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Adrien Chauvier, Jason C. Porta, Indrajit Deb, Emily Ellinger, Katarina Meze, Aaron T. Frank, Melanie D. Ohi (Lead / Corresponding author), Nils G. Walter (Lead / Corresponding author)
Research output: Contribution to journal › Article › peer-review
Folding of nascent transcripts can be modulated by the RNA polymerase (RNAP) that carries out their transcription, and vice versa. A pause of RNAP during transcription of a preQ1 riboswitch (termed que-PEC) is stabilized by a previously characterized template consensus sequence and the ligand-free conformation of the nascent RNA. Ligand binding to the riboswitch induces RNAP pause release and downstream transcription termination; however, the mechanism by which riboswitch folding modulates pausing is unclear. Here, we report single-particle cryo-electron microscopy reconstructions of que-PEC in ligand-free and ligand-bound states. In the absence of preQ1, the RNA transcript is in an unexpected hyper-translocated state, preventing downstream nucleotide incorporation. Strikingly, on ligand binding, the riboswitch rotates around its helical axis, expanding the surrounding RNAP exit channel and repositioning the transcript for elongation. Our study reveals the tight coupling by which nascent RNA structures and their ligands can functionally regulate the macromolecular transcription machinery.
Original language | English |
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Pages (from-to) | 902–913 |
Number of pages | 12 |
Journal | Nature Structural & Molecular Biology |
Volume | 30 |
Issue number | 7 |
Early online date | 1 Jun 2023 |
DOIs | |
Publication status | Published - Jul 2023 |
Research output: Working paper/Preprint › Preprint