多发性硬化症孕妇使用富马酸二甲酯和纳他珠单抗的临床经验:四例患者病例系列。

IF 0.9 Q4 CLINICAL NEUROLOGY
Case Reports in Neurological Medicine Pub Date : 2024-07-16 eCollection Date: 2024-01-01 DOI:10.1155/2024/7808140
Satoshi Saito, Ryotaro Ikeguchi, Kazuo Kitagawa, Yuko Shimizu
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引用次数: 0

摘要

多发性硬化症(MS)孕妇使用β干扰素和醋酸格拉替雷被认为是相对安全的疾病修饰药物(DMD);然而,富马酸二甲酯(DMF)和纳他珠单抗(NTZ)在这一人群中的安全性仍无定论。在此,我们介绍了四例在怀孕期间接受 DMF 和 NTZ 治疗的多发性硬化症孕妇(每例 2 人),并讨论了我们对这些药物的使用和患者临床病程的观察结果。我们回顾性地检查了多发性硬化症在妊娠期间和分娩后的复发情况;接触 DMDs 的持续时间;母体、胎儿和新生儿不良事件;母乳喂养;以及恢复使用 DMDs 的时间。两名接受DMF治疗的患者在发现怀孕5周或6周后停止了治疗。产后 1 周恢复使用 DMF,并开始混合母乳喂养。一名患者在产后 9 个月进行脑磁共振成像检查时发现了新的病灶,但未被归类为临床复发。在两名接受 NTZ 治疗的患者中,用药间隔延长至发现怀孕后 6 周。一名患者在妊娠 30 周时停用了 NTZ,另一名患者在妊娠 25 周时停用了 NTZ,原因是妊娠剧吐导致胎儿生长受到轻微限制。这两名患者都选择了配方奶喂养,产后一年内均未发现复发。此外,围产期也未发现异常,发育正常。由于开展随机对照试验存在伦理限制,对孕妇和产妇用药安全性的调查主要依赖于登记、上市后监测和病例报告。我们的研究结果表明,多发性硬化症妇女在妊娠期或围产期并不禁用DMF和NTZ;然而,警惕性监测对于确保这些药物的安全性至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Clinical Experience with Dimethyl Fumarate and Natalizumab in Pregnant Women with Multiple Sclerosis: A Four-Patient Case Series.

Interferon β and glatiramer acetate are the disease-modifying drugs (DMDs) considered relatively safe for use in pregnant women with multiple sclerosis (MS); however, the safety profile of dimethyl fumarate (DMF) and natalizumab (NTZ) in this population remains inconclusive. Here, we present four cases of pregnant women with MS who were treated with DMF and NTZ (n = 2 patients, each) during their pregnancy and discuss our observations with the use of these drugs and the clinical courses of the patients. We retrospectively examined relapse of MS during pregnancy and after delivery; duration of exposure to DMDs; maternal, fetal, and neonatal adverse events; breastfeeding; and timing of resumption of DMDs. The two patients treated with DMF discontinued treatment 5 or 6 weeks after the discovery of pregnancy. DMF was resumed 1 week postpartum, and mixed breastfeeding was initiated. Brain magnetic resonance imaging in one patient 9 months after delivery revealed a new lesion; however, it was not classified as a clinical relapse. In two patients treated with NTZ, the dosing interval was extended to 6 weeks after the discovery of pregnancy. One patient discontinued NTZ at 30 weeks and the other at 25 weeks of gestation, as a slight restriction in fetal growth was observed owing to hyperemesis gravidarum. Both patients opted for formula feeding, and no relapse was observed within 1 year postpartum. Additionally, no abnormalities were observed in any of the patients during the perinatal period, and their development was normal. Investigation of drug safety in pregnant and parturient women primarily relies on registries, postmarketing surveillance, and case reports due to ethical limitations on conducting randomized controlled trials. Our findings demonstrated that DMF and NTZ were not contraindicated during pregnancy or the perinatal period in women with MS; nevertheless, vigilant monitoring is essential to ensure the safety of these drugs.

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