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通过鱼类与哺乳动物的比较揭示朊病毒蛋白结构域的不同进化以及多普蛋白和朊病毒相关基因座的不同起源。

Disparate evolution of prion protein domains and the distinct origin of Doppel- and prion-related loci revealed by fish-to-mammal comparisons.

作者信息

Rivera-Milla Eric, Oidtmann Birgit, Panagiotidis Cynthia H, Baier Michael, Sklaviadis Theodoros, Hoffmann Rudolf, Zhou Yi, Solis Gonzalo P, Stuermer Claudia A O, Málaga-Trillo Edward

机构信息

Department of Biology, University of Konstanz, Konstanz, Germany.

出版信息

FASEB J. 2006 Feb;20(2):317-9. doi: 10.1096/fj.05-4279fje. Epub 2005 Dec 13.

DOI:10.1096/fj.05-4279fje
PMID:16352647
Abstract

Prions result from the misfolding and selective accumulation of the host-encoded prion protein (PrP) in the brain. Despite intensive research on mammalian models, basic questions about the biological role of PrP and the evolutionary origin of prion disease remain unanswered. Following our previous identification of novel fish PrP homologues, here we generated new fish PrP sequences and performed genomic analysis to demonstrate the existence of two homologous PrP loci in bony fish, which display extensive molecular variation and are highly expressed in adult and developing fish brains. The fish PrP genomic regions contain PrP-related loci directly downstream of each PrP locus, suggesting an independent origin of prion-related proteins in fish and mammals. Our structural prediction analysis uncovers a conserved molecular "bauplan" for all vertebrate PrPs. The C- and N-terminal protein domains have evolved independently from one another, the former having retained its basic globular structure despite high sequence divergence and the latter having undergone differential expansion-degeneration cycles in its repetitive domains. Our evolutionary analysis redefines fundamental concepts on the functional significance of PrP domains and opens up new possibilities for the experimental analysis of prion misfolding and neurodegeneration in a non-mammalian model like the zebrafish.

摘要

朊病毒是由宿主编码的朊病毒蛋白(PrP)在大脑中错误折叠和选择性积累产生的。尽管对哺乳动物模型进行了深入研究,但关于PrP的生物学作用以及朊病毒疾病的进化起源等基本问题仍未得到解答。继我们之前鉴定出新型鱼类PrP同源物之后,我们在此生成了新的鱼类PrP序列并进行了基因组分析,以证明硬骨鱼中存在两个同源PrP基因座,它们表现出广泛的分子变异且在成年鱼和发育中的鱼脑中高度表达。鱼类PrP基因组区域在每个PrP基因座的直接下游都包含与PrP相关的基因座,这表明鱼类和哺乳动物中朊病毒相关蛋白具有独立的起源。我们的结构预测分析揭示了所有脊椎动物PrP的保守分子“蓝图”。C端和N端蛋白结构域彼此独立进化,前者尽管序列差异很大但仍保留了其基本的球状结构,而后者在其重复结构域中经历了不同的扩增 - 退化循环。我们的进化分析重新定义了关于PrP结构域功能意义的基本概念,并为在斑马鱼等非哺乳动物模型中对朊病毒错误折叠和神经退行性变进行实验分析开辟了新的可能性。

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