Nature Communications (Oct 2024)

Non-averaged single-molecule tertiary structures reveal RNA self-folding through individual-particle cryo-electron tomography

  • Jianfang Liu,
  • Ewan K. S. McRae,
  • Meng Zhang,
  • Cody Geary,
  • Ebbe Sloth Andersen,
  • Gang Ren

DOI
https://doi.org/10.1038/s41467-024-52914-1
Journal volume & issue
Vol. 15, no. 1
pp. 1 – 18

Abstract

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Abstract Large-scale and continuous conformational changes in the RNA self-folding process present significant challenges for structural studies, often requiring trade-offs between resolution and observational scope. Here, we utilize individual-particle cryo-electron tomography (IPET) to examine the post-transcriptional self-folding process of designed RNA origami 6-helix bundle with a clasp helix (6HBC). By avoiding selection, classification, averaging, or chemical fixation and optimizing cryo-ET data acquisition parameters, we reconstruct 120 three-dimensional (3D) density maps from 120 individual particles at an electron dose of no more than 168 e–Å−2, achieving averaged resolutions ranging from 23 to 35 Å, as estimated by Fourier shell correlation (FSC) at 0.5. Each map allows us to identify distinct RNA helices and determine a unique tertiary structure. Statistical analysis of these 120 structures confirms two reported conformations and reveals a range of kinetically trapped, intermediate, and highly compacted states, demonstrating a maturation folding landscape likely driven by helix-helix compaction interactions.