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DNA and Chromosomes
2 Results
- Accelerated CommunicationsOpen Access
Mfd translocase is necessary and sufficient for transcription-coupled repair in Escherichia coli
Journal of Biological ChemistryVol. 292Issue 45p18386–18391Published online: October 6, 2017- Ogun Adebali
- Aziz Sancar
- Christopher P. Selby
Cited in Scopus: 29Nucleotide excision repair in Escherichia coli is stimulated by transcription, specifically in the transcribed strand. Previously, it was shown that this transcription-coupled repair (TCR) is mediated by the Mfd translocase. Recently, it was proposed that in fact the majority of TCR in E. coli is catalyzed by a second pathway (“backtracking-mediated TCR”) that is dependent on the UvrD helicase and the guanosine pentaphosphate (ppGpp) alarmone/stringent response regulator. Recently, we reported that as measured by the excision repair–sequencing (XR-seq), UvrD plays no role in TCR genome-wide. - MinireviewsOpen Access
Molecular mechanisms and genomic maps of DNA excision repair in Escherichia coli and humans
Journal of Biological ChemistryVol. 292Issue 38p15588–15597Published online: August 10, 2017- Jinchuan Hu
- Christopher P. Selby
- Sheera Adar
- Ogun Adebali
- Aziz Sancar
Cited in Scopus: 51Nucleotide excision repair is a major DNA repair mechanism in all cellular organisms. In this repair system, the DNA damage is removed by concerted dual incisions bracketing the damage and at a precise distance from the damage. Here, we review the basic mechanisms of excision repair in Escherichia coli and humans and the recent genome-wide mapping of DNA damage and repair in these organisms at single-nucleotide resolution.