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重新审视真核生物起始因子 4E 同源物在动基体生物中的 mRNA 帽结合蛋白的结合特征。

Taking a re-look at cap-binding signatures of the mRNA cap-binding protein eIF4E orthologues in trypanosomatids.

机构信息

Translational Health Science and Technology Institute, NCR Biotech Science Cluster, 3rd Milestone, Faridabad-Gurgaon Expressway, PO Box #04, Faridabad, Haryana, 121001, India.

出版信息

Mol Cell Biochem. 2021 Feb;476(2):1037-1049. doi: 10.1007/s11010-020-03970-w. Epub 2020 Nov 10.

DOI:10.1007/s11010-020-03970-w
PMID:33169189
Abstract

Protein translation leading to polypeptide synthesis involves three distinct events, namely, initiation, elongation, and termination. Translation initiation is a multi-step process that is carried out by ribosomes on the mRNA with the assistance of a large number of proteins called translation initiation factors. Trypanosomatids are kinetoplastidas (flagellated protozoans), some of which cause acute disease syndromes in humans. Vector-borne transmission of protozoan parasites like Leishmania and Trypanosoma causes diseases that affect a large section of the world population and lead to significant morbidity and mortality. The mechanisms of translation initiation in higher eukaryotes are relatively well understood. However, structural and functional conservation of initiation factors in trypanosomatids are only beginning to be understood. Studies carried out so far suggests that at least in Leishmania and Trypanosoma eIF4E function may not be restricted to canonical translation initiation and some of the homologues may have alternate/non-canonical functions. Nonetheless, all of them bind the cap analogs, albeit with different efficiencies, indicating that this property may play an important role in the functionality of eIF4Es. Here, I give a brief background of trypanosomatid eIF4Es and revisit the cap-binding signatures of eIF4E orthologues in trypanosomatids, whose genome sequences are available, in detail, in comparison to human eIF4E1 and Trypanosoma cruzi eIF4E5, with an expanded list of members of this group in light of newer findings. The group 1 and 2 eIF4Es may use either a variation of heIF4E1 or T. cruzi eIF4E5 cap-4-binding signatures, while eIF4E5 and eIF4E6 use distinct amino acid contacts.

摘要

蛋白质翻译导致多肽合成涉及三个不同的事件,即起始、延伸和终止。翻译起始是一个多步骤的过程,由核糖体在 mRNA 上进行,在大量称为翻译起始因子的蛋白质的协助下进行。动基体生物(鞭毛原生动物)是一类原生动物,其中一些会导致人类急性疾病综合征。像利什曼原虫和锥虫这样的原生动物寄生虫通过媒介传播,导致影响世界很大一部分人口的疾病,并导致严重的发病率和死亡率。高等真核生物翻译起始的机制相对较好理解。然而,动基体生物中起始因子的结构和功能保守性才刚刚开始被理解。迄今为止的研究表明,至少在利什曼原虫和锥虫中,eIF4E 的功能可能不限于经典翻译起始,并且一些同源物可能具有替代/非经典功能。尽管如此,它们都与帽类似物结合,尽管效率不同,这表明该特性可能在 eIF4E 的功能中发挥重要作用。在这里,我简要介绍了动基体生物的 eIF4E,并详细回顾了可用于比较的动基体生物中 eIF4E 同源物的帽结合特征,这些生物的基因组序列可用,与人类 eIF4E1 和锥虫 eIF4E5 相比,在根据最新发现扩展了该组的成员列表后。组 1 和 2 eIF4E 可能使用 heIF4E1 或 T. cruzi eIF4E5 帽-4 结合特征的变体,而 eIF4E5 和 eIF4E6 使用不同的氨基酸接触。

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Crystal structure of the Trypanosoma cruzi EIF4E5 translation factor homologue in complex with mRNA cap-4.克氏锥虫 EIF4E5 翻译因子同源物与 mRNA 帽-4 复合物的晶体结构
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