The nascent polypeptide-associated complex (NAC) coordinates enzymatic modifications and membrane targeting of nascent chains during translation. While the role of NAC as a dynamic hub for other factors is well established, its direct role in co-translational folding is unclear. By proteome-wide profiling of co-translational NAC interactions in human cells, we found that NAC recognizes emerging segments enriched in hydrophobicity and α-helical propensity within folded domains of cytonuclear proteins. Single-molecule and structural analyses reveal that NAC, via its β-barrel domain, dynamically interacts with nascent chains at the ribosomal tunnel exit and is capable of promoting on-pathway folding. Compartment-specific nascent chain interactions of NAC further elucidate its role in targeting to the endoplasmic reticulum and in mitochondrial membrane protein biogenesis. Together, these findings show that human NAC acts as a bona fide co-translational chaperone that directly promotes early protein folding at the ribosomal tunnel exit, expanding its functional repertoire in protein biogenesis.
NAC promotes co-translational protein folding at the ribosomal tunnel exit.
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作者:Santos Jaime, Günnigmann Manuel, Gora Radoslaw J, Iljina Marija, Predin Masa, Kotan Ilgin Eser, De Pratiman, Choudhary Dhawal, Jang Juwon, Tippmann Frank, Hins Christopher, Ban Nenad, Tans Sander J, Shan Shu-Ou, Kramer Günter, Bukau Bernd
| 期刊: | Molecular Cell | 影响因子: | 16.600 |
| 时间: | 2026 | 起止号: | 2026 Apr 2; 86(7):1311-1326 |
| doi: | 10.1016/j.molcel.2026.02.022 | ||
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