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线粒体中的一种tRNA修饰酶对秀丽隐杆线虫生理速率的调控。

Regulation of physiological rates in Caenorhabditis elegans by a tRNA-modifying enzyme in the mitochondria.

作者信息

Lemieux J, Lakowski B, Webb A, Meng Y, Ubach A, Bussière F, Barnes T, Hekimi S

机构信息

Department of Biology, McGill University, Montréal, Québec H3A 1B1, Canada.

出版信息

Genetics. 2001 Sep;159(1):147-57. doi: 10.1093/genetics/159.1.147.

Abstract

We show that the phenotype associated with gro-1(e2400) comprises the whole suite of features that characterize the phenotype of the clk mutants in Caenorhabditis elegans, including deregulated developmental, behavioral, and reproductive rates, as well as increased life span and a maternal effect. We cloned gro-1 and found that it encodes a highly conserved cellular enzyme, isopentenylpyrophosphate:tRNA transferase (IPT), which modifies a subset of tRNAs. In yeast, two forms of the enzyme are produced by alternative translation initiation, one of which is mitochondrial. In the gro-1 transcript there are also two possible initiator ATGs, between which there is a sequence predicted to encode a mitochondrial localization signal. A functional GRO-1::GFP fusion protein is localized diffusely throughout the cytoplasm and nucleus. A GRO-1::GFP initiated from the first methionine is localized exclusively to the mitochondria and rescues the mutant phenotype. In contrast, a protein initiated from the second methionine is localized diffusely throughout the cell and does not rescue the mutant phenotype. As oxygen consumption and ATP concentration have been reported to be unaffected in gro-1 mutants, our observations suggest that GRO-1 acts in mitochondria and regulates global physiology by unknown mechanisms.

摘要

我们发现,与gro-1(e2400)相关的表型包含了秀丽隐杆线虫中clk突变体表型的全部特征,包括发育、行为和繁殖速率失调,以及寿命延长和母体效应。我们克隆了gro-1,发现它编码一种高度保守的细胞酶,异戊烯基焦磷酸:tRNA转移酶(IPT),该酶可修饰一部分tRNA。在酵母中,该酶的两种形式由交替翻译起始产生,其中一种定位于线粒体。在gro-1转录本中也有两个可能的起始ATG,它们之间有一个预测编码线粒体定位信号的序列。功能性GRO-1::GFP融合蛋白弥漫性地定位于整个细胞质和细胞核。从第一个甲硫氨酸起始的GRO-1::GFP仅定位于线粒体,并能挽救突变体表型。相反,从第二个甲硫氨酸起始的蛋白弥漫性地定位于整个细胞,不能挽救突变体表型。由于据报道gro-1突变体中的氧消耗和ATP浓度不受影响,我们的观察结果表明,GRO-1在线粒体中起作用,并通过未知机制调节整体生理功能。

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