早产新生儿迟发性促甲状腺激素升高:多重筛查样本的价值和详细的临床特征。

IF 6.7 1区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Thyroid Pub Date : 2025-07-01 Epub Date: 2025-06-11 DOI:10.1089/thy.2025.0051
Emese Boros, Lionel Marcelis, Claudine Heinrichs, Vinciane Vlieghe, Marwa Abdoulmoula, Guy Van Vliet, Cécile Brachet
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引用次数: 0

摘要

背景:自20世纪70年代以来,高收入国家一直在实施先天性甲状腺功能减退症(CH)的新生儿筛查,以预防智力残疾。促甲状腺激素(TSH)延迟上升与正常TSH在第一个干血点(DBS)样本,随后异常TSH在随后的DBS,有时在早产新生儿中观察到。早产儿永久性CH的发病率和筛查过程仍存在争议。我们的目的是评估早产儿短暂性和永久性CH以及延迟性TSH升高的发生率。讨论了多重筛选样本的效用。方法:我们对早产新生儿进行回顾性研究(结果:在纳入研究的3578名早产新生儿中,10名被诊断为CH(0.3%)。大多数CH病例是短暂性的(10例中有6例短暂性,1例死亡,1例持续服用l -甲状腺素,年龄太小,无法尝试断奶)。在第一次星展检查中发现6例,在随后的星展检查中发现4例。只有2例确诊为永久性CH, 1789年早产儿永久性CH的发生率为1例(0.05%)。其中一人的TSH上升延迟。基因检测有助于建立永久性CH原位腺体的诊断。结论:永久性CH在早产新生儿中似乎比短暂性CH更罕见(1/1789 vs 1/596)。在碘暴露或甲状腺超声显示原位腺阴性基因检测和缺乏母体阻断抗体的情况下,可怀疑短暂性CH。在这种情况下,早期停用左旋甲状腺素可能有助于避免过度治疗。延迟TSH升高导致假阴性的第一次DBS在永久性CH的早产新生儿中并不罕见。这证明了在早产儿中进行第二次DBS的理由。鉴于本研究的回顾性性质,这些发现应谨慎解释,并有必要进一步的前瞻性研究来证实这些观察结果。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Delayed Thyrotropin Rise in Preterm Newborns: Value of Multiple Screening Samples and of a Detailed Clinical Characterization.

Background: Newborn screening for congenital hypothyroidism (CH) has been implemented in high-income countries since the 1970s to prevent intellectual disability. A delayed thyrotropin (TSH) rise with a normal TSH on the first dry blood spot (DBS) sample, followed by an abnormal TSH on the subsequent DBS, is sometimes observed in preterm newborns. The incidence of permanent CH and the screening process in preterm newborns remain controversial. Our aim was to evaluate the incidence of transient and permanent CH and delayed TSH rise in preterm newborns. The utility of a multiple screening samples is discussed. Methods: We conducted a retrospective study on preterm newborns (<37 weeks of gestation) screened at the Newborn Screening Center of Université Libre de Bruxelles between January 2014 and December 2023. A literature review was performed to identify cases of permanent CH with delayed TSH rise in cohorts of preterm newborns. Results: Of the 3578 preterm newborns included in the study, 10 were diagnosed with CH (0.3%). The majority of CH cases were transient (6 out of 10 transient, one deceased and one under ongoing L-thyroxine, too young for weaning attempt). Six cases were detected at the first DBS, four at subsequent DBS. Only two cases were confirmed as permanent CH, yielding an incidence of 1 in 1789 for permanent CH in preterms (0.05%). One of the two had a delayed TSH rise. Genetic testing helped in establishing the diagnosis of permanent CH with gland in situ. Conclusions: Permanent CH appears to be rarer than transient CH among preterm newborns (1/1789 vs. 1/596). Transient CH may be suspected in case of iodine exposure or thyroid ultrasound showing an in situ gland with negative genetic testing and absent maternal blocking antibodies. In such cases, early L-thyroxine weaning may help avoid overtreatment. A delayed TSH rise leading to a false negative first DBS is not uncommon in preterm newborns with permanent CH. This justifies a second DBS in preterms. Given the retrospective nature of this study, these findings should be interpreted with caution, and further prospective research is warranted to confirm these observations.

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来源期刊
Thyroid
Thyroid 医学-内分泌学与代谢
CiteScore
12.30
自引率
6.10%
发文量
195
审稿时长
6 months
期刊介绍: This authoritative journal program, including the monthly flagship journal Thyroid, Clinical Thyroidology® (monthly), and VideoEndocrinology™ (quarterly), delivers in-depth coverage on topics from clinical application and primary care, to the latest advances in diagnostic imaging and surgical techniques and technologies, designed to optimize patient care and outcomes. Thyroid is the leading, peer-reviewed resource for original articles, patient-focused reports, and translational research on thyroid cancer and all thyroid related diseases. The Journal delivers the latest findings on topics from primary care to clinical application, and is the exclusive source for the authoritative and updated American Thyroid Association (ATA) Guidelines for Managing Thyroid Disease.
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