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Specificity shifts in the rRNA and tRNA nucleotide targets of archaeal and bacterial m5U methyltransferases.

机译:古细菌和细菌m5U甲基转移酶的rRNA和tRNA核苷酸靶标的特异性转移。

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Methyltransferase enzymes that use S-adenosylmethionine as a cofactor to catalyze 5-methyl uridine (m(5)U) formation in tRNAs and rRNAs are widespread in Bacteria and Eukaryota, but are restricted to the Thermococcales and Nanoarchaeota groups amongst the Archaea. The RNA m(5)U methyltransferases appear to have arisen in Bacteria and were then dispersed by horizontal transfer of an rlmD-type gene to the Archaea and Eukaryota. The bacterium Escherichia coli has three gene paralogs and these encode the methyltransferases TrmA that targets m(5)U54 in tRNAs, RlmC (formerly RumB) that modifies m(5)U747 in 23S rRNA, and RlmD (formerly RumA) the archetypical enzyme that is specific for m(5)U1939 in 23S rRNA. The thermococcale archaeon Pyrococcus abyssi possesses two m(5)U methyltransferase paralogs, PAB0719 and PAB0760, with sequences most closely related to the bacterial RlmD. Surprisingly, however, neither of the two P. abyssi enzymes displays RlmD-like activity in vitro. PAB0719 acts in a TrmA-like manner to catalyze m(5)U54 methylation in P. abyssi tRNAs, and here we show that PAB0760 possesses RlmC-like activity and specifically methylates the nucleotide equivalent to U747 in P. abyssi 23S rRNA. The findings indicate that PAB0719 and PAB0760 originated as RlmD-type m(5)U methyltransferases and underwent changes in target specificity after their acquisition by a Thermococcales ancestor from a bacterial source.
机译:使用S-腺苷甲硫氨酸作为辅助因子催化tRNA和rRNA中5-甲基尿苷(m(5)U)形成的甲基转移酶在细菌和真核生物中很普遍,但仅限于古生菌中的嗜热球菌和纳米古菌群。 RNA m(5)U甲基转移酶似乎已经出现在细菌中,然后通过rlmD型基因水平转移到古细菌和真核生物而分散。大肠杆菌具有三个基因旁系同源物,它们编码靶向tRNA中m(5)U54的甲基转移酶TrmA,修饰23S rRNA中m(5)U747的RlmC(以前的RumB)和原型酶RlmD(以前的RumA)。对23S rRNA中的m(5)U1939具有特异性。嗜热球菌古毕赤酵母具有两个m(5)U甲基转移酶旁系同源物,PAB0719和PAB0760,其序列与细菌RlmD最密切相关。然而,令人惊讶的是,两种深海毕赤酵母酶均未在体外显示出RlmD样活性。 PAB0719以类似TrmA的方式起作用,以催化深渊毕赤酵母tRNA中的m(5)U54甲基化,在这里我们显示PAB0760具有RlmC样活性,并特异性地甲基化了深渊毕赤酵母23S rRNA中与U747等效的核苷酸。这些发现表明,PAB0719和PAB0760起源于RlmD型m(5)U甲基转移酶,在被细菌嗜热球菌祖先收购后,其靶标特异性发生了变化。

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