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17β-雌二醇和染料木黄酮对小鼠胸腺影响的基因表达谱分析

Gene expression profiling of 17beta-estradiol and genistein effects on mouse thymus.

作者信息

Selvaraj Vimal, Bunick David, Finnigan-Bunick Carrol, Johnson Rodney W, Wang Huixia, Liu Lei, Cooke Paul S

机构信息

Department of Veterinary Biosciences, University of Illinois at Urbana-Champaign, Urbana, Illinois 61802, USA.

出版信息

Toxicol Sci. 2005 Sep;87(1):97-112. doi: 10.1093/toxsci/kfi219. Epub 2005 Jun 9.

Abstract

Estrogen regulates thymic development and involution and modulates immune function. Despite its critical role in thymus, as well as in autoimmune disorders, the mechanism by which estrogen affects the thymus is not well understood. We previously reported that the estrogenic soy isoflavone genistein, as well as 17beta-estradiol (E2), could induce thymic involution, but genistein effects were only partially mediated through estrogen receptors. To provide insights into mechanisms of estrogenic effects in the thymus, we investigated thymic gene expression changes induced by E2 (125 ng/day) and genistein (1500 ppm in feed) in weanling mice using high-density DNA arrays. We identified several E2-responsive genes involved in thymic development and thymocyte signaling during selection and maturation. Functional characterization indicated effects on genes involved in transcription, apoptosis, and the cell cycle. This study also identified changes in several E2-regulated transcripts essential to maintain immune self-tolerance. E2 upregulated more genes than genistein, while genistein downregulated more genes than E2. Though each treatment regulated several genes not altered by the other, there was considerable overlap in the genes regulated by E2 and genistein. Changes in transcription factors and cell cycle factors were consistent with decreases in cell proliferation induced by both genistein and E2. As indicated by the regulation of non-E2-responsive genes, genistein also induced unique effects through non-estrogenic mechanisms. The specific downregulation of the CD4 coreceptor transcript by genistein was consistent with the decline of CD4+ thymocytes in genistein-treated mice in our previous study. This is the first study identifying E2 and genistein target genes in the thymus. These findings provide new mechanistic insights toward explaining estrogen action on thymocyte development, selection, and maturation, as well as the effects of genistein on prenatal and neonatal thymic development and function.

摘要

雌激素调节胸腺的发育与退化,并调节免疫功能。尽管雌激素在胸腺以及自身免疫性疾病中起着关键作用,但其影响胸腺的机制尚未完全明确。我们之前报道过,雌激素样大豆异黄酮染料木黄酮以及17β-雌二醇(E2)均可诱导胸腺退化,但染料木黄酮的作用仅部分通过雌激素受体介导。为深入了解雌激素在胸腺中的作用机制,我们使用高密度DNA阵列研究了断奶小鼠中E2(125 ng/天)和染料木黄酮(饲料中1500 ppm)诱导的胸腺基因表达变化。我们鉴定出了几个在胸腺发育以及胸腺细胞选择和成熟过程中的信号传导中起作用的E2反应基因。功能特征表明其对参与转录、凋亡和细胞周期的基因有影响。本研究还鉴定出了几种对维持免疫自我耐受至关重要的E2调节转录本的变化。E2上调的基因比染料木黄酮更多,而染料木黄酮下调的基因比E2更多。尽管每种处理都调节了一些未被另一种处理改变的基因,但E2和染料木黄酮调节的基因有相当大的重叠。转录因子和细胞周期因子的变化与染料木黄酮和E2诱导的细胞增殖减少一致。如对非E2反应基因的调节所示,染料木黄酮还通过非雌激素机制诱导独特的效应。染料木黄酮对CD4共受体转录本的特异性下调与我们之前研究中染料木黄酮处理小鼠中CD4+胸腺细胞的减少一致。这是第一项鉴定胸腺中E2和染料木黄酮靶基因的研究。这些发现为解释雌激素对胸腺细胞发育、选择和成熟的作用以及染料木黄酮对产前和新生儿胸腺发育及功能的影响提供了新的机制见解。

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