Co-translational assembly of mammalian nuclear multisubunit complexes

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作者
Ivanka Kamenova
Pooja Mukherjee
Sascha Conic
Florian Mueller
Farrah El-Saafin
Paul Bardot
Jean-Marie Garnier
Doulaye Dembele
Simona Capponi
H. T. Marc Timmers
Stéphane D. Vincent
László Tora
机构
[1] Institut de Génétique et de Biologie Moléculaire et Cellulaire,Computational Imaging & Modeling Unit, Institut Pasteur
[2] Centre National de la Recherche Scientifique (UMR7104),German Cancer Consortium (DKTK) partner site Freiburg, German Cancer Research, Center (DKFZ) and Department of Urology
[3] Institut National de la Santé et de la Recherche Médicale (U1258),undefined
[4] Université de Strasbourg,undefined
[5] Département Biologie Cellulaire et Infections,undefined
[6] Medical Center-University of Freiburg,undefined
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摘要
Cells dedicate significant energy to build proteins often organized in multiprotein assemblies with tightly regulated stoichiometries. As genes encoding subunits assembling in a multisubunit complex are dispersed in the genome of eukaryotes, it is unclear how these protein complexes assemble. Here, we show that mammalian nuclear transcription complexes (TFIID, TREX-2 and SAGA) composed of a large number of subunits, but lacking precise architectural details are built co-translationally. We demonstrate that dimerization domains and their positions in the interacting subunits determine the co-translational assembly pathway (simultaneous or sequential). The lack of co-translational interaction can lead to degradation of the partner protein. Thus, protein synthesis and complex assembly are linked in building mammalian multisubunit complexes, suggesting that co-translational assembly is a general principle in mammalian cells to avoid non-specific interactions and protein aggregation. These findings will also advance structural biology by defining endogenous co-translational building blocks in the architecture of multisubunit complexes.
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