Cryo-electron microscopy structure of the 70S ribosome from Enterococcus faecalis

被引:0
作者
Eileen L. Murphy
Kavindra V. Singh
Bryant Avila
Torsten Kleffmann
Steven T. Gregory
Barbara E. Murray
Kurt L. Krause
Reza Khayat
Gerwald Jogl
机构
[1] Brown University,Department of Molecular Biology, Cell Biology, and Biochemistry
[2] University of Texas Health Science Center,Division of Infectious Diseases, Department of Internal Medicine
[3] University of Texas Health Science Center,Center for Antimicrobial Resistance and Microbial Genomics
[4] The City College of New York,Department of Chemistry and Biochemistry
[5] University of Otago,Department of Biochemistry
[6] The University of Rhode Island,Department of Cell and Molecular Biology
[7] University of Texas Health Science Center,Department of Microbiology and Molecular Genetics
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Scientific Reports | / 10卷
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摘要
Enterococcus faecalis is a gram-positive organism responsible for serious infections in humans, but as with many bacterial pathogens, resistance has rendered a number of commonly used antibiotics ineffective. Here, we report the cryo-EM structure of the E. faecalis 70S ribosome to a global resolution of 2.8 Å. Structural differences are clustered in peripheral and solvent exposed regions when compared with Escherichia coli, whereas functional centres, including antibiotic binding sites, are similar to other bacterial ribosomes. Comparison of intersubunit conformations among five classes obtained after three-dimensional classification identifies several rotated states. Large ribosomal subunit protein bL31, which forms intersubunit bridges to the small ribosomal subunit, assumes different conformations in the five classes, revealing how contacts to the small subunit are maintained throughout intersubunit rotation. A tRNA observed in one of the five classes is positioned in a chimeric pe/E position in a rotated ribosomal state. The 70S ribosome structure of E. faecalis now extends our knowledge of bacterial ribosome structures and may serve as a basis for the development of novel antibiotic compounds effective against this pathogen.
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