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小鼠肾上腺发育需要GATA4和GATA6转录因子。

Adrenal Development in Mice Requires GATA4 and GATA6 Transcription Factors.

作者信息

Tevosian Sergei G, Jiménez Elizabeth, Hatch Heather M, Jiang Tianyu, Morse Deborah A, Fox Shawna C, Padua Maria B

机构信息

Department of Physiological Sciences (S.G.T., E.J., H.M.H., T.J., S.C.F., M.B.P.), College of Veterinary Medicine, University of Florida, Gainesville, Florida 32610-0144; and Department of Applied Physiology and Kinesiology (D.A.M.), College of Health and Human Performance, University of Florida, Gainesville, Florida 32611-8200.

出版信息

Endocrinology. 2015 Jul;156(7):2503-17. doi: 10.1210/en.2014-1815. Epub 2015 May 1.

Abstract

The adrenal glands consist of an outer cortex and an inner medulla, and their primary purposes include hormone synthesis and secretion. The adrenal cortex produces a complex array of steroid hormones, whereas the medulla is part of the sympathetic nervous system and produces the catecholamines epinephrine and norepinephrine. In the mouse, GATA binding protein (GATA) 4 and GATA6 transcription factors are coexpressed in several embryonic tissues, including the adrenal cortex. To explore the roles of GATA4 and GATA6 in mouse adrenal development, we conditionally deleted these genes in adrenocortical cells using the Sf1Cre strain of animals. We report here that mice with Sf1Cre-mediated double deletion of Gata4 and Gata6 genes lack identifiable adrenal glands, steroidogenic factor 1-positive cortical cells and steroidogenic gene expression in the adrenal location. The inactivation of the Gata6 gene alone (Sf1Cre;Gata6(flox/flox)) drastically reduced the adrenal size and corticosterone production in the adult animals. Adrenocortical aplasia is expected to result in the demise of the animal within 2 weeks after birth unless glucocorticoids are provided. In accordance, Sf1Cre;Gata4(flox/flox)Gata6(flox/flox) females depend on steroid supplementation to survive after weaning. Surprisingly, Sf1Cre;Gata4(flox/flox)Gata6(flox/flox) males appear to live normal lifespans as vital steroidogenic synthesis shifts to their testes. Our results reveal a requirement for GATA factors in adrenal development and provide a novel tool to characterize the transcriptional network controlling adrenocortical cell fates.

摘要

肾上腺由外层皮质和内层髓质组成,其主要功能包括激素合成与分泌。肾上腺皮质产生一系列复杂的类固醇激素,而髓质是交感神经系统的一部分,产生儿茶酚胺类物质肾上腺素和去甲肾上腺素。在小鼠中,GATA结合蛋白(GATA)4和GATA6转录因子在包括肾上腺皮质在内的几种胚胎组织中共同表达。为了探究GATA4和GATA6在小鼠肾上腺发育中的作用,我们使用Sf1Cre品系动物在肾上腺皮质细胞中条件性删除了这些基因。我们在此报告,经Sf1Cre介导双缺失Gata4和Gata6基因的小鼠缺乏可识别的肾上腺、类固醇生成因子1阳性皮质细胞以及肾上腺部位的类固醇生成基因表达。单独敲除Gata6基因(Sf1Cre;Gata6(flox/flox))会显著减小成年动物的肾上腺大小并降低皮质酮的产生。肾上腺皮质发育不全预计会导致动物在出生后2周内死亡,除非提供糖皮质激素。相应地,Sf1Cre;Gata4(flox/flox)Gata6(flox/flox)雌性小鼠断奶后依赖类固醇补充才能存活。令人惊讶的是,Sf1Cre;Gata4(flox/flox)Gata6(flox/flox)雄性小鼠似乎能正常寿命,因为重要的类固醇生成合成转移到了它们的睾丸。我们的结果揭示了肾上腺发育中对GATA因子的需求,并提供了一种新工具来表征控制肾上腺皮质细胞命运的转录网络。

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