Dynamics of Leading-Strand Lesion Skipping by the Replisome
The E. coli replisome stalls transiently when it encounters a lesion in the leading-strand template, skipping over the damage by reinitiating replication at a new primer synthesized downstream by the primase. We report here that template unwinding and lagging-strand synthesis continue downstream of...
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Veröffentlicht in: | Molecular cell 2013-12, Vol.52 (6), p.855-865 |
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Sprache: | eng |
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Zusammenfassung: | The E. coli replisome stalls transiently when it encounters a lesion in the leading-strand template, skipping over the damage by reinitiating replication at a new primer synthesized downstream by the primase. We report here that template unwinding and lagging-strand synthesis continue downstream of the lesion at a reduced rate after replisome stalling, that one replisome is capable of skipping multiple lesions, and that the rate-limiting steps of replication restart involve the synthesis and activation of the new primer downstream. We also find little support for the concept that polymerase uncoupling, where extensive lagging-strand synthesis proceeds downstream in the absence of leading-strand synthesis, involves physical separation of the leading-strand polymerase from the replisome. Instead, our data indicate that extensive uncoupled replication likely results from a failure of the leading-strand polymerase still associated with the DNA helicase and the lagging-strand polymerase that are proceeding downstream to reinitiate synthesis.
•Uncoupled replication occurs downstream of a leading-strand lesion prior to restart•Priming and clamp assembly are rate limiting for leading-strand reinitiation•Rapid replication rates are resumed following leading-strand reinitiation•A single replisome can bypass multiple leading-strand lesions |
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ISSN: | 1097-2765 1097-4164 |
DOI: | 10.1016/j.molcel.2013.10.020 |