Reg Anesth Pain Med. 2003 Mar 1;28(2):144-7.
Background And ObjectivesCentral nervous system and cardiac toxicity following the administration of local anesthetics is a recognized complication of regional anesthesia. Levobupivacaine, the pure S(-) enantiomer of bupivacaine, was developed to improve the cardiac safety profile of bupivacaine. We describe 2 cases of grand mal seizures following accidental intravascular injection of levobupivacaine.Case ReportTwo patients presenting for elective orthopedic surgery of the lower limb underwent blockade of the lumbar plexus via the posterior approach. Immediately after the administration of levobupivacaine 0.5% with epinephrine 2.5 microgram/mL, the patients developed grand mal seizures, despite negative aspiration for blood and no clinical signs of intravenous epinephrine administration. The seizures were successfully treated with sodium thiopental in addition to succinylcholine in 1 patient. Neither patient developed signs of cardiovascular toxicity. Both patients were treated preoperatively with beta-adrenergic antagonist medications, which may have masked the cardiovascular signs of the unintentional intravascular administration of levobupivacaine with epinephrine.ConclusionsAlthough levobupivacaine may have a safer cardiac toxicity profile than racemic bupivacaine, if adequate amounts of levobupivacaine reach the circulation, it will result in convulsions. Plasma concentrations sufficient to result in central nervous system toxicity did not produce manifestations of cardiac toxicity in these 2 patients.
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