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成束和延伸ζ蛋白1和2:从结构灵活性到功能多样性

Fasciculation and elongation zeta proteins 1 and 2: From structural flexibility to functional diversity.

作者信息

Teixeira Mariana Bertini, Alborghetti Marcos Rodrigo, Kobarg Jörg

机构信息

Institute of Biology, Department of Biochemistry and Tissue Biology, University of Campinas, Campinas 13083-862, Brazil.

Department of Cell Biology, University of Brasilia, Brasilia 70919-970, Brazil.

出版信息

World J Biol Chem. 2019 Feb 21;10(2):28-43. doi: 10.4331/wjbc.v10.i2.28.

Abstract

Fasciculation and elongation zeta/zygin (FEZ) proteins are a family of hub proteins and share many characteristics like high connectivity in interaction networks, they are involved in several cellular processes, evolve slowly and in general have intrinsically disordered regions. In 1985, gene was firstly described and involved in axonal growth in , and in 1997 Bloom and Horvitz enrolled also the human homologues genes, and , in this process. While nematodes possess one gene (), mammalians have one more copy ( and ). Several animal models have been used to study FEZ family functions like: , and human cells. Complementation assays were performed and demonstrated the function conservation between paralogues. Human FEZ1 protein is more studied followed by UNC-76 and FEZ2 proteins, respectively. While FEZ1 and UNC-76 shared interaction partners, FEZ2 evolved and increased the number of protein-protein interactions (PPI) with cytoplasmatic partners. FEZ proteins are implicated in intracellular transport, acting as bivalent cargo transport adaptors in kinesin-mediated movement. Especially in light of this cellular function, this family of proteins has been involved in several processes like neuronal development, neurological disorders, viral infection and autophagy. However, nuclear functions of FEZ proteins have been explored as well, due to high content of PPI with nuclear proteins, correlating FEZ1 expression to and gene regulation and retinoic acid signaling. These recent findings open new avenue to study FEZ proteins functions and its involvement in already described processes. This review intends to reunite aspects of evolution, structure, interaction partners and function of FEZ proteins and correlate them to physiological and pathological processes.

摘要

成束与延伸ζ/合胞素(FEZ)蛋白是一类枢纽蛋白,具有许多共同特征,如在相互作用网络中具有高连接性,参与多种细胞过程,进化缓慢,且一般具有内在无序区域。1985年,该基因首次被描述,并参与了秀丽隐杆线虫的轴突生长,1997年,布卢姆和霍维茨也将人类同源基因FEZ1和FEZ2纳入这一过程。线虫只有一个FEZ基因(unc-76),而哺乳动物有两个拷贝(FEZ1和FEZ2)。已经使用了几种动物模型来研究FEZ家族的功能,如秀丽隐杆线虫、果蝇和人类细胞。进行了互补试验,证明了旁系同源物之间的功能保守性。对人类FEZ1蛋白的研究最多,其次是UNC-76和FEZ2蛋白。虽然FEZ1和UNC-76共享相互作用伙伴,但FEZ2发生了进化,并增加了与细胞质伙伴的蛋白质-蛋白质相互作用(PPI)数量。FEZ蛋白参与细胞内运输,在驱动蛋白介导的运动中作为二价货物运输衔接蛋白发挥作用。特别是鉴于这种细胞功能,该蛋白家族参与了多个过程,如神经元发育、神经疾病、病毒感染和自噬。然而,由于与核蛋白的PPI含量高,FEZ蛋白的核功能也得到了探索,这将FEZ1的表达与HOXA和HOXB基因调控以及视黄酸信号传导联系起来。这些最新发现为研究FEZ蛋白的功能及其在已描述过程中的作用开辟了新途径。本综述旨在汇总FEZ蛋白的进化、结构、相互作用伙伴和功能等方面,并将它们与生理和病理过程联系起来。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/b430/6388297/6b47106b81c9/WJBC-10-28-g001.jpg

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