TUSK:调节锥虫表面蛋白丰度的泛素水解酶复合物

Kayo Yamada, Ning Zhang, Farzana K. Yaqub, M. Zoltner, Mark C. Field
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引用次数: 1

摘要

蛋白质水平的控制对于维持细胞稳态、协调分化过程中的变化和其他作用至关重要。在非洲锥虫中,表面蛋白有助于免疫逃避、药物敏感性和环境感知。锥虫表面主要由gpi锚定的变体表面糖蛋白主导,但其他gpi锚定和跨膜结构域蛋白存在,已知其作为营养受体和信号转导器的作用。在锥虫中,进化上保守的Usp7和Vdu1的去泛素酶同源物调节许多表面蛋白的丰富度,包括在免疫逃避和药物敏感性中起作用的不变性表面糖蛋白。在这里,我们确定了多个锥虫Skp1平行体,特别是一个发散平行体SkpZ。亲和分离和LCMSMS表明,SkpZ与TbUsp7和TbTpr86形成异三聚体复合物,TbTpr86是一种四肽重复蛋白。SkpZ的沉默降低了TbUsp7和TbTpr86的丰度,证实了两者之间的直接关联。此外,SkpZ敲低降低了多个跨膜结构域(TMD)蛋白的丰度,但增加了gpi锚定的表面蛋白水平。因此,TbTpr86、TbUsp7和SkpZ的异源三聚体复合体(TUSK)调节了一系列重要的锥虫表面蛋白的表达水平,介导了TMD和gpi锚定蛋白表达水平之间的协调。
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TUSK: a ubiquitin hydrolase complex modulating surface protein abundance in trypanosomes
Control of protein levels is vital to cellular homeostasis, for maintaining a steady state, to coordinate changes during differentiation and other roles. In African trypanosomes surface proteins contribute to immune evasion, drug sensitivity and environmental sensing. The trypanosome surface is dominated by the GPI-anchored variant surface glycoprotein, but additional GPI-anchored and trans-membrane domain proteins are present with known roles as nutrient receptors and signal transducers. The evolutionarily conserved deubiquitinase orthologs of Usp7 and Vdu1 in trypanosomes modulate abundance of many surface proteins, including the invariant surface glycoproteins, which have roles in immune evasion and drug sensitivity. Here we identify multiple trypanosome Skp1 paralogs and specifically a divergent paralog SkpZ. Affinity isolation and LCMSMS indicates that SkpZ forms a heterotrimeric complex with TbUsp7 and TbTpr86, a tetratricopeptide-repeat protein. Silencing SkpZ decreases TbUsp7 and TbTpr86 abundance, confirming a direct association. Further, SkpZ knockdown decreases the abundance of multiple trans-membrane domain (TMD) proteins but increases GPI-anchored surface protein levels. Hence, a heterotrimeric complex of TbTpr86, TbUsp7 and SkpZ (TUSK) regulates expression levels of a significant cohort of trypanosome surface proteins mediating coordination between TMD and GPI-anchored protein expression levels.
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