Weisskopf Etienne, Guidi Monia, Fischer Céline J, Bickle Graz Myriam, Beaufils Etienne, Nguyen Kim An, Morisod Harari Mathilde, Rouiller Sylvie, Rothenburger Sophie, Gaucherand Pascal, Kassai-Koupai Behrouz, Borradori Tolsa Cristina, Epiney Manuella, Tolsa Jean-François, Vial Yvan, Hascoët Jean-Michel, Claris Olivier, Eap Chin B, Panchaud Alice, Csajka Chantal
Center for Research and Innovation in Clinical Pharmaceutical Sciences, Institute of Pharmaceutical Sciences of Western Switzerland, Lausanne University Hospital and University of Lausanne, University of Geneva, Switzerland.
Service of Clinical Pharmacology, Lausanne University Hospital, Lausanne, Switzerland.
Br J Clin Pharmacol. 2020 Aug;86(8):1642-1653. doi: 10.1111/bcp.14278. Epub 2020 Apr 14.
Escitalopram (SCIT) is frequently prescribed to breastfeeding women. Available information on SCIT excretion into breast milk is based on heterogeneous and incomplete data. A population pharmacokinetic model that aimed to better characterize maternal and infant exposure to SCIT and its metabolite was developed.
The study population was composed of women treated by SCIT or racemic citalopram and enrolled in the multicenter prospective cohort study SSRI-Breast Milk study (ClinicalTrial.gov NCT01796132). A joint structural model was first built for SCIT and S-desmethylcitalopram (SDCIT) in plasma using NONMEM and the milk-to-plasma ratio (MPR) was estimated by adding the drug breast milk concentrations. The effect of different influential covariates was tested and the average drug exposure with variability through breastfeeding was predicted under various conditions by simulation.
The study enrolled 33 patients treated with SCIT or racemic citalopram who provided 80 blood and 104 milk samples. Mean MPR for both parent drug and metabolite was 1.9. Increased milk fat content was significantly associated with an increased drug transfer into breast milk (+28% for SCIT and +18% for SDCIT when fat amount doubles from 3.1 to 6.2 g/100 mL). Simulations suggested that an exclusively breastfed infant would ingest daily through breast milk 3.3% of the weight-adjusted maternal SCIT dose on average.
The moderate between-subject variability in milk concentration of SCIT and the limited exposure to escitalopram through breast milk observed provide reassurance for treated mothers of breastfed healthy infants.
艾司西酞普兰(SCIT)常用于哺乳期妇女。目前关于SCIT在母乳中排泄的信息基于异质性且不完整的数据。因此,构建了一个群体药代动力学模型,旨在更好地表征母体和婴儿对SCIT及其代谢物的暴露情况。
研究人群由接受SCIT或消旋西酞普兰治疗的女性组成,她们参与了多中心前瞻性队列研究“SSRI-母乳研究”(ClinicalTrial.gov标识符:NCT01796132)。首先使用NONMEM为血浆中的SCIT和S-去甲基西酞普兰(SDCIT)建立联合结构模型,并通过添加药物母乳浓度来估算母乳与血浆的比率(MPR)。测试了不同影响协变量的作用,并通过模拟预测了在各种条件下母乳喂养期间药物暴露的平均值及其变异性。
该研究纳入了33例接受SCIT或消旋西酞普兰治疗的患者,他们提供了80份血液样本和104份母乳样本。母体药物及其代谢物的平均MPR为1.9。母乳脂肪含量增加与药物向母乳中的转移增加显著相关(当脂肪含量从3.1 g/100 mL增加一倍至6.2 g/100 mL时,SCIT增加28%,SDCIT增加18%)。模拟结果表明,纯母乳喂养的婴儿平均每天通过母乳摄入的母体SCIT剂量按体重调整后为3.3%。
观察到SCIT在母乳中的浓度个体间变异性中等,且通过母乳接触艾司西酞普兰的量有限,这为接受治疗的母乳喂养健康婴儿的母亲提供了安心保障。