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建立一种新型的支持从头合成和操纵类固醇生成的人胎儿肾上腺培养模型。

Establishment of a Novel Human Fetal Adrenal Culture Model that Supports de Novo and Manipulated Steroidogenesis.

机构信息

Department of Growth and Reproduction, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.

International Center for Research and Research Training in Endocrine Disruption of Male Reproduction and Child Health, Rigshospitalet, University of Copenhagen, Copenhagen, Denmark.

出版信息

J Clin Endocrinol Metab. 2021 Mar 8;106(3):843-857. doi: 10.1210/clinem/dgaa852.

Abstract

CONTEXT

Disorders affecting adrenal steroidogenesis promote an imbalance in the normally tightly controlled secretion of mineralocorticoids, glucocorticoids, and androgens. This may lead to differences/disorders of sex development in the fetus, as seen in virilized girls with congenital adrenal hyperplasia (CAH). Despite the important endocrine function of human fetal adrenals, neither normal nor dysregulated adrenal steroidogenesis is understood in detail.

OBJECTIVE

Due to significant differences in adrenal steroidogenesis between human and model species (except higher primates), we aimed to establish a human fetal adrenal model that enables examination of both de novo and manipulated adrenal steroidogenesis.

DESIGN AND SETTING

Human adrenal tissue from 54 1st trimester fetuses were cultured ex vivo as intact tissue fragments for 7 or 14 days.

MAIN OUTCOME MEASURES

Model validation included examination of postculture tissue morphology, viability, apoptosis, and quantification of steroid hormones secreted to the culture media measured by liquid chromatography-tandem mass spectrometry.

RESULTS

The culture approach maintained cell viability, preserved cell populations of all fetal adrenal zones, and recapitulated de novo adrenal steroidogenesis based on continued secretion of steroidogenic intermediates, glucocorticoids, and androgens. Adrenocorticotropic hormone and ketoconazole treatment of ex vivo cultured human fetal adrenal tissue resulted in the stimulation of steroidogenesis and inhibition of androgen secretion, respectively, demonstrating a treatment-specific response.

CONCLUSIONS

Together, these data indicate that ex vivo culture of human fetal adrenal tissue constitutes a novel approach to investigate local effects of pharmaceutical exposures or emerging therapeutic options targeting imbalanced steroidogenesis in adrenal disorders, including CAH.

摘要

背景

影响肾上腺甾体生成的疾病会导致矿物质皮质激素、糖皮质激素和雄激素的正常严格控制的分泌失衡。这可能导致胎儿出现性别发育差异/障碍,如先天性肾上腺增生症(CAH)的女性化女孩。尽管人类胎儿肾上腺具有重要的内分泌功能,但正常和失调的肾上腺甾体生成都没有得到详细的了解。

目的

由于人类和模型物种(除了高等灵长类动物)之间在肾上腺甾体生成方面存在显著差异,我们旨在建立一种人类胎儿肾上腺模型,以检查新生成的和受操作的肾上腺甾体生成。

设计和设置

将 54 例 1 期胎儿的肾上腺组织作为完整的组织片段进行离体培养 7 或 14 天。

主要观察指标

模型验证包括检查培养后组织形态、活力、凋亡,以及通过液相色谱-串联质谱法测量分泌到培养基中的类固醇激素的定量。

结果

该培养方法保持了细胞活力,保留了所有胎儿肾上腺区的细胞群体,并基于类固醇生成中间产物、糖皮质激素和雄激素的持续分泌,重新生成了新的肾上腺甾体生成。促肾上腺皮质激素和酮康唑对离体培养的人类胎儿肾上腺组织的处理分别导致了甾体生成的刺激和雄激素分泌的抑制,表明存在特定于处理的反应。

结论

总之,这些数据表明,人类胎儿肾上腺组织的离体培养构成了一种新的方法,可以研究药物暴露或针对肾上腺疾病中失衡的甾体生成的新兴治疗选择的局部效应,包括 CAH。

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