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Human SIDT1 mediates dsRNA uptake via its phospholipase activity

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Fig. 1: Structures of human SIDT1 and its phospholipase activity-dependent dsRNA uptake.

Data availability

All relevant data are available from the authors and/or included in the manuscript or Supplementary information. The cryo-EM structures of wild-type SIDT1 complexed with PA and SIDT1E555Q have been deposited at PDB under the codes of 8JUL and 8JUN, respectively. The cryo-EM density maps of two structures have been deposited at the Electron Microscopy Data Bank under accession codes: EMD-36661 for PA-bound SIDT1, and EMD-36662 for SIDT1E555Q.

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Acknowledgements

We thank Dr. Yong-Xiang Gao for technical support on cryo-EM data collection at the Cryo-EM Center at the University of Science and Technology of China (USTC). This work was supported by the Strategic Priority Research Program of the Chinese Academy of Sciences (XDB37020202) and Research Funds of Center for Advanced Interdisciplinary Science and Biomedicine of IHM (QYZD20220001).

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Authors

Contributions

C.Z.Z., Y.C. and Q.L. conceptualized and supervised the project. C.R.S., D.X. and Q.L. designed all the experiments. C.Y.Z. provides the plasmid encoding SIDT1. C.R.S. performed cloning, expression, purification and cryo-EM sample preparation. C.R.S. and D.X. preformed cryo-EM data collection, structure determination and model refinement. C.R.S. preformed phospholipase activity assays. Z.H. and G.H. performed mass spectrometry analyses. F.Y., X.Y., Y.L. and G.S. performed fluorescence experiments and data analyses. Q.L., C.R.S., C.Z.Z. and Y.C. wrote the manuscript.

Corresponding authors

Correspondence to Xuebiao Yao, Yuxing Chen, Qiong Li or Cong-Zhao Zhou.

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The authors declare no competing interests.

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Sun, CR., Xu, D., Yang, F. et al. Human SIDT1 mediates dsRNA uptake via its phospholipase activity. Cell Res 34, 84–87 (2024). https://doi.org/10.1038/s41422-023-00889-x

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