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Merck
  • Structural insight into negative DNA supercoiling by DNA gyrase, a bacterial type 2A DNA topoisomerase.

Structural insight into negative DNA supercoiling by DNA gyrase, a bacterial type 2A DNA topoisomerase.

Nucleic acids research (2013-06-28)
Julie Papillon, Jean-François Ménétret, Claire Batisse, Reynald Hélye, Patrick Schultz, Noëlle Potier, Valérie Lamour
摘要

Type 2A DNA topoisomerases (Topo2A) remodel DNA topology during replication, transcription and chromosome segregation. These multisubunit enzymes catalyze the transport of a double-stranded DNA through a transient break formed in another duplex. The bacterial DNA gyrase, a target for broad-spectrum antibiotics, is the sole Topo2A enzyme able to introduce negative supercoils. We reveal here for the first time the architecture of the full-length Thermus thermophilus DNA gyrase alone and in a cleavage complex with a 155 bp DNA duplex in the presence of the antibiotic ciprofloxacin, using cryo-electron microscopy. The structural organization of the subunits of the full-length DNA gyrase points to a central role of the ATPase domain acting like a 'crossover trap' that may help to sequester the DNA positive crossover before strand passage. Our structural data unveil how DNA is asymmetrically wrapped around the gyrase-specific C-terminal β-pinwheel domains and guided to introduce negative supercoils through cooperativity between the ATPase and β-pinwheel domains. The overall conformation of the drug-induced DNA binding-cleavage complex also suggests that ciprofloxacin traps a DNA pre-transport conformation.

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Sigma-Aldrich
环丙沙星, ≥98% (HPLC)
Supelco
盐酸环丙沙星, Pharmaceutical Secondary Standard; Certified Reference Material
Supelco
环丙沙星, Pharmaceutical Secondary Standard; Certified Reference Material
盐酸环丙沙星, European Pharmacopoeia (EP) Reference Standard
环丙沙星, European Pharmacopoeia (EP) Reference Standard
盐酸环丙沙星, European Pharmacopoeia (EP) Reference Standard