Flucloxacillin instantly decreases serum levels of valproic acid: A case report

IF 4.3 3区 材料科学 Q1 ENGINEERING, ELECTRICAL & ELECTRONIC
Douwe H. van der Meer, Lisa J. Elting, Pleun S. van Egmond
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Abstract

Valproic acid (VPA) is used for epilepsy and bipolar disorder. It has near-complete bioavailability and is primarily metabolized by glucuronosyltransferases and mitochondrial oxidation. This case highlights a 79-year-old male with bipolar disorder on VPA therapy that started with flucloxacillin for Staphylococcus aureus bacteraemia and exhibited significantly reduced VPA serum levels. During hospitalization, flucloxacillin treatment correlated with a sharp decline of 75% in VPA total serum levels, a novel drug–drug interaction not previously reported. Nonadherence and absorption issues of VPA were ruled out, confirming flucloxacillin's role in reducing VPA levels. Because free-fraction serum levels of VPA remained within therapeutic range (5–25 mg/L) and our patient's bipolar disorder remained stable at 1000 mg twice daily, a dose increase was not necessary. Previous reports described cytochrome P450 enzyme induction as the mechanism of flucloxacillin lowering serum levels of immunosuppressants and antimycotics. Because only 10% of VPA is metabolized by cytochrome P450 enzymes, this is not plausible for this case. The proposed mechanism for the VPA–flucloxacillin drug–drug interaction is flucloxacillin as inducer of glucuronosyltransferase enzymes via the pregnane X receptor pathway, accelerating VPA metabolism. Because this case showed that free-fraction serum levels remained within therapeutic range, it underscores the need for free-fraction VPA monitoring in bipolar disorder and flucloxacillin therapy. When VPA is used for epilepsy, it is advised to consider alternative antibiotics to avoid this interaction.

氟氯西林会瞬间降低丙戊酸的血清水平:病例报告
丙戊酸(VPA)用于治疗癫痫和躁郁症。它的生物利用度接近完全,主要通过葡萄糖醛酸转移酶和线粒体氧化作用进行代谢。本病例重点介绍了一名 79 岁的双相情感障碍男性患者在接受 VPA 治疗后,开始使用氟氯西林治疗金黄色葡萄球菌菌血症,结果显示 VPA 血清水平明显降低。住院期间,氟氯西林治疗导致 VPA 血清总水平急剧下降 75%,这是一种新的药物间相互作用,此前未曾报道过。VPA的非依从性和吸收问题已被排除,这证实了氟氯西林在降低VPA水平方面的作用。由于 VPA 的游离部分血清水平保持在治疗范围内(5-25 毫克/升),而且患者的躁郁症在每天两次、每次 1000 毫克的剂量下保持稳定,因此没有必要增加剂量。之前的报道称,细胞色素 P450 酶诱导是氟氯西林降低免疫抑制剂和抗霉菌药物血清水平的机制。由于只有 10% 的 VPA 通过细胞色素 P450 酶代谢,因此这种说法在本病例中并不成立。VPA-氟氯西林药物间相互作用的拟议机制是氟氯西林通过孕烷 X 受体途径诱导葡萄糖醛酸转移酶,加速 VPA 的代谢。由于该病例显示游离部分血清水平仍在治疗范围内,因此强调了在双相情感障碍和氟氯西林治疗中监测游离部分VPA的必要性。在使用 VPA 治疗癫痫时,建议考虑使用其他抗生素来避免这种相互作用。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
7.20
自引率
4.30%
发文量
567
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