The evolutionary history of the HUP domain

生物 核苷酸 NAD+激酶 腺苷酸化 遗传学 系统发育树 结合位点 计算生物学 进化生物学 生物化学 生物合成 基因
作者
Ita Gruic‐Sovulj,Liam M. Longo,Jagoda Jabłońska,Dan S. Tawfik
出处
期刊:Critical Reviews in Biochemistry and Molecular Biology [Informa]
卷期号:57 (1): 1-15 被引量:15
标识
DOI:10.1080/10409238.2021.1957764
摘要

Among the enzyme lineages that undoubtedly emerged prior to the last universal common ancestor is the so-called HUP, which includes Class I aminoacyl tRNA synthetases (AARSs) as well as enzymes mediating NAD, FAD, and CoA biosynthesis. Here, we provide a detailed analysis of HUP evolution, from emergence to structural and functional diversification. The HUP is a nucleotide binding domain that uniquely catalyzes adenylation via the release of pyrophosphate. In contrast to other ancient nucleotide binding domains with the αβα sandwich architecture, such as P-loop NTPases, the HUP’s most conserved feature is not phosphate binding, but rather ribose binding by backbone interactions to the tips of β1 and/or β4. Indeed, the HUP exhibits unusual evolutionary plasticity and, while ribose binding is conserved, the location and mode of binding to the base and phosphate moieties of the nucleotide, and to the substrate(s) reacting with it, have diverged with time, foremost along the emergence of the AARSs. The HUP also beautifully demonstrates how a well-packed scaffold combined with evolvable surface elements promotes evolutionary innovation. Finally, we offer a scenario for the emergence of the HUP from a seed βαβ fragment, and suggest that despite an identical architecture, the HUP and the Rossmann represent independent emergences.

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