首页> 外文期刊>Genes and Development: a Journal Devoted to the Molecular Analysis of Gene Expression in Eukaryotes, Prokaryotes, and Viruses >A Mediator subunit, MDT-15, integrates regulation of fatty acid metabolism by NHR-49-dependent and -independent pathways in C. elegans.
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A Mediator subunit, MDT-15, integrates regulation of fatty acid metabolism by NHR-49-dependent and -independent pathways in C. elegans.

机译:介体亚基MDT-15通过秀丽隐杆线虫的NHR-49依赖性和非依赖性途径整合脂肪酸代谢的调控。

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The Caenorhabditis elegans Nuclear Hormone Receptor NHR-49 coordinates expression of fatty acid (FA) metabolic genes during periods of feeding and in response to fasting. Here we report the identification of MDT-15, a subunit of the C. elegans Mediator complex, as an NHR-49-interacting protein and transcriptional coactivator. Knockdown of mdt-15 by RNA interference (RNAi) prevented fasting-induced mRNA accumulation of NHR-49 targets in vivo, and fasting-independent expression of other NHR-49 target genes, including two FA-Delta9-desaturases (fat-5, fat-7). Interestingly, mdt-15 RNAi affected additional FA-metabolism genes (including the third FA-Delta9-desaturase, fat-6) that are regulated independently of NHR-49, suggesting that distinct unidentified regulatory factors also recruit MDT-15 to selectively modulate metabolic gene expression. The deregulation of FA-Delta9-desaturases by knockdown of mdt-15 correlated with dramatically decreased levels of unsaturated FAs and multiple deleterious phenotypes(short life span, sterility, uncoordinated locomotion, and morphological defects). Importantly, dietary addition of specific polyunsaturated FAs partially suppressed these pleiotropic phenotypes. Thus, failure to properly govern FA-Delta9-desaturation contributed to decreased nematode viability. Our findings imply that a single subunit of the Mediator complex, MDT-15, integrates the activities of several distinct regulatory factors to coordinate metabolic and hormonal regulation of FA metabolism.
机译:秀丽隐杆线虫核激素受体NHR-49协调进食期间和禁食时脂肪酸(FA)代谢基因的表达。在这里,我们报告鉴定线虫介体复合物的亚基MDT-15作为NHR-49相互作用蛋白和转录共激活因子。通过RNA干扰(RNAi)敲除mdt-15可以防止空腹诱导的NHR-49靶标在体内的mRNA积累以及其他NHR-49靶标基因的空腹非依赖性表达,包括两个FA-Delta9-去饱和酶(fat-5胖7)。有趣的是,mdt-15 RNAi影响了独立于NHR-49调控的其他FA代谢基因(包括第三个FA-Delta9-去饱和酶fat-6),这表明不同的未知调控因子也募集了MDT-15来选择性地调节代谢基因表达。通过敲低mdt-15来解除对FA-Delta9-去饱和酶的调节,这与不饱和FA的水平显着降低和多种有害表型(寿命短,不育,运动不协调和形态缺陷)有关。重要的是,饮食中添加特定的多不饱和脂肪酸可以部分抑制这些多效性表型。因此,未能正确控制FA-Delta9-去饱和作用导致线虫活力降低。我们的发现暗示,介体复合物MDT-15的单个亚基整合了几个不同调节因子的活性,以协调FA代谢的代谢和激素调节。

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