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Homology modeling provides insights into the binding mode of the PAAD/DAPIN/pyrin domain, a fourth member of the CARD/DD/DED domain family

机译:同源建模可深入了解PAAD / DAPIN / pyrin域的结合模式,PAAD / DAPIN / pyrin域是CARD / DD / DED域家族的第四位成员

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摘要

The PAAD/DAPIN/pyrin domain is the fourth member of the death domain superfamily, but unlike other members of this family, it is involved not only in apoptosis but also in innate immunity and several other processes. We have identified 40 PAAD domain-containing proteins by extensively searching the genomes of higher eukaryotes and viruses. Phylogenetic analyses suggest that there are five categories of PAAD domains that correlate with the domain architecture of the entire proteins. Homology models built on CARD and DD structures identified functionally important residues by studying conservation patterns on the surface of the models. Surface maps of each subfamily show different distributions of these residues, suggesting that domains from different subfamilies do not interact with each other, forming independent regulatory networks. Helix3 of PAAD is predicted to be critical for dimerization. Multiple alignment analysis and modeling suggest that it may be partly disordered, following a new paradigm for interaction proteins that are stabilized by protein–protein interactions.
机译:PAAD / DAPIN / pyrin结构域是死亡结构域超家族的第四个成员,但与该家族的其他成员不同,它不仅参与细胞凋亡,而且还参与先天免疫和其他一些过程。通过广泛搜索高级真核生物和病毒的基因组,我们已经鉴定出40种含PAAD结构域的蛋白质。系统发育分析表明,有五类PAAD域与整个蛋白质的域结构相关。建立在CARD和DD结构上的同源性模型通过研究模型表面的保守性模式来识别功能上重要的残基。每个亚科的表面图谱显示了这些残基的不同分布,这表明来自不同亚科的结构域不会彼此相互作用,从而形成独立的调控网络。预测PAAD的Helix3对于二聚化至关重要。多重比对分析和建模表明,对于相互作用蛋白通过蛋白质-蛋白质相互作用稳定的新范式而言,它可能部分无序。

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