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脊椎动物CPEB蛋白家族中低复杂性区域的趋异进化。

Divergent evolution of low-complexity regions in the vertebrate CPEB protein family.

作者信息

Vaglietti Serena, Boggio Bozzo Stefania, Ghirardi Mirella, Fiumara Ferdinando

机构信息

"Rita Levi-Montalcini" Department of Neuroscience, University of Turin, Turin, Italy.

出版信息

Front Bioinform. 2025 Mar 20;5:1491735. doi: 10.3389/fbinf.2025.1491735. eCollection 2025.

Abstract

The (CPEBs) are a family of translational regulators involved in multiple biological processes, including memory-related synaptic plasticity. In vertebrates, four paralogous genes (CPEB1-4) encode proteins with phylogenetically conserved C-terminal RNA-binding domains and variable N-terminal regions (NTRs). The CPEB NTRs are characterized by low-complexity regions (LCRs), including homopolymeric amino acid repeats (AARs), and have been identified as mediators of liquid-liquid phase separation (LLPS) and prion-like aggregation. After their appearance following gene duplication, the four paralogous CPEB proteins functionally diverged in terms of activation mechanisms and modes of mRNA binding. The paralog-specific NTRs may have contributed substantially to such functional diversification but their evolutionary history remains largely unexplored. Here, we traced the evolution of vertebrate CPEBs and their LCRs/AARs focusing on primary sequence composition, complexity, repetitiveness, and their possible functional impact on LLPS propensity and prion-likeness. We initially defined these composition- and function-related quantitative parameters for the four human CPEB paralogs and then systematically analyzed their evolutionary variation across more than 500 species belonging to nine major clades of different stem age, from Chondrichthyes to Euarchontoglires, along the vertebrate lineage. We found that the four CPEB proteins display highly divergent, paralog-specific evolutionary trends in composition- and function-related parameters, primarily driven by variation in their LCRs/AARs and largely related to clade stem ages. These findings shed new light on the molecular and functional evolution of LCRs in the CPEB protein family, in both quantitative and qualitative terms, highlighting the emergence of CPEB2 as a proline-rich prion-like protein in younger vertebrate clades, including Primates.

摘要

细胞质多聚腺苷酸化元件结合蛋白(CPEBs)是一类参与多种生物学过程的翻译调节因子,包括与记忆相关的突触可塑性。在脊椎动物中,四个旁系同源基因(CPEB1 - 4)编码的蛋白质具有系统发育上保守的C端RNA结合结构域和可变的N端区域(NTRs)。CPEB的NTRs以低复杂性区域(LCRs)为特征,包括同聚氨基酸重复序列(AARs),并且已被确定为液 - 液相分离(LLPS)和类朊病毒聚集的介质。在基因复制后出现后,这四个旁系同源CPEB蛋白在激活机制和mRNA结合模式方面功能发生了分化。旁系同源特异性的NTRs可能在很大程度上促成了这种功能多样化,但其进化历史在很大程度上仍未被探索。在这里,我们追踪了脊椎动物CPEBs及其LCRs/AARs的进化,重点关注一级序列组成、复杂性、重复性以及它们对LLPS倾向和类朊病毒特性可能的功能影响。我们首先为四个人类CPEB旁系同源物定义了这些与组成和功能相关的定量参数,然后系统地分析了它们在沿着脊椎动物谱系从软骨鱼到真灵长总目九个不同茎龄的主要进化枝的500多个物种中的进化变异。我们发现,这四种CPEB蛋白在与组成和功能相关的参数上表现出高度不同的、旁系同源特异性的进化趋势,主要由它们的LCRs/AARs的变异驱动,并且在很大程度上与进化枝的茎龄有关。这些发现从定量和定性角度为CPEB蛋白家族中LCRs的分子和功能进化提供了新的见解,突出了CPEB2作为富含脯氨酸的类朊病毒蛋白在包括灵长类在内的较年轻脊椎动物进化枝中的出现。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6404/11965684/c9a2573582f3/fbinf-05-1491735-g001.jpg

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