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粗糙脉孢菌的RCO-1共抑制因子对昼夜节律基因表达和代谢补偿的调控

Modulation of Circadian Gene Expression and Metabolic Compensation by the RCO-1 Corepressor of Neurospora crassa.

作者信息

Olivares-Yañez Consuelo, Emerson Jillian, Kettenbach Arminja, Loros Jennifer J, Dunlap Jay C, Larrondo Luis F

机构信息

Millennium Nucleus for Fungal Integrative and Synthetic Biology, Departamento de Genética Molecular y Microbiología, Facultad de Ciencias Biológicas, Pontificia Universidad Católica de Chile, Santiago RM 114-D, Chile.

Department of Genetics, Geisel School of Medicine at Dartmouth College, Hanover, New Hampshire 03755.

出版信息

Genetics. 2016 Sep;204(1):163-76. doi: 10.1534/genetics.116.191064. Epub 2016 Jul 22.

Abstract

Neurospora crassa is a model organism for the study of circadian clocks, molecular machineries that confer ∼24-hr rhythms to different processes at the cellular and organismal levels. The FREQUENCY (FRQ) protein is a central component of the Neurospora core clock, a transcription/translation negative feedback loop that controls genome-wide rhythmic gene expression. A genetic screen aimed at determining new components involved in the latter process identified regulation of conidiation 1 (rco-1), the ortholog of the Saccharomyces cerevisiae Tup1 corepressor, as affecting period length. By employing bioluminescent transcriptional and translational fusion reporters, we evaluated frq and FRQ expression levels in the rco-1 mutant background observing that, in contrast to prior reports, frq and FRQ expression are robustly rhythmic in the absence of RCO-1, although both amplitude and period length of the core clock are affected. Moreover, we detected a defect in metabolic compensation, such that high-glucose concentrations in the medium result in a significant decrease in period when RCO-1 is absent. Proteins physically interacting with RCO-1 were identified through co-immunoprecipitation and mass spectrometry; these include several components involved in chromatin remodeling and transcription, some of which, when absent, lead to a slight change in period. In the aggregate, these results indicate a dual role for RCO-1: although it is not essential for core-clock function, it regulates proper period and amplitude of core-clock dynamics and is also required for the rhythmic regulation of several clock-controlled genes.

摘要

粗糙脉孢菌是用于研究生物钟的模式生物,生物钟是在细胞和机体水平赋予不同过程约24小时节律的分子机制。频率(FRQ)蛋白是粗糙脉孢菌核心生物钟的核心组成部分,核心生物钟是一个转录/翻译负反馈环,控制全基因组范围的节律性基因表达。一项旨在确定参与后一过程的新组分的遗传筛选鉴定出分生孢子形成调控因子1(rco-1),它是酿酒酵母Tup1共抑制因子的直系同源物,会影响周期长度。通过使用生物发光转录和翻译融合报告基因,我们评估了rco-1突变背景下frq和FRQ的表达水平,观察到与先前报道相反,在没有RCO-1的情况下,frq和FRQ的表达具有强烈的节律性,尽管核心生物钟的振幅和周期长度均受到影响。此外,我们检测到代谢补偿缺陷,使得在没有RCO-1的情况下,培养基中的高葡萄糖浓度会导致周期显著缩短。通过免疫共沉淀和质谱鉴定了与RCO-1发生物理相互作用的蛋白质;这些蛋白质包括参与染色质重塑和转录的几个组分,其中一些组分缺失时会导致周期略有变化。总体而言,这些结果表明RCO-1具有双重作用:尽管它对于核心生物钟功能不是必需的,但它调节核心生物钟动态的适当周期和振幅,并且也是几个生物钟控制基因节律性调节所必需的。

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