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PAX蛋白及其重构的传奇故事。

PAX proteins and fables of their reconstruction.

作者信息

Underhill Darrell Alan

机构信息

Department of Oncology, School of Cancer, Engineering & Imaging Sciences, Faculty of Medicine & Dentistry, University of Alberta, 2328 Cross Cancer Institute, 11560 University Avenue, Edmonton, Alberta, Canada.

出版信息

Crit Rev Eukaryot Gene Expr. 2012;22(2):161-77. doi: 10.1615/critreveukargeneexpr.v22.i2.70.

Abstract

The PAX proteins derive their name from the "paired box," a region of homology first described between the Drosophila paired (Prd) and gooseberry (Gsb) proteins and later found to encode a sequence-specific DNA-binding activity. Both Prd and Gsb also contain a homeodomain, and this combination of DNA-binding domains is conserved in ancestral predecessors, reflecting an early "homeodomain-capturing" event. In addition, the prototypic PAX protein was thought to contain 2 additional features, namely the octapeptide (or eh1) motif and PHT (or OAR) domain-both modulate PAX regulatory activity but are not unique to the PAX family. Together with gene duplications and mutagenesis, a domain loss model accounts for the distinct architecture and sequence of extant PAX proteins. Despite the disparate evolutionary history of these 4 conserved motifs, there is a remarkable level of interplay that is modulated by discrete sequences elsewhere in the protein. Here, the implications with respect to the evolution of PAX protein structure and activity are discussed, it is suggested that the sum of these constituent domains is more than the contribution of individual parts. When combined with alternative splicing and posttranslational modifications, this model confers an extraordinary degree of functional diversity to even highly related PAX proteins.

摘要

PAX蛋白得名于“成对结构域”,这是一个同源区域,最初在果蝇的成对(Prd)蛋白和醋栗(Gsb)蛋白之间被描述,后来发现它编码一种序列特异性DNA结合活性。Prd和Gsb都还包含一个同源异型结构域,这种DNA结合结构域的组合在祖先前身中是保守的,反映了早期的“同源异型结构域捕获”事件。此外,原型PAX蛋白被认为还具有另外两个特征,即八肽(或eh1)基序和PHT(或OAR)结构域——两者都调节PAX的调控活性,但并非PAX家族所特有。与基因复制和诱变一起,结构域丢失模型解释了现存PAX蛋白独特的结构和序列。尽管这4个保守基序的进化历史不同,但蛋白质其他部位的离散序列会调节它们之间存在着显著程度的相互作用。在此,讨论了PAX蛋白结构和活性进化方面的影响,认为这些组成结构域的总和大于各个部分的贡献。当与可变剪接和翻译后修饰相结合时,该模型赋予了即使是高度相关的PAX蛋白非凡程度的功能多样性。

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