| Literature DB >> 28723557 |
Ivan B Lomakin1, Elena A Stolboushkina2, Anand T Vaidya3, Chenguang Zhao3, Maria B Garber4, Sergey E Dmitriev5, Thomas A Steitz6.
Abstract
The repertoire of the density-regulated protein (DENR) and the malignant T cell-amplified sequence 1 (MCT-1/MCTS1) oncoprotein was recently expanded to include translational control of a specific set of cancer-related mRNAs. DENR and MCT-1 form the heterodimer, which binds to the ribosome and operates at both translation initiation and reinitiation steps, though by a mechanism that is yet unclear. Here, we determined the crystal structure of the human small ribosomal subunit in complex with DENR-MCT-1. The structure reveals the location of the DENR-MCT-1 dimer bound to the small ribosomal subunit. The binding site of the C-terminal domain of DENR on the ribosome has a striking similarity with those of canonical initiation factor 1 (eIF1), which controls the fidelity of translation initiation and scanning. Our findings elucidate how the DENR-MCT-1 dimer interacts with the ribosome and have functional implications for the mechanism of unconventional translation initiation and reinitiation.Entities:
Keywords: density regulated protein; malignant T cell-amplified sequence 1; protein synthesis; ribosome; translation initiation; translation reinitiation
Mesh:
Substances:
Year: 2017 PMID: 28723557 PMCID: PMC5551485 DOI: 10.1016/j.celrep.2017.06.025
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423