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Identification of the Proteins Required for Biosynthesis of Diphthamide the Target of Bacterial ADP-Ribosylating Toxins on Translation Elongation Factor 2

机译:鉴定双硫酰胺生物合成所需的蛋白质双硫酰胺是细菌细菌ADP-核糖基化毒素在翻译延伸因子2上的靶标

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摘要

Diphthamide, a posttranslational modification of translation elongation factor 2 that is conserved in all eukaryotes and archaebacteria and is the target of diphtheria toxin, is formed in yeast by the actions of five proteins, Dph1 to -5, and a still unidentified amidating enzyme. Dph2 and Dph5 were previously identified. Here, we report the identification of the remaining three yeast proteins (Dph1, -3, and -4) and show that all five Dph proteins have either functional (Dph1, -2, -3, and -5) or sequence (Dph4) homologs in mammals. We propose a unified nomenclature for these proteins (e.g., HsDph1 to -5 for the human proteins) and their genes based on the yeast nomenclature. We show that Dph1 and Dph2 are homologous in sequence but functionally independent. The human tumor suppressor gene OVCA1, previously identified as homologous to yeast DPH2, is shown to actually be HsDPH1. We show that HsDPH3 is the previously described human diphtheria toxin and Pseudomonas exotoxin A sensitivity required gene 1 and that DPH4 encodes a CSL zinc finger-containing DnaJ-like protein. Other features of these genes are also discussed. The physiological function of diphthamide and the basis of its ubiquity remain a mystery, but evidence is presented that Dph1 to -3 function in vivo as a protein complex in multiple cellular processes.
机译:白喉酰胺是翻译延伸因子2的翻译后修饰,它在所有真核生物和古细菌中均是保守的,并且是白喉毒素的靶标,它是通过5种蛋白质Dph1至-5和仍未鉴定的酰胺化酶的作用在酵母中形成的。 Dph2和Dph5先前已确定。在这里,我们报告了剩余的三种酵母蛋白(Dph1,-3和-4)的鉴定,并表明所有五个Dph蛋白具有功能性(Dph1,-2,-3和-5)或序列(Dph4)哺乳动物的同系物。我们针对这些蛋白质(例如,人类蛋白质的HsDph1至-5)及其基于酵母命名法的基因提出了统一的命名法。我们显示Dph1和Dph2在序列上是同源的,但在功能上是独立的。先前鉴定为与酵母DPH2同源的人类肿瘤抑制基因OVCA1实际上是HsDPH1。我们显示HsDPH3是先前描述的人白喉毒素和假单胞菌外毒素A敏感性所需的基因1,并且DPH4编码CSL含锌指的DnaJ样蛋白。还讨论了这些基因的其他特征。白喉酰胺的生理功能及其普遍存在的基础仍是一个谜,但有证据表明,Dph1至-3在体内在多种细胞过程中作为蛋白质复合物起作用。

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