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使用阿达木单抗(修美乐(®))治疗 IVF 患者免疫性不孕的女性出生缺陷率。

Birth defect rates in women using Adalimumab (Humira(®) ) to treat immunologic-based infertility in IVF patients.

机构信息

Laboratory for Reproductive Medicine and Immunology, San Francisco, CA, USA Assisted Reproduction & Gynaecology Centre, London, UK.

出版信息

Am J Reprod Immunol. 2011 Sep;66(3):237-41. doi: 10.1111/j.1600-0897.2011.00994.x. Epub 2011 Apr 19.

DOI:10.1111/j.1600-0897.2011.00994.x
PMID:21501282
Abstract

PROBLEM

This study compares the birth defect rate in women using preconception TNF-α inhibitor (Adalimumab) during an in vitro fertilization (IVF) cycle to a similar population of women not using these immunologic therapies.

METHOD OF STUDY

One hundred subfertile women aged ≤38years experienced ongoing pregnancies of which 36 resulted in twin pregnancies (136 babies). These successful cycles were divided into two different treatment groups: group I comprised 31 cycles (23 ICSI) using preconception Adalimumab (Humira) with or without pre- or post-conception intravenous immunoglobulin (IVIG) (last dose of Humira given 65.3±41.5days before embryo transfer). Group II comprised 69 cycles (58 ICSI) with no exposure to Humira or IVIG. Group I included all eligible fresh cycles containing at least five 5-celled embryos on day 3. Group II had similar entry criteria, but eligible cycles were randomly selected owing to a larger population size. Patients were later contacted by the clinic for neonatal health information.

RESULTS

Delivery outcomes were as follows: group I experienced one case of DiGeorge syndrome (chromosome 22 deletion) that was electively terminated out of 41 babies (10 sets of twins) delivered. Group II experienced one case of neonatal heart defect and another case of Edward's syndrome (Trisomy 18) out of 95 babies (26 sets of twins) delivered. The anomaly rate was 2.44% (1/41) and 2.11% (2/95) for groups I and II, respectively, comparable to the expected birth defect rate for the normal IVF population.

CONCLUSION

Preconception TNF-α inhibitor does not appear to increase the birth defect rate in women undergoing IVF. A larger, clinical trial with blinded delivery assessment is needed to confirm these safety conclusions.

摘要

问题

本研究比较了在体外受精(IVF)周期中使用 TNF-α 抑制剂(阿达木单抗)的女性与未使用这些免疫治疗药物的类似人群的出生缺陷率。

方法

100 名年龄≤38 岁的不孕女性经历了持续妊娠,其中 36 例导致双胞胎妊娠(136 例婴儿)。这些成功的周期分为两组不同的治疗组:I 组 31 个周期(23 个 ICSI),在受孕前使用阿达木单抗(修美乐),并伴有或不伴有受孕前或受孕后静脉免疫球蛋白(IVIG)(最后一次使用修美乐的时间距离胚胎移植前 65.3±41.5 天)。II 组 69 个周期(58 个 ICSI)未接触过修美乐或 IVIG。I 组包括所有符合条件的新鲜周期,这些周期在第 3 天至少有 5 个 5 细胞胚胎。II 组具有类似的纳入标准,但由于人群较大,随机选择了合格的周期。随后诊所联系了患者以获取新生儿健康信息。

结果

分娩结果如下:I 组 41 名婴儿(10 对双胞胎)中,1 例患有 DiGeorge 综合征(22 号染色体缺失),该婴儿被选择性终止妊娠。II 组 95 名婴儿(26 对双胞胎)中,1 例新生儿心脏缺陷,另 1 例爱德华氏综合征(18 三体),I 组和 II 组的异常率分别为 2.44%(1/41)和 2.11%(2/95),与正常 IVF 人群的预期出生缺陷率相当。

结论

在接受 IVF 的女性中,受孕前 TNF-α 抑制剂似乎不会增加出生缺陷率。需要进行更大的、具有盲法分娩评估的临床试验来证实这些安全性结论。

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