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Structural insights into dimethylation of 12S rRNA by TFB1M: indispensable role in translation of mitochondrial genes and mitochondrial function

机译:TFB1M对12S rRNA进行二甲基化的结构见解:线粒体基因翻译和线粒体功能中不可或缺的作用

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Mitochondria are essential molecular machinery for the maintenance of cellular energy supply by the oxidative phosphorylation system (OXPHOS). Mitochondrial transcription factor B1 (TFB1M) is a dimethyltransferase that maintains mitochondrial homeostasis by catalyzing dimethylation of two adjacent adenines located in helix45 (h45) of 12S rRNA. This m62A modification is indispensable for the assembly and maturation of human mitochondrial ribosomes. However, both the mechanism of TFB1M catalysis and the precise function of TFB1M in mitochondrial homeostasis are unknown. Here we report the crystal structures of a ternary complex of human (hs) TFB1M–h45–S-adenosyl-methionine and a binary complex hsTFB1M–h45. The structures revealed a distinct mode of hsTFB1M interaction with its rRNA substrate and with the initial enzymatic state involved in m62A modification. The suppression of hsTFB1M protein level or the overexpression of inactive hsTFB1M mutants resulted in decreased ATP production and reduced expression of components of the mitochondrial OXPHOS without affecting transcription of the corresponding genes and their localization to the mitochondria. Therefore, hsTFB1M regulated the translation of mitochondrial genes rather than their transcription via m62A modification in h45.
机译:线粒体是通过氧化磷酸化系统(OXPHOS)维持细胞能量供应的必不可少的分子机制。线粒体转录因子B1(TFB1M)是一种二甲基转移酶,可通过催化位于12S rRNA螺旋45(h45)中的两个相邻腺嘌呤的二甲基化来维持线粒体的体内稳态。这种m62A修饰对于人类线粒体核糖体的组装和成熟是必不可少的。但是,TFB1M催化的机理和TFB1M在线粒体内稳态中的精确功能均未知。在这里,我们报告了人(hs)TFB1M–h45–S-腺苷甲硫氨酸和二元复合物hsTFB1M–h45三元复合物的晶体结构。该结构揭示了hsTFB1M与rRNA底物以及参与m62A修饰的初始酶促状态相互作用的独特模式。抑制hsTFB1M蛋白水平或过度表达无活性的hsTFB1M突变体会导致ATP产量降低和线粒体OXPHOS组分的表达降低,而不会影响相应基因的转录及其在线粒体中的定位。因此,hsTFB1M通过h45中的m62A修饰来调节线粒体基因的翻译,而不是其转录。

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