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贾景怡, 陈光辉, 舒婷婷, 娄气永, 金霞, 贺江燕, 肖武汉, 翟刚, 殷战. 2024: 雄激素信号通路通过抑制斑马鱼体内脂肪从头合成进而减少脂质沉积. 动物学研究, 45(2): 355-366. DOI: 10.24272/j.issn.2095-8137.2023.324
引用本文: 贾景怡, 陈光辉, 舒婷婷, 娄气永, 金霞, 贺江燕, 肖武汉, 翟刚, 殷战. 2024: 雄激素信号通路通过抑制斑马鱼体内脂肪从头合成进而减少脂质沉积. 动物学研究, 45(2): 355-366. DOI: 10.24272/j.issn.2095-8137.2023.324
Jing-Yi Jia, Guang-Hui Chen, Ting-Ting Shu, Qi-Yong Lou, Xia Jin, Jiang-Yan He, Wu-Han Xiao, Gang Zhai, Zhan Yin. 2024. Androgen signaling inhibits de novo lipogenesis to alleviate lipid deposition in zebrafish. Zoological Research, 45(2): 355-366. DOI: 10.24272/j.issn.2095-8137.2023.324
Citation: Jing-Yi Jia, Guang-Hui Chen, Ting-Ting Shu, Qi-Yong Lou, Xia Jin, Jiang-Yan He, Wu-Han Xiao, Gang Zhai, Zhan Yin. 2024. Androgen signaling inhibits de novo lipogenesis to alleviate lipid deposition in zebrafish. Zoological Research, 45(2): 355-366. DOI: 10.24272/j.issn.2095-8137.2023.324

雄激素信号通路通过抑制斑马鱼体内脂肪从头合成进而减少脂质沉积

Androgen signaling inhibits de novo lipogenesis to alleviate lipid deposition in zebrafish

  • 摘要: 睾酮可以影响雄性体内脂肪成分和肌肉质量,与脂质代谢密切相关。然而,在硬骨鱼中,睾酮对脂质代谢的作用机制尚不清晰。在该研究中,我们首先观察到雄激素合成的cyp17a1-/-斑马鱼表现出增多的内脏脂肪组织(VAT),其脂肪含量以及肝脏脂肪从头合成(DNL)酶的表达和活性上调。染色质转座酶可及性测序分析(ATAC-seq)的结果表明,与cyp17a1+/+雄鱼相比,cyp17a1-/-鱼的DNL基因的染色质可及性增加,包括硬脂酰辅酶a去饱和酶(scd)和脂肪酸合成酶(fasn)。雄激素信号通路中的雄激素反应元件(ARE)基序在cyp17a1+/+雄鱼中显著富集,但未在cyp17a1-/-鱼中富集。同样地,雄激素受体(ar)-/-斑马鱼和雄激素受体拮抗剂氟他胺(Flutamide)处理的野生型斑马鱼也表现出VAT增多和脂质含量增加,肝脏脂肪从头合成酶的表达和活性上调。相反,雄激素受体激动剂BMS-564929显著减少了VAT和脂质含量,下调了乙酰辅酶a羧化酶a(acaca)、fasnscd的表达。有趣的是,睾酮处理可以有效挽救cyp17a1-/-斑马鱼的上述表型,但在ar被额外敲除后(即在cyp17a1-/-;ar-/-斑马鱼中)则未见挽救效果。综上所述,我们的研究揭示了睾酮通过Ar下调DNL基因表达和活性,进而抑制斑马鱼的脂质沉积。该研究有助于深入理解硬骨鱼类的雄激素调节脂质代谢的分子机制。

     

    Abstract: Testosterone is closely associated with lipid metabolism and known to affect body fat composition and muscle mass in males. However, the mechanisms by which testosterone acts on lipid metabolism are not yet fully understood, especially in teleosts. In this study, cyp17a1-/- zebrafish (Danio rerio) exhibited excessive visceral adipose tissue (VAT), lipid content, and up-regulated expression and activity of hepatic de novo lipogenesis (DNL) enzymes. The assay for transposase accessible chromatin with sequencing (ATAC-seq) results demonstrated that chromatin accessibility of DNL genes was increased in cyp17a1-/- fish compared to cyp17a1+/+ male fish, including stearoyl-CoA desaturase (scd) and fatty acid synthase (fasn). Androgen response element (ARE) motifs in the androgen signaling pathway were significantly enriched in cyp17a1+/+ male fish but not in cyp17a1-/- fish. Both androgen receptor (ar)-/- and wild-type (WT) zebrafish administered with Ar antagonist flutamide displayed excessive visceral adipose tissue, lipid content, and up-regulated expression and activity of hepatic de novo lipogenesis enzymes. The Ar agonist BMS-564929 reduced the content of VAT and lipid content, and down-regulated acetyl-CoA carboxylase a (acaca), fasn, and scd expression. Mechanistically, the rescue effect of testosterone on cyp17a1-/- fish in terms of phenotypes was abolished when ar was additionally depleted. Collectively, these findings reveal that testosterone inhibits lipid deposition by down-regulating DNL genes via Ar in zebrafish, thus expanding our understanding of the relationship between testosterone and lipid metabolism in teleosts.

     

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