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联合结构与功能注释方法为 SPD-2 的功能多样性提供了机制见解。

A combined and approach to the structure-function annotation of SPD-2 provides mechanistic insight into its functional diversity.

机构信息

Department of Biology, City University of New York, Brooklyn College, New York, NY, USA.

Department of Biology, The Graduate Center at City University of New York, New York, NY, USA.

出版信息

Cell Cycle. 2022 Sep;21(18):1958-1979. doi: 10.1080/15384101.2022.2078458. Epub 2022 Jun 9.

DOI:10.1080/15384101.2022.2078458
PMID:35678569
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC9415446/
Abstract

Centrosomes are organelles that function as hubs of microtubule nucleation and organization, with key roles in organelle positioning, asymmetric cell division, ciliogenesis, and signaling. Aberrant centrosome number, structure or function is linked to neurodegenerative diseases, developmental abnormalities, ciliopathies, and tumor development. A major regulator of centrosome biogenesis and function in is the conserved Spindle-defective protein 2 (SPD-2), a homolog of the human CEP-192 protein. CeSPD-2 is required for centrosome maturation, centriole duplication, spindle assembly and possibly cell polarity establishment. Despite its importance, the specific molecular mechanism of CeSPD-2 regulation and function is poorly understood. Here, we combined computational analysis with cell biology approaches to uncover possible structure-function relationships of CeSPD-2 that may shed mechanistic light on its function. Domain prediction analysis corroborated and refined previously identified coiled-coils and ASH (Aspm-SPD-2 Hydin) domains and identified new domains: a GEF domain, an Ig-like domain, and a PDZ-like domain. In addition to these predicted structural features, CeSPD-2 is also predicted to be intrinsically disordered. Surface electrostatic maps identified a large basic region unique to the ASH domain of CeSPD-2. This basic region overlaps with most of the residues predicted to be involved in protein-protein interactions. , ASH::GFP localized to centrosomes and centrosome-associated microtubules. Our analysis groups ASH domains, PapD, Usher chaperone domains, and Major Sperm Protein (MSP) domains into a single superfold within the larger Immunoglobulin superfamily. This study lays the groundwork for designing rational hypothesis-based experiments to uncover the mechanisms of CeSPD-2 function AIR, Aurora kinase; ASH, Aspm-SPD-2 Hydin; ASP, Abnormal Spindle Protein; ASPM, Abnormal Spindle-like Microcephaly-associated Protein; CC, coiled-coil; CDK, Cyclin-dependent Kinase; Ce, Caenorhabditis elegans; CEP, Centrosomal Protein; CPAP, centrosomal P4.1-associated protein; D, Drosophila; GAP, GTPase activating protein; GEF, GTPase guanine nucleotide exchange factor; Hs, Homo sapiens/Human; Ig, Immunoglobulin; MAP, Microtubule associated Protein; MSP, Major Sperm Protein; MDP, Major Sperm Domain-Containing Protein; OCRL-1, Golgi endocytic trafficking protein Inositol polyphosphate 5-phosphatase; PAR, abnormal embryonic PARtitioning of the cytosol; PCM, Pericentriolar material; PCMD, pericentriolar matrix deficient; PDZ, PSD95/Dlg-1/zo-1; PLK, Polo like kinase; RMSD, Root Mean Square Deviation; SAS, Spindle assembly abnormal proteins; SPD, Spindle-defective protein; TRAPP, TRAnsport Protein Particle; Xe, Xenopus; ZYG, zygote defective protein.

摘要

中心体是作为微管成核和组织的中心发挥作用的细胞器,在细胞器定位、不对称细胞分裂、纤毛发生和信号转导中具有关键作用。中心体数量、结构或功能异常与神经退行性疾病、发育异常、纤毛病和肿瘤发展有关。Spindle-defective protein 2(SPD-2)是一种保守的纺锤体缺陷蛋白,是人类 CEP-192 蛋白的同源物,是调节中心体生物发生和功能的主要调节剂。CeSPD-2 对于中心体成熟、中心粒复制、纺锤体组装和可能的细胞极性建立是必需的。尽管它很重要,但 CeSPD-2 调节和功能的具体分子机制仍知之甚少。在这里,我们结合计算分析和细胞生物学方法来揭示 CeSPD-2 的可能结构-功能关系,这可能为其功能提供机制上的启示。结构域预测分析证实并细化了先前鉴定的卷曲螺旋和 ASH(Aspm-SPD-2 Hydin)结构域,并鉴定了新的结构域:GEF 结构域、免疫球蛋白样结构域和 PDZ 样结构域。除了这些预测的结构特征外,CeSPD-2 也被预测为固有无序的。表面静电图谱确定了 CeSPD-2 的 ASH 结构域中独特的大碱性区域。该碱性区域与大多数预测参与蛋白-蛋白相互作用的残基重叠。CeSPD-2 中的 GFP 定位于中心体和中心体相关微管。我们的分析将 ASH 结构域、PapD、Usher 伴侣蛋白结构域和主要精子蛋白(MSP)结构域归入免疫球蛋白超家族内的单个超折叠中。这项研究为设计基于合理假设的实验奠定了基础,以揭示 CeSPD-2 功能的机制。AIR、Aurora 激酶;ASH、Aspm-SPD-2 Hydin;ASP、异常纺锤体蛋白;ASPM、异常纺锤体样小头畸形相关蛋白;CC、卷曲螺旋;CDK、周期蛋白依赖性激酶;Ce、秀丽隐杆线虫;CEP、中心体蛋白;CPAP、中心体 P4.1 相关蛋白;D、果蝇;GAP、GTPase 激活蛋白;GEF、GTPase 鸟嘌呤核苷酸交换因子;Hs、Homo sapiens/Human;Ig、免疫球蛋白;MAP、微管相关蛋白;MSP、主要精子蛋白;MDP、主要精子结构域包含蛋白;OCRL-1、高尔基体内吞运输蛋白肌醇多磷酸 5-磷酸酶;PAR、胚胎异常 PAR 细胞质分区;PCM、中心粒周围物质;PCMD、中心粒基质缺乏;PDZ、PSD95/Dlg-1/zo-1;PLK、Polo 样激酶;RMSD、均方根偏差;SAS、纺锤体组装异常蛋白;SPD、纺锤体缺陷蛋白;TRAPP、转运蛋白颗粒;Xe、非洲爪蟾;ZYG、合子缺陷蛋白。

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