Structural basis of amino acid surveillance by higher-order tRNA-mRNA interactions

被引:0
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作者
Shuang Li
Zhaoming Su
Jean Lehmann
Vassiliki Stamatopoulou
Nikoleta Giarimoglou
Frances E. Henderson
Lixin Fan
Grigore D. Pintilie
Kaiming Zhang
Muyuan Chen
Steven J. Ludtke
Yun-Xing Wang
Constantinos Stathopoulos
Wah Chiu
Jinwei Zhang
机构
[1] Laboratory of Molecular Biology,Department of Bioengineering and Department of Microbiology and Immunology, James H. Clark Center
[2] National Institute of Diabetes and Digestive and Kidney Diseases,Department of Biochemistry, School of Medicine
[3] Stanford University,Division of CryoEM and Bioimaging, SSRL, SLAC National Accelerator Laboratory, Menlo Park
[4] Institute for Integrative Biology of the Cell (I2BC),undefined
[5] CEA,undefined
[6] CNRS,undefined
[7] Université Paris-Sud,undefined
[8] Campus Paris-Saclay,undefined
[9] University of Patras,undefined
[10] Small-Angle X-ray Scattering Core Facility,undefined
[11] Center for Cancer Research of the National Cancer Institute,undefined
[12] Frederick National Laboratory for Cancer Research,undefined
[13] Leidos Biomedical Research,undefined
[14] Inc,undefined
[15] Verna Marrs and McLean Department of Biochemistry and Molecular Biology,undefined
[16] Baylor College of Medicine,undefined
[17] Structural Biophysics Laboratory,undefined
[18] Center for Cancer Research,undefined
[19] National Cancer Institute,undefined
[20] Stanford University,undefined
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摘要
Amino acid availability in Gram-positive bacteria is monitored by T-box riboswitches. T-boxes directly bind tRNAs, assess their aminoacylation state, and regulate the transcription or translation of downstream genes to maintain nutritional homeostasis. Here, we report cocrystal and cryo-EM structures of Geobacillus kaustophilus and Bacillus subtilis T-box–tRNA complexes, detailing their multivalent, exquisitely selective interactions. The T-box forms a U-shaped molecular vise that clamps the tRNA, captures its 3′ end using an elaborate ‘discriminator’ structure, and interrogates its aminoacylation state using a steric filter fashioned from a wobble base pair. In the absence of aminoacylation, T-boxes clutch tRNAs and form a continuously stacked central spine, permitting transcriptional readthrough or translation initiation. A modeled aminoacyl disrupts tRNA-T-box stacking, severing the central spine and blocking gene expression. Our data establish a universal mechanism of amino acid sensing on tRNAs and gene regulation by T-box riboswitches and exemplify how higher-order RNA-RNA interactions achieve multivalency and specificity.
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页码:1094 / 1105
页数:11
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