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秀丽隐杆线虫 PDZ 结构域的结构特征与计算分析。

Structural characterization and computational analysis of PDZ domains in Monosiga brevicollis.

机构信息

Department of Chemistry, Western Washington University, Bellingham, Washington, USA.

Institute for Protein Innovation, Boston, Massachusetts, USA.

出版信息

Protein Sci. 2020 Nov;29(11):2226-2244. doi: 10.1002/pro.3947. Epub 2020 Sep 25.

Abstract

Identification of the molecular networks that facilitated the evolution of multicellular animals from their unicellular ancestors is a fundamental problem in evolutionary cellular biology. Choanoflagellates are recognized as the closest extant nonmetazoan ancestors to animals. These unicellular eukaryotes can adopt a multicellular-like "rosette" state. Therefore, they are compelling models for the study of early multicellularity. Comparative studies revealed that a number of putative human orthologs are present in choanoflagellate genomes, suggesting that a subset of these genes were necessary for the emergence of multicellularity. However, previous work is largely based on sequence alignments alone, which does not confirm structural nor functional similarity. Here, we focus on the PDZ domain, a peptide-binding domain which plays critical roles in myriad cellular signaling networks and which underwent a gene family expansion in metazoan lineages. Using a customized sequence similarity search algorithm, we identified 178 PDZ domains in the Monosiga brevicollis proteome. This includes 11 previously unidentified sequences, which we analyzed using Rosetta and homology modeling. To assess conservation of protein structure, we solved high-resolution crystal structures of representative M. brevicollis PDZ domains that are homologous to human Dlg1 PDZ2, Dlg1 PDZ3, GIPC, and SHANK1 PDZ domains. To assess functional conservation, we calculated binding affinities for mbGIPC, mbSHANK1, mbSNX27, and mbDLG-3 PDZ domains from M. brevicollis. Overall, we find that peptide selectivity is generally conserved between these two disparate organisms, with one possible exception, mbDLG-3. Overall, our results provide novel insight into signaling pathways in a choanoflagellate model of primitive multicellularity.

摘要

从单细胞祖先进化为多细胞动物的分子网络的鉴定是进化细胞生物学的一个基本问题。领鞭毛虫被认为是与动物最接近的现存非动物祖先。这些单细胞真核生物可以采用类似于多细胞的“玫瑰花结”状态。因此,它们是研究早期多细胞性的引人注目的模型。比较研究表明,在领鞭毛虫基因组中存在许多假定的人类直系同源物,这表明这些基因中的一部分对于多细胞性的出现是必要的。然而,以前的工作主要基于序列比对,这并不能确认结构和功能的相似性。在这里,我们专注于 PDZ 结构域,这是一种肽结合结构域,在众多细胞信号网络中发挥着关键作用,并且在后生动物谱系中经历了基因家族的扩张。使用定制的序列相似性搜索算法,我们在 Monosiga brevicollis 蛋白质组中鉴定出 178 个 PDZ 结构域。这包括 11 个以前未识别的序列,我们使用 Rosetta 和同源建模对其进行了分析。为了评估蛋白质结构的保守性,我们解决了代表 M. brevicollis PDZ 结构域的高分辨率晶体结构,这些结构域与人类 Dlg1 PDZ2、Dlg1 PDZ3、GIPC 和 SHANK1 PDZ 结构域同源。为了评估功能保守性,我们计算了来自 M. brevicollis 的 mbGIPC、mbSHANK1、mbSNX27 和 mbDLG-3 PDZ 结构域的结合亲和力。总体而言,我们发现这些截然不同的生物体之间的肽选择性通常是保守的,只有一个可能的例外,即 mbDLG-3。总体而言,我们的结果为原始多细胞性的领鞭毛虫模型中的信号通路提供了新的见解。

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