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4OIP

Crystal structure of Thermus thermophilus transcription initiation complex soaked with GE23077, ATP, and CMPcPP

Summary for 4OIP
Entry DOI10.2210/pdb4oip/pdb
Related4OIN 4OIO 4OIQ 4OIR
Related PRD IDPRD_001181
DescriptorDNA-directed RNA polymerase subunit alpha, ZINC ION, ADENOSINE-5'-TRIPHOSPHATE, ... (13 entities in total)
Functional Keywordsge23077, transcription inhibitor, transcription open complex, transcription initiation complex, i site, i+1 site, cmpcpp, rna polymerase, dna/rna/ntp binding, polymerization of ribonucleotides, nucleoid, transcription, transferase-antibiotic complex, transferase/antibiotic
Biological sourceThermus thermophilus
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Cellular locationCytoplasm (By similarity): Q5SKW1
Total number of polymer chains9
Total formula weight445374.21
Authors
Zhang, Y.,Ebright, R.H.,Arnold, E. (deposition date: 2014-01-20, release date: 2014-05-07, Last modification date: 2023-09-20)
Primary citationZhang, Y.,Degen, D.,Ho, M.X.,Sineva, E.,Ebright, K.Y.,Ebright, Y.W.,Mekler, V.,Vahedian-Movahed, H.,Feng, Y.,Yin, R.,Tuske, S.,Irschik, H.,Jansen, R.,Maffioli, S.,Donadio, S.,Arnold, E.,Ebright, R.H.
GE23077 binds to the RNA polymerase 'i' and 'i+1' sites and prevents the binding of initiating nucleotides.
Elife, 3:e02450-e02450, 2014
Cited by
PubMed Abstract: Using a combination of genetic, biochemical, and structural approaches, we show that the cyclic-peptide antibiotic GE23077 (GE) binds directly to the bacterial RNA polymerase (RNAP) active-center 'i' and 'i+1' nucleotide binding sites, preventing the binding of initiating nucleotides, and thereby preventing transcription initiation. The target-based resistance spectrum for GE is unusually small, reflecting the fact that the GE binding site on RNAP includes residues of the RNAP active center that cannot be substituted without loss of RNAP activity. The GE binding site on RNAP is different from the rifamycin binding site. Accordingly, GE and rifamycins do not exhibit cross-resistance, and GE and a rifamycin can bind simultaneously to RNAP. The GE binding site on RNAP is immediately adjacent to the rifamycin binding site. Accordingly, covalent linkage of GE to a rifamycin provides a bipartite inhibitor having very high potency and very low susceptibility to target-based resistance. DOI: http://dx.doi.org/10.7554/eLife.02450.001.
PubMed: 24755292
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (3.4 Å)
Structure validation

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