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Profiling of myristoylation in Toxoplasma gondii reveals an N-myristoylated protein important for host cell penetration

机译:在弓形虫弓形虫中的剖析显示出对宿主细胞渗透的n-myristoylated蛋白质重要性

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摘要

N-myristoylation is a ubiquitous class of protein lipidation across eukaryotes and N-myristoyl transferase (NMT) has been proposed as an attractive drug target in several pathogens. Myristoylation often primes for subsequent palmitoylation and stable membrane attachment, however, growing evidence suggests additional regulatory roles for myristoylation on proteins. Here we describe the myristoylated proteome of Toxoplasma gondii using chemoproteomic methods and show that a small-molecule NMT inhibitor developed against related Plasmodium spp. is also functional in Toxoplasma. We identify myristoylation on a transmembrane protein, the microneme protein 7 (MIC7), which enters the secretory pathway in an unconventional fashion with the myristoylated N-terminus facing the lumen of the micronemes. MIC7 and its myristoylation play a crucial role in the initial steps of invasion, likely during the interaction with and penetration of the host cell. Myristoylation of secreted eukaryotic proteins represents a substantial expansion of the functional repertoire of this co-translational modification.
机译:N-MyRistoylation是一类普遍存在的蛋白质脂质,在真核生物上,并且N-Myristoyl转移酶(NMT)已经提出了几种病原体中具有吸引力的药物靶标。 MyRistoylation通常用于随后的棕榈酰基和稳定的膜附着,然而,日益增长的证据表明蛋白质蛋白质的含量额外的调节作用。在这里,我们使用化学蛋白质方法描述弓形虫的MyRistoylated蛋白质组,并表明一种小分子NMT抑制剂与相关疟原虫SPP开发。在弓形上也是功能性的。我们识别跨膜蛋白的MyRistoylation,微米蛋白7(MIC7),其以非常规时的方式进入分泌途径,与面向微粒的内腔的MyRistoyaated n-terminus。 MIC7及其MyRistoylation在初始侵袭步骤中发挥至关重要的作用,可能在与宿主细胞的相互作用和渗透和渗透期间。分泌的真核蛋白的MyRistoylation表示该协同改性的功能性曲目的大量膨胀。

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