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4. Molecular switching of a DNA-sliding clamp to a repressor mediates long-range gene silencing

6. Widespread prevalence of a methylation-dependent switch to activate an essential DNA damage response in bacteria.

10. Connecting the dots: key insights on ParB for chromosome segregation from single-molecule studies.

22. Structural and biochemical analyses of Caulobacter crescentus ParB reveal the role of its N-terminal domain in chromosome segregation

29. Evolving a new protein-DNA interface via sequential introduction of permissive and specificity-switching mutations

31. Mechanistic insight into the repair of C8-linked pyrrolobenzodiazepine monomer-mediated DNA damageElectronic supplementary information (ESI) available. See DOI: https://doi.org/10.1039/d2md00194b

39. Rapid pairing and resegregation of distant homologous loci enables double-strand break repair in bacteria.

40. Condensin promotes the juxtaposition of DNA flanking its loading site in Bacillus subtilis.

41. The CTP-binding domain is disengaged from the DNA-binding domain in a cocrystal structure of Bacillus subtilis Noc-DNA complex.

42. Rapid pairing and resegregation of distant homologous loci enables double-strand break repair in bacteria

43. CTP regulates membrane-binding activity of the nucleoid occlusion protein Noc.

44. Diversification of DNA-Binding Specificity by Permissive and Specificity-Switching Mutations in the ParB/Noc Protein Family.

45. Chromosome Conformation Capture with Deep Sequencing to Study the Roles of the Structural Maintenance of Chromosomes Complex In Vivo.

46. SMC Progressively Aligns Chromosomal Arms in Caulobacter crescentus but Is Antagonized by Convergent Transcription.

47. Condensin promotes the juxtaposition of DNA flanking its loading site in Bacillus subtilis.

48. SimC7 Is a Novel NAD(P)H-Dependent Ketoreductase Essential for the Antibiotic Activity of the DNA Gyrase Inhibitor Simocyclinone.

49. Bacterial chromosome organization and segregation.

50. Structures of the TetR-like simocyclinone efflux pump repressor, SimR, and the mechanism of ligand-mediated derepression.

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