University of California San Francisco, San Francisco, California, USA.
Janssen Research and Development, LLC, Raritan, New Jersey, USA.
Aliment Pharmacol Ther. 2022 Aug;56(3):477-490. doi: 10.1111/apt.16960. Epub 2022 May 12.
Ustekinumab, a human immunoglobulin G1 monoclonal antibody that binds to and inhibits interleukin (IL)-12/IL-23, is indicated for multiple immune-mediated diseases. Ustekinumab is actively transported across the placenta and theoretically could impact pregnancy outcomes. Limited data on pregnancy outcomes with ustekinumab exposure are available.
To assess pregnancy outcomes in patients exposed to ustekinumab during pregnancy METHODS: Cumulative data on medically confirmed ustekinumab-exposed pregnancies from the manufacturer's Global Safety Database were summarised. Descriptive data for pregnancy outcomes were presented overall and by patient subgroups.
As of 31 August 2020, 408 medically confirmed, prospective, maternal ustekinumab-exposed pregnancies with reported outcomes were identified. The mean maternal age was 31 years. Of the 420 pregnancy outcomes (including 4 sets of twins), 340 (81%) were live births, 51 (12.1%) spontaneous abortions, 25 (6%) elective/induced abortions, 3 (0.7%) stillbirths and 1 (0.2%) ongoing pregnancy with foetal congenital anomaly (CA). Among 340 live births, 33 (9.7%) were born pre-term. The rate of major CAs was similar by indication (Crohn's disease vs psoriasis), ustekinumab dose (45 mg vs 90 mg) and timing and duration of maternal exposure to ustekinumab. Prospective outcomes of pregnancies with paternal periconceptional ustekinumab exposure (n = 87) included 92% live births (1.2% major CA), 5.7% spontaneous abortions and 2.3% elective/induced abortions.
Rates of adverse pregnancy outcomes or CAs with ustekinumab exposure were consistent with rates reported for the US general population and do not suggest a higher risk associated with maternal or paternal exposure to ustekinumab.
乌司奴单抗是一种人免疫球蛋白 G1 单克隆抗体,可与白细胞介素(IL)-12/IL-23 结合并抑制其活性,适用于多种免疫介导的疾病。乌司奴单抗可被主动转运至胎盘,并可能对妊娠结局产生影响。目前仅有有限的乌司奴单抗暴露相关妊娠结局数据。
评估妊娠期间暴露于乌司奴单抗的患者的妊娠结局。
对来自制造商全球安全数据库的已确诊的、前瞻性的、暴露于乌司奴单抗的妊娠病例数据进行汇总。对妊娠结局的描述性数据进行了总体呈现,并根据患者亚组进行了呈现。
截至 2020 年 8 月 31 日,共确定了 408 例已确诊、前瞻性、母亲暴露于乌司奴单抗且报告结局的妊娠病例。母亲的平均年龄为 31 岁。在 420 例妊娠结局(包括 4 组双胞胎)中,340 例(81%)为活产,51 例(12.1%)为自然流产,25 例(6%)为选择性/人工流产,3 例(0.7%)为死胎,1 例(0.2%)为继续妊娠且胎儿存在先天性异常(CA)。在 340 例活产中,33 例(9.7%)为早产。按适应证(克罗恩病 vs 银屑病)、乌司奴单抗剂量(45mg vs 90mg)以及母亲暴露于乌司奴单抗的时间和持续时间,主要 CA 的发生率相似。父亲在受孕前接触乌司奴单抗的妊娠病例(n=87)的结局包括 92%的活产(1.2%存在主要 CA)、5.7%的自然流产和 2.3%的选择性/人工流产。
乌司奴单抗暴露与不良妊娠结局或 CA 发生率与美国一般人群的报告一致,并不提示与母亲或父亲暴露于乌司奴单抗相关的风险增加。
