In infertile women with subclinical hypothyroidism, with or without thyroid peroxidase antibodies, serum TSH during pregnancy follows preconception values and thyroid hormones remain stable.

IF 8.3 Q1 OBSTETRICS & GYNECOLOGY
Human reproduction open Pub Date : 2023-10-09 eCollection Date: 2023-01-01 DOI:10.1093/hropen/hoad038
C De Geyter, L Matt, I De Geyter, R Moffat, C Meier
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引用次数: 0

Abstract

Study question: How does subclinical hypothyroidism, defined in infertile women during preconception by thyroid-stimulating hormone (TSH) >2.5 or >4.5 mIU/l, with or without thyroid peroxidase antibodies (anti-TPO) >100 IU/ml, impact thyroid hormone levels during pregnancy and after birth?

Summary answer: During pregnancy, TSH levels remain similar to those in preconception, even with supplementary thyroxine, whereas the serum levels of anti-TPO progressively decline.

What is known already: Overt hypothyroidism impacts both pregnancy and offspring but randomized clinical trials and cohort studies failed to detect the benefit of treatment with thyroxine in cases with low-threshold TSH or with anti-TPO during pregnancy.

Study design size duration: First, the prevalence and reproducibility of two candidate cut-off levels of subclinical hypothyroidism in a cohort of 177 infertile women was compared with 171 women not aiming for pregnancy. Second, the impact of distinct setpoints of TSH in preconception (with or without anti-TPO) was monitored during pregnancy in 87 previously infertile women by high-frequency monitoring of thyroid function. Both studies were carried out from 2007 to 2019.

Participants/materials setting methods: Reproducibility and prevalence of subclinical hypothyroidism were examined in infertile women presenting in the fertility care unit of an academic institution. Women not aiming for pregnancy participated as controls. In both groups, TSH and anti-TPO were measured two times on different occasions. In addition, a group of previously infertile women with known preconception setpoints of TSH (with or without anti-TPO) were followed up prospectively throughout pregnancy and after birth. During pregnancy, serum was sampled weekly until Week 12, then monthly until delivery, and once after birth. Only cases with preconception TSH >4.5 mIU/l were supplemented with thyroxine. After collection of all samples, the serum levels of anti-TPO and the major thyroid hormones were measured. Prolactin with known fluctuations during pregnancy was used as reference.

Main results and the role of chance: Measures of both TSH and anti-TPO at two different time points were accurate and reproducible. The odds of subclinical hypothyroidism in infertile women and controls were similar. During pregnancy, TSH closely followed preconception TSH levels, whereas serum levels of the thyroid hormones predominantly remained within or above (not below) the reference. Treatment of infertile women with preconception TSH >4.5 mIU/l with thyroxine resulted in higher free thyroxine (fT4) serum levels. The serum levels of anti-TPO declined as pregnancies evolved.

Limitations reasons for caution: The numbers of participants both in the prevalence study and in pregnancy did not reach the a priori estimated numbers. For ethical reasons, the patients with preconception TSH >4.5 mIU/l were treated with thyroxine. The findings apply to infertile women only.

Wider implications of the findings: We propose to use >4.5 mIU/l as the serum TSH threshold for supplementing women with thyroxine before pregnancy. During pregnancy, fT4 may be the better marker to monitor thyroid function. The consistent decrease of anti-TPO antibody levels during ongoing pregnancies must be considered a protective element.

Study funding/competing interests: The prevalence part of this study was supported by Merck-Serono, Geneva (TH006/EMR200007-603). The hormone measurements of the serum samples collected during the follow-up pregnancies were made possible by financial support of Roche Diagnostica (November 1721, 2017, Rotkreuz, Switzerland). I.D.G. was supported by a grant of the Repronatal Foundation, Basel, Switzerland. All authors declare no conflict of interest.

Trial registration number: Research Database of UniBasel, project no. 576691 (2007).

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在患有亚临床甲状腺功能减退症的不孕妇女中,无论是否有甲状腺过氧化物酶抗体,妊娠期血清TSH都遵循先入为主的值,甲状腺激素保持稳定。
研究问题:亚临床甲状腺功能减退症是如何在不孕妇女怀孕前通过促甲状腺激素(TSH)>2.5或>4.5 mIU/l定义的,有或没有甲状腺过氧化物酶抗体(抗TPO)>100 IU/ml,影响妊娠期和产后甲状腺激素水平?简要回答:在妊娠期间,即使补充了甲状腺素,TSH水平仍与妊娠前相似,而血清抗TPO水平逐渐下降。已知情况:显性甲状腺功能减退对妊娠和后代都有影响,但随机临床试验和队列研究未能发现在妊娠期低阈值TSH或抗TPO患者中使用甲状腺素治疗的益处。研究设计规模持续时间:首先,在177名不孕妇女和171名不打算怀孕的妇女的队列中,比较了亚临床甲状腺功能减退症两个候选临界水平的患病率和可重复性。其次,通过对甲状腺功能的高频监测,在87名既往不孕妇女的妊娠期间监测了孕前TSH的不同设定点(有或没有抗TPO)的影响。这两项研究都是在2007年至2019年进行的。参与者/材料设置方法:在一家学术机构的生育护理室检查不孕妇女的亚临床甲状腺功能减退症的再现性和患病率。不打算怀孕的妇女作为对照参加。在两组中,在不同的场合测量TSH和抗TPO两次。此外,对一组具有已知TSH预设值(含或不含抗TPO)的既往不孕妇女在整个妊娠期和出生后进行前瞻性随访。在怀孕期间,每周对血清进行采样,直到第12周,然后每月进行一次,直到分娩,并在出生后进行一次。只有在孕前TSH>4.5mIU/l的病例中才补充甲状腺素。采集所有样本后,测量血清抗TPO和主要甲状腺激素水平。妊娠期间已知波动的催乳素被用作参考。主要结果和偶然性的作用:TSH和抗TPO在两个不同时间点的测量是准确和可重复的。不孕妇女和对照组患亚临床甲状腺功能减退症的几率相似。在妊娠期间,TSH与孕前TSH水平密切相关,而血清甲状腺激素水平主要保持在参考值之内或之上(而不是低于参考值)。用甲状腺素治疗孕前TSH>4.5 mIU/l的不孕妇女可提高血清游离甲状腺素(fT4)水平。血清抗TPO水平随着妊娠的发展而下降。谨慎的局限性原因:患病率研究和妊娠期的参与者人数都没有达到先验估计的数字。出于伦理原因,先入为主TSH>4.5mIU/l的患者接受甲状腺素治疗。这一发现仅适用于不孕妇女。研究结果的更广泛含义:我们建议使用>4.5 mIU/l作为妊娠前补充甲状腺素的血清TSH阈值。在妊娠期间,fT4可能是监测甲状腺功能的更好标志物。持续妊娠期间抗TPO抗体水平的持续下降必须被视为一种保护因素。研究资金/竞争利益:本研究的流行率部分得到了Merck Serono,Geneva(TH006/ERM200007-603)的支持。在罗氏诊断公司的财政支持下(2017年11月1721日,瑞士Rotkreuz),对后续妊娠期间收集的血清样本进行了激素测量。I.D.G.得到了瑞士巴塞尔再生基金会的资助。所有作者均声明不存在利益冲突。试验注册号:巴塞尔大学研究数据库,项目编号576691(2007)。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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