Weinstock-Guttman Bianca, Ross Amy Perrin, Planton Jonathan, White Kurt, Pandhi Avni, Greco Andres, Kumar Achint, Everage Nicholas, Vignos Megan
Jacobs School of Medicine and Biomedical Sciences, University of Buffalo, 1010 Main St, 2nd floor, Buffalo, NY, 14202, USA.
Loyola University Chicago, Chicago, IL, USA.
Drugs Real World Outcomes. 2023 Dec;10(4):503-511. doi: 10.1007/s40801-023-00384-0. Epub 2023 Sep 22.
There is a lack of well-controlled US studies of intramuscular (IM) interferon beta (IFNβ)-1a use in pregnant women with multiple sclerosis; however, in the European Medicines Agency region, IFNβ formulations may be considered during pregnancy if clinically needed based on data from European Union cohort registries. The AVONEX Pregnancy Exposure Registry was established to prospectively study the effects of IM IFNβ-1a on the risk of birth defects and spontaneous pregnancy loss in a US population.
Pregnant women with multiple sclerosis exposed to IM IFNβ-1a within ~ 1 week of conception or during the first trimester were included. Participants were followed until there was a pregnancy outcome, live-born infants were followed until age 8-12 weeks. Data were collected on IM IFNβ-1a exposure, demographics, patient characteristics, medical history, and pregnancy outcomes, including live births (with or without birth defect), spontaneous abortions/miscarriages and fetal death/stillbirth, elective abortions (with and without birth defect), and ectopic pregnancies. A population-based birth defect surveillance program, the Metropolitan Atlanta Congenital Defects Program (MACDP), served as the primary external control group for evaluating the risk of birth defects.
Three-hundred and two patients with a median (range) age of 31.0 (16-48) years and a median (range) gestational age at the time of enrollment of 10.1 (4-39) weeks were evaluable. Most patients (n = 278/302; 92%) reported IM IFNβ-1a exposure in the week before conception and most (n = 293/302; 97%) discontinued treatment before the end of the first trimester. Of 306 pregnancy outcomes, there were 272 live births, 28 spontaneous abortions of 266 pregnancies enrolled before 22 weeks' gestation (rate 10.5%; 95% confidence interval 7.2-15.0), five elective abortions, and one stillbirth. There were 17 adjudicator-confirmed major birth defects of 272 live births (rate 6.3%; 95% confidence interval 3.8-10.0); the pattern of birth defects observed was not suggestive of a relationship to prenatal IM IFNβ-1a exposure.
This large US registry study suggests IM IFNβ-1a exposure during early pregnancy was not clinically associated with adverse pregnancy outcomes in women with multiple sclerosis. These findings help inform clinicians and patients in weighing the risks and benefits of IM IFNβ-1a use during pregnancy.
ClinicalTrials.gov: NCT00168714, 15 September, 2005.
在美国,缺乏对患有多发性硬化症的孕妇使用肌内注射(IM)干扰素β(IFNβ)-1a的严格对照研究;然而,在欧洲药品管理局辖区,如果根据欧盟队列登记的数据在临床上有需要,妊娠期间可考虑使用IFNβ制剂。建立了AVONEX妊娠暴露登记处,以前瞻性研究IM IFNβ-1a对美国人群出生缺陷风险和自然流产的影响。
纳入在受孕前约1周内或孕早期接触过IM IFNβ-1a的患有多发性硬化症的孕妇。对参与者进行随访直至有妊娠结局,对活产婴儿随访至8 - 12周龄。收集有关IM IFNβ-1a暴露、人口统计学、患者特征、病史和妊娠结局的数据,包括活产(有或无出生缺陷)、自然流产/流产和胎儿死亡/死产、选择性流产(有和无出生缺陷)以及宫外孕。一个基于人群的出生缺陷监测项目,即大亚特兰大先天性缺陷项目(MACDP),作为评估出生缺陷风险的主要外部对照组。
302例患者可进行评估,年龄中位数(范围)为31.0(16 - 48)岁,入组时孕周中位数(范围)为10.1(4 - 39)周。大多数患者(n = 278/302;92%)报告在受孕前一周接触过IM IFNβ-1a,大多数(n = 293/302;97%)在孕早期结束前停止治疗。在306例妊娠结局中,有272例活产,266例在妊娠22周前入组的妊娠中有28例自然流产(发生率10.5%;95%置信区间7.2 - 15.0),5例选择性流产,1例死产。272例活产中有17例经判定确认的主要出生缺陷(发生率6.3%;95%置信区间3.8 - 10.0);观察到的出生缺陷模式未提示与产前IM IFNβ-1a暴露有关。
这项大型美国登记研究表明,妊娠早期接触IM IFNβ-1a与患有多发性硬化症的女性的不良妊娠结局在临床上无关联。这些发现有助于临床医生和患者权衡妊娠期间使用IM IFNβ-1a的风险和益处。
ClinicalTrials.gov:NCT00168714,2005年9月15日。
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