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早产儿雄激素代谢组反映胎儿肾上腺萎缩。

The Androgen Metabolome of Preterm Infants Reflects Fetal Adrenal Gland Involution.

机构信息

Department of Pediatrics, Division of Endocrinology, Diabetology and Metabolism, Inselspital, Bern University Hospital, University of Bern, 3010 Bern, Switzerland.

Department of BioMedical Research, Inselspital, Bern University Hospital, University of Bern, 3010 Bern, Switzerland.

出版信息

J Clin Endocrinol Metab. 2022 Nov 23;107(11):3111-3119. doi: 10.1210/clinem/dgac482.

Abstract

CONTEXT

The human adrenal cortex changes with fetal-neonatal transition from the fetal to the adult organ, accompanied by changes in the steroid metabolome.

OBJECTIVE

As it is unclear how the observed developmental changes differ between preterm and full-term neonates, we investigated whether the involution of the fetal adrenals is following a fixed time course related to postmenstrual age or whether it is triggered by birth. Furthermore, the fetal and postnatal androgen metabolome of preterm infants was characterized in comparison to term babies.

METHODS

This was a prospective, longitudinal, 2-center study collecting spot urines of preterm and term infants during the first 12 to 18 months of life. Steroid metabolites were measured from spot urines by gas chromatography-mass spectrometry. Data relating were modeled according to established pre- and postnatal pathways.

RESULTS

Fetal adrenal involution occurs around term-equivalent age in preterm infants and is not triggered by premature birth. Testosterone levels are higher in preterm infants at birth and decline slower until term compared to full-term babies. Dihydrotestosterone levels and the activity of the classic androgen biosynthesis pathway are lower in premature infants as is 5α-reductase activity. No difference was found in the activity of the alternate backdoor pathway for androgen synthesis.

CONCLUSION

Human adrenal involution follows a strict timing that is not affected by premature birth. By contrast, prematurity is associated with an altered androgen metabolome after birth. Whether this reflects altered androgen biosynthesis in utero remains to be investigated.

摘要

背景

人类肾上腺皮质在胎儿-新生儿过渡期会从胎儿期转变为成人器官,同时其类固醇代谢组也会发生变化。

目的

由于尚不清楚早产儿和足月儿之间观察到的发育变化有何不同,我们研究了胎儿肾上腺的退化是否遵循与胎龄相关的固定时间过程,还是由出生触发。此外,我们还比较了早产儿和足月儿的胎儿和产后雄激素代谢组。

方法

这是一项前瞻性、纵向、2 中心研究,在婴儿出生后的前 12 至 18 个月内收集早产儿和足月儿的尿液样本。通过气相色谱-质谱法从尿液样本中测量类固醇代谢物。根据已建立的产前和产后途径对相关数据进行建模。

结果

早产儿的胎儿肾上腺退化发生在胎龄相等的年龄,而不是由早产触发。与足月儿相比,早产儿在出生时的睾酮水平更高,下降速度更慢,直到足月。与足月儿相比,早产儿的二氢睾酮水平和经典雄激素生物合成途径的活性较低,5α-还原酶活性也较低。未发现替代后门途径(用于雄激素合成)的活性存在差异。

结论

人类肾上腺的退化遵循严格的时间规律,不受早产的影响。相比之下,早产儿在出生后会出现雄激素代谢组的改变。这是否反映了胎儿期雄激素生物合成的改变还有待研究。

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