Author
Listed:
- Seiichi Hirano
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Kalli Kappel
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Han Altae-Tran
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Guilhem Faure
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Max E. Wilkinson
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Soumya Kannan
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- F. Esra Demircioglu
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Rui Yan
(Howard Hughes Medical Institute, Janelia Research Campus)
- Momoko Shiozaki
(Howard Hughes Medical Institute, Janelia Research Campus)
- Zhiheng Yu
(Howard Hughes Medical Institute, Janelia Research Campus)
- Kira S. Makarova
(National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health)
- Eugene V. Koonin
(National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health)
- Rhiannon K. Macrae
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
- Feng Zhang
(Broad Institute of MIT and Harvard
McGovern Institute for Brain Research at MIT
Massachusetts Institute of Technology
Massachusetts Institute of Technology)
Abstract
RNA-guided systems, such as CRISPR–Cas, combine programmable substrate recognition with enzymatic function, a combination that has been used advantageously to develop powerful molecular technologies1,2. Structural studies of these systems have illuminated how the RNA and protein jointly recognize and cleave their substrates, guiding rational engineering for further technology development3. Recent work identified a new class of RNA-guided systems, termed OMEGA, which include IscB, the likely ancestor of Cas9, and the nickase IsrB, a homologue of IscB lacking the HNH nuclease domain4. IsrB consists of only around 350 amino acids, but its small size is counterbalanced by a relatively large RNA guide (roughly 300-nt ωRNA). Here, we report the cryogenic-electron microscopy structure of Desulfovirgula thermocuniculi IsrB (DtIsrB) in complex with its cognate ωRNA and a target DNA. We find the overall structure of the IsrB protein shares a common scaffold with Cas9. In contrast to Cas9, however, which uses a recognition (REC) lobe to facilitate target selection, IsrB relies on its ωRNA, part of which forms an intricate ternary structure positioned analogously to REC. Structural analyses of IsrB and its ωRNA as well as comparisons to other RNA-guided systems highlight the functional interplay between protein and RNA, advancing our understanding of the biology and evolution of these diverse systems.
Suggested Citation
Seiichi Hirano & Kalli Kappel & Han Altae-Tran & Guilhem Faure & Max E. Wilkinson & Soumya Kannan & F. Esra Demircioglu & Rui Yan & Momoko Shiozaki & Zhiheng Yu & Kira S. Makarova & Eugene V. Koonin &, 2022.
"Structure of the OMEGA nickase IsrB in complex with ωRNA and target DNA,"
Nature, Nature, vol. 610(7932), pages 575-581, October.
Handle:
RePEc:nat:nature:v:610:y:2022:i:7932:d:10.1038_s41586-022-05324-6
DOI: 10.1038/s41586-022-05324-6
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