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2ZJQ

Interaction of L7 with L11 induced by Microccocin binding to the Deinococcus radiodurans 50S subunit

Summary for 2ZJQ
Entry DOI10.2210/pdb2zjq/pdb
Related2ZJP 2ZJR 3CF5
Descriptorribosomal 23S RNA, 50S ribosomal protein L14, 50S ribosomal protein L15, ... (31 entities in total)
Functional Keywordsribosome, ribosomal subunit, 50s, thiopeptide antibiotics, complex, translational regulation, l11, molecular switch, l7, ribonucleoprotein, ribosomal protein, rna-binding, rrna-binding, trna-binding, methylation, metal-binding, zinc-finger
Biological sourceDeinococcus radiodurans
More
Total number of polymer chains31
Total formula weight1376751.89
Authors
Harms, J.M.,Wilson, D.N.,Schluenzen, F.,Connell, S.R.,Stachelhaus, T.,Zaborowska, Z.,Spahn, C.M.T.,Fucini, P. (deposition date: 2008-03-08, release date: 2008-06-17, Last modification date: 2023-11-01)
Primary citationHarms, J.M.,Wilson, D.N.,Schluenzen, F.,Connell, S.R.,Stachelhaus, T.,Zaborowska, Z.,Spahn, C.M.,Fucini, P.
Translational regulation via L11: molecular switches on the ribosome turned on and off by thiostrepton and micrococcin.
Mol.Cell, 30:26-38, 2008
Cited by
PubMed Abstract: The thiopeptide class of antibiotics targets the GTPase-associated center (GAC) of the ribosome to inhibit translation factor function. Using X-ray crystallography, we have determined the binding sites of thiostrepton (Thio), nosiheptide (Nosi), and micrococcin (Micro), on the Deinococcus radiodurans large ribosomal subunit. The thiopeptides, by binding within a cleft located between the ribosomal protein L11 and helices 43 and 44 of the 23S rRNA, overlap with the position of domain V of EF-G, thus explaining how this class of drugs perturbs translation factor binding to the ribosome. The presence of Micro leads to additional density for the C-terminal domain (CTD) of L7, adjacent to and interacting with L11. The results suggest that L11 acts as a molecular switch to control L7 binding and plays a pivotal role in positioning one L7-CTD monomer on the G' subdomain of EF-G to regulate EF-G turnover during protein synthesis.
PubMed: 18406324
DOI: 10.1016/j.molcel.2008.01.009
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (3.3 Å)
Structure validation

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