Computational design of three-dimensional RNA structure and function

被引:0
|
作者
Joseph D. Yesselman
Daniel Eiler
Erik D. Carlson
Michael R. Gotrik
Anne E. d’Aquino
Alexandra N. Ooms
Wipapat Kladwang
Paul D. Carlson
Xuesong Shi
David A. Costantino
Daniel Herschlag
Julius B. Lucks
Michael C. Jewett
Jeffrey S. Kieft
Rhiju Das
机构
[1] Stanford University School of Medicine,Department of Biochemistry
[2] University of Colorado Denver School of Medicine,Department of Biochemistry and Molecular Genetics
[3] Northwestern University,Department of Chemical and Biological Engineering
[4] Northwestern University,Chemistry of Life Processes Institute
[5] Northwestern University,Center for Synthetic Biology
[6] Northwestern University,Interdisciplinary Biological Sciences Graduate Program
[7] Stanford University School of Medicine,Department of Cancer Genetics & Genomics
[8] Cornell University,Robert F. Smith School of Chemical and Biomolecular Engineering
[9] Stanford University School of Medicine,Department of Chemistry
[10] Stanford University,Stanford ChEM
[11] Stanford University,H (Chemistry, Engineering, and Medicine for Human Health)
来源
Nature Nanotechnology | 2019年 / 14卷
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摘要
RNA nanotechnology seeks to create nanoscale machines by repurposing natural RNA modules. The field is slowed by the current need for human intuition during three-dimensional structural design. Here, we demonstrate that three distinct problems in RNA nanotechnology can be reduced to a pathfinding problem and automatically solved through an algorithm called RNAMake. First, RNAMake discovers highly stable single-chain solutions to the classic problem of aligning a tetraloop and its sequence-distal receptor, with experimental validation from chemical mapping, gel electrophoresis, solution X-ray scattering and crystallography with 2.55 Å resolution. Second, RNAMake automatically generates structured tethers that integrate 16S and 23S ribosomal RNAs into single-chain ribosomal RNAs that remain uncleaved by ribonucleases and assemble onto messenger RNA. Third, RNAMake enables the automated stabilization of small-molecule binding RNAs, with designed tertiary contacts that improve the binding affinity of the ATP aptamer and improve the fluorescence and stability of the Spinach RNA in cell extracts and in living Escherichia coli cells.
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页码:866 / 873
页数:7
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