The absence of effect of
 gid
 or
 mioC
 transcription on the initiation of chromosomal replication in
 Escherichia coli

Bates, David; Boye, Erik; Asai, Tomohisa; Kogoma, Tokio

doi:10.1073/pnas.94.23.12497

Cited by 39 publications

(54 citation statements)

References 38 publications

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“…The proposed mechanisms by which transcription from mioC could inhibit replication were that transcription could impair formation of initiation complex at the origin via physical interactions which would displace DnaA from DNA or through the generation of local changes in the DNA topology destabilizing the initiation complex. However, while the replication time in cells lacking mioC promoter was unaffected (Bates et al 1997;Lobner-Olesen et al 1992), transcription from this promoter became essential for cell viability when the dnaA box R4 was deleted suggesting a positive role for mioC transcription in replication initiation (Bates et al 1997). Despite of all the data obtained over 3 decades, no clear consensus on the role of transcription from the mioC gene on replication has been achieved.…”

Section: Transcription Of Mioc and Its Effect On Replication Initiationmentioning

confidence: 89%

Relations Between Replication and Transcription

Castro-Roa¹,

Zenkin²

2011

Fundamental Aspects of DNA Replication

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Section: Transcription Of Mioc and Its Effect On Replication Initiationmentioning

confidence: 89%

Relations Between Replication and Transcription

Castro-Roa¹,

Zenkin²

2011

Fundamental Aspects of DNA Replication

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“…The mioC gene is located next to oriC on the E. coli chromosome and although several investigations have tried to establish a role for mioC transcription in chromosome replication (22)(23)(24), the results were inconclusive (25,26 (7); lane 5, assay containing all standard components plus fraction 25 from the final Mono Q column (see Fig. 2) .…”

Section: Discussionmentioning

confidence: 99%

MioC Is an FMN-binding Protein That Is Essential forEscherichia coli Biotin Synthase Activity in Vitro

Birch

Hewitson

Fuhrmann

et al. 2000

Journal of Biological Chemistry

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“…Activation of DNA replication by transcription has been found in both prokaryotic (3,11,35,56,70) and eukaryotic (48, 60) cells. On the other hand, transcription has been found to suppress replication in bacterial plasmid DNA (47, 53) and in yeast (77, 82), tetrahymena (61), and human (33) cells.…”

mentioning

confidence: 99%

“…The CMV enhancer was also found to exhibit an inhibitory effect on the CMV enhancer-promoter driving chloramphenicol acetyltransferase expression in a dose-dependent manner. Together these results suggest that inhibition of SV40 origin-based DNA replication by the CMV enhancer is due to intramolecular competition for the formation of active chromatin structure.A majority of DNA replication origins in both prokaryotic (3,11,35,42,53,56,59) and eukaryotic (1, 5, 12, 17-19, 24, 25, 36, 38, 41, 43, 48, 60, 62-66, 68, 71, 75, 78, 81, 83, 84, 93-95) cells are closely associated with a transcription unit. Recent characterization of origins of replication in mammalian cells has shown that the origins are located very close to a transcription unit or even within a transcription unit (see review in reference 20).…”

mentioning

confidence: 99%

“…A majority of DNA replication origins in both prokaryotic (3,11,35,42,53,56,59) and eukaryotic (1, 5, 12, 17-19, 24, 25, 36, 38, 41, 43, 48, 60, 62-66, 68, 71, 75, 78, 81, 83, 84, 93-95) cells are closely associated with a transcription unit. Recent characterization of origins of replication in mammalian cells has shown that the origins are located very close to a transcription unit or even within a transcription unit (see review in reference 20).…”

mentioning

confidence: 99%

See 1 more Smart Citation

Interference of the Simian Virus 40 Origin of Replication by the Cytomegalovirus Immediate Early Gene Enhancer: Evidence for Competition of Active Regulatory Chromatin Conformation in a Single Domain

Chen

Tseng

Chu³

et al. 2000

Molecular and Cellular Biology

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Replication origins are often found closely associated with transcription regulatory elements in both prokaryotic and eukaryotic cells. To examine the relationship between these two elements, we studied the effect of a strong promoter-enhancer on simian virus 40 (SV40) DNA replication. The human cytomegalovirus (CMV) immediate early gene enhancer-promoter was found to exert a strong inhibitory effect on SV40 origin-based plasmid replication in Cos-1 cells in a position-and dose-dependent manner. Deletion analysis indicated that the effect was exerted by sequences located in the enhancer portion of the CMV sequence, thus excluding the mechanism of origin occlusion by transcription. Insertion of extra copies of the SV40 origin only partially alleviated the inhibition. Analysis of nuclease-sensitive cleavage sites of chromatin containing the transfected plasmids indicate that the chromatin was cleaved at one of the regulatory sites in the plasmids containing more than one regulatory site, suggesting that only one nuclease-hypersensitive site existed per chromatin. A positive correlation was found between the degree of inhibition of DNA replication and the decrease of P1 cleavage frequency at the SV40 origin. The CMV enhancer was also found to exhibit an inhibitory effect on the CMV enhancer-promoter driving chloramphenicol acetyltransferase expression in a dose-dependent manner. Together these results suggest that inhibition of SV40 origin-based DNA replication by the CMV enhancer is due to intramolecular competition for the formation of active chromatin structure.A majority of DNA replication origins in both prokaryotic (3,11,35,42,53,56,59) and eukaryotic (1, 5, 12, 17-19, 24, 25, 36, 38, 41, 43, 48, 60, 62-66, 68, 71, 75, 78, 81, 83, 84, 93-95) cells are closely associated with a transcription unit. Recent characterization of origins of replication in mammalian cells has shown that the origins are located very close to a transcription unit or even within a transcription unit (see review in reference 20). The tight association between transcription and replication units has raised the question of whether or not these two processes are coupled (32,36,42,64,91).Mutual influences between replication and transcription processes have been demonstrated. Activation of DNA replication by transcription has been found in both prokaryotic (3,11,35,56,70) and eukaryotic (48, 60) cells. On the other hand, transcription has been found to suppress replication in bacterial plasmid DNA (47, 53) and in yeast (77, 82), tetrahymena (61), and human (33) cells. Conversely, DNA replication can enhance transcription (28,32,64,90,91). Evidence for coupling or a correlation between transcription and replication processes has also been observed in Bacillus subtilis (42), in Physarum (64), in temporal regulation of transcription in active genes in early S phase (26, 37), and in several mammalian genes (5,41,71,94). Transcription factors have also been implicated in regulating replication origins (7,13,18,19,30,31,38,52).To understand the...

show abstract

The absence of effect of gid or mioC transcription on the initiation of chromosomal replication in Escherichia coli

Cited by 39 publications

References 38 publications

Relations Between Replication and Transcription

Relations Between Replication and Transcription

MioC Is an FMN-binding Protein That Is Essential forEscherichia coli Biotin Synthase Activity in Vitro

Interference of the Simian Virus 40 Origin of Replication by the Cytomegalovirus Immediate Early Gene Enhancer: Evidence for Competition of Active Regulatory Chromatin Conformation in a Single Domain

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