L-carnitine does not improve valproic acid poisoning management: a cohort study with toxicokinetics and concentration/effect relationships

Philippe Nguyen; Lucie Chevillard; Ahmed S Gouda; Hervé Gourlain; Laurence Labat; Isabelle Malissin; Nicolas Deye; Sebastian Voicu; Bruno Mégarbane

doi:10.1186/s13613-022-00984-z

L-carnitine does not improve valproic acid poisoning management: a cohort study with toxicokinetics and concentration/effect relationships

Ann Intensive Care. 2022 Jan 29;12(1):7. doi: 10.1186/s13613-022-00984-z.

Authors

Philippe Nguyen¹, Lucie Chevillard², Ahmed S Gouda^{1

3}, Hervé Gourlain⁴, Laurence Labat⁴, Isabelle Malissin^{1

2}, Nicolas Deye¹, Sebastian Voicu^{1

2}, Bruno Mégarbane^{5

6}

Affiliations

¹ Department of Medical and Toxicological Critical Care, Federation of Toxicology APHP, Lariboisière Hospital, 2 Rue Ambroise Paré, 75010, Paris, France.
² University of Paris, Inserm UMRS-1144, Paris, France.
³ National Egyptian Center for Toxicological Researches, Faculty of Medicine, Cairo University, Cairo, Egypt.
⁴ Laboratory of Toxicology, Lariboisière Hospital, Paris, France.
⁵ Department of Medical and Toxicological Critical Care, Federation of Toxicology APHP, Lariboisière Hospital, 2 Rue Ambroise Paré, 75010, Paris, France. bruno.megarbane@lrb.aphp.fr.
⁶ University of Paris, Inserm UMRS-1144, Paris, France. bruno.megarbane@lrb.aphp.fr.

Abstract

Background: Valproic acid (VPA) poisoning is responsible for life-threatening neurological and metabolic impairments. Despite only low-level evidence of effectiveness, L-carnitine has been used for years to prevent or reverse VPA-related toxicity. We aimed to evaluate the effects of L-carnitine used to treat acute VPA poisoning on the time-course of plasma VPA concentrations and VPA-related toxicity. We designed a single-center cohort study including all VPA-poisoned patients admitted to the intensive care unit. We studied VPA toxicokinetics using a nonlinear mixed-effects model-based population approach and modeled individual plasma VPA/blood lactate concentration relationships. Then, we evaluated L-carnitine-attributed effects by comparing VPA elimination half-lives and time-courses of blood lactate levels and organ dysfunction [assessed by the Sequential Organ Failure Assessment (SOFA) score] between matched L-carnitine-treated and non-treated patients using a multivariate analysis including a propensity score.

Results: Sixty-nine VPA-poisoned patients (40F/29 M; age, 41 years [32-47]) (median [25th-75th percentiles]; SOFA score, 4 [1-6]) were included. The presumed VPA ingested dose was 15 g [10-32]. Plasma VPA concentration on admission was 231 mg/L [147-415]. The most common manifestations were coma (70%), hyperlactatemia (3.9 mmol/L [2.7-4.9]) and hyperammonemia (127 mmol/L [92-159]). VPA toxicokinetics well fitted a one-compartment linear model with a mean elimination half-life of 22.9 h (coefficient of variation, 28.1%). Plasma VPA (C)/blood lactate concentration (E) relationships were well described by an exponential growth equation [[Formula: see text]; with baseline E₀ = 1.3 mmol/L (43.9%) and rate constant of the effect, k = 0.003 L/mg (59.5%)]. Based on a multivariate analysis, peak blood lactate concentration was the only factor independently associated with L-carnitine administration (odds ratio, 1.9, 95% confidence interval, 1.2-2.8; P = 0.004). We found no significant contribution of L-carnitine to enhancing VPA elimination, accelerating blood lactate level normalization and/or preventing organ dysfunction.

Conclusions: VPA poisoning results in severe toxicity. While L-carnitine does not contribute to enhancing VPA clearance, its impact on accelerating blood lactate level normalization and/or preventing organ dysfunction remains uncertain. Investigating VPA toxicokinetics and concentration/effect relationships may help understanding how to improve VPA-poisoned patient management.

Keywords: Antidote; L-carnitine; Lactate; Pharmacokinetics; Poisoning; Valproic acid.