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Intrinsic Disorder of the C-Terminal Domain of Drosophila Methoprene-Tolerant Protein

机译:果蝇甲基戊二烯耐受蛋白C末端结构域的内在障碍

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摘要

Methoprene tolerant protein (Met) has recently been confirmed as the long-sought juvenile hormone (JH) receptor. This protein plays a significant role in the cross-talk of the 20-hydroxyecdysone (20E) and JH signalling pathways, which are important for control of insect development and maturation. Met belongs to the basic helix-loop-helix/Per-Arnt-Sim (bHLH-PAS) family of transcription factors. In these proteins, bHLH domains are typically responsible for DNA binding and dimerization, whereas the PAS domains are crucial for the choice of dimerization partner and the specificity of target gene activation. The C-terminal region is usually responsible for the regulation of protein complex activity. The sequence of the Met C-terminal region (MetC) is not homologous to any sequence deposited in the Protein Data Bank (PDB) and has not been structurally characterized to date. In this study, we show that the MetC exhibits properties typical for an intrinsically disordered protein (IDP). The final averaged structure obtained with small angle X-ray scattering (SAXS) experiments indicates that intrinsically disordered MetC exists in an extended conformation. This extended shape and the long unfolded regions characterise proteins with high flexibility and dynamics. Therefore, we suggest that the multiplicity of conformations adopted by the disordered MetC is crucial for its activity as a biological switch modulating the cross-talk of different signalling pathways in insects.
机译:近期,已确认甲氧戊丁耐受蛋白(Met)是长期寻求的少年激素(JH)受体。该蛋白在20-羟基蜕皮激素(20E)和JH信号传导通路的相互作用中起重要作用,这对于控制昆虫的发育和成熟很重要。 Met属于转录因子的基本螺旋-环-螺旋/ Per-Arnt-Sim(bHLH-PAS)家族。在这些蛋白质中,bHLH结构域通常负责DNA结合和二聚化,而PAS结构域对于二聚化伴侣的选择和靶基因激活的特异性至关重要。 C末端区域通常负责蛋白质复合物活性的调节。 Met C末端区域(MetC)的序列与蛋白质数据库(PDB)中存储的任何序列都不同源,并且迄今为止尚未进行结构表征。在这项研究中,我们表明MetC表现出固有的无序蛋白(IDP)的典型属性。通过小角度X射线散射(SAXS)实验获得的最终平均结构表明,固有无序的MetC存在于扩展构象中。这种延伸的形状和较长的未折叠区域表征具有高柔韧性和动态性的蛋白质。因此,我们建议无序的MetC所采用的构象的多样性对于其作为调节昆虫中不同信号通路的串扰的生物开关的活性至关重要。

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