Crystallographic analysis revealed that the 17-member polyketide antibiotic lankacidin produced by Streptomyces rochei binds at the peptidyl transferase center of the eubacterial large ribosomal subunit. Biochemical and functional studies verified this finding and showed interference with peptide bond formation. Chemical probing indicated that the macrolide lankamycin, a second antibiotic produced by the same species, binds at a neighboring site, at the ribosome exit tunnel. These two antibiotics can bind to the ribosome simultaneously and display synergy in inhibiting bacterial growth. The binding site of lankacidin and lankamycin partially overlap with the binding site of another pair of synergistic antibiotics, the streptogramins. Thus, at least two pairs of structurally dissimilar compounds have been selected in the course of evolution to act synergistically by targeting neighboring sites in the ribosome. These results underscore the importance of the corresponding ribosomal sites for development of clinically relevant synergistic antibiotics and demonstrate the utility of structural analysis for providing new directions for drug discovery.
The structure of ribosome-lankacidin complex reveals ribosomal sites for synergistic antibiotics.
核糖体-兰卡西丁复合物的结构揭示了核糖体上协同抗生素的结合位点
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作者:Auerbach Tamar, Mermershtain Inbal, Davidovich Chen, Bashan Anat, Belousoff Matthew, Wekselman Itai, Zimmerman Ella, Xiong Liqun, Klepacki Dorota, Arakawa Kenji, Kinashi Haruyasu, Mankin Alexander S, Yonath Ada
| 期刊: | Proceedings of the National Academy of Sciences of the United States of America | 影响因子: | 9.100 |
| 时间: | 2010 | 起止号: | 2010 Feb 2; 107(5):1983-8 |
| doi: | 10.1073/pnas.0914100107 | ||
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