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Literature DB >> 9214648

Deletions at stalled replication forks occur by two different pathways.

Abstract

Replication blockage induces non-homologous deletions in Escherichia coli. The mechanism of the formation of these deletions was investigated. A pBR322-mini-oriC hybrid plasmid carrying two E. coli replication terminators (Ter sites) in opposite orientations was used. Deletions which remove at least the pBR322 blocking site (named Ter1) occurred at a frequency of 2 x 10(-6) per generation. They fall into two equally large classes: deletions that join sequences with no homology, and others that join sequences of 3-10 bp of homology. Some 95% of the deletions in the former class resulted from the fusion of sequences immediately preceding the two Ter sites, indicating a direct role for blocked replication forks in their formation. These deletions were not found in a topA10 mutant, suggesting a topoisomerase I-mediated process. In contrast, deletions joining short homologous sequences were not affected by the topA10 mutation. However, the incidence of this second class of deletions increased 10-fold in a recD mutant, devoid of exonuclease V activity. This indicates that linear molecules are intermediates in their formation. In addition, approximately 50% of these deletions were clustered in the region flanking the Ter1 site. We propose that they are produced by repair of molecules broken at the blocked replication forks.

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Year: 1997 PMID： 9214648 PMCID： PMC1169949 DOI： 10.1093/emboj/16.11.3332

Source DB: PubMed Journal: EMBO J ISSN： 0261-4189 Impact factor: 11.598

43 in total

1. DNA replication fork pause sites dependent on transcription.

Authors: A M Deshpande; C S Newlon
Journal: Science Date: 1996-05-17 Impact factor: 47.728

2. Bacterial DNA topoisomerase I can relax positively supercoiled DNA containing a single-stranded loop.

Authors: K Kirkegaard; J C Wang
Journal: J Mol Biol Date: 1985-10-05 Impact factor: 5.469

3. In vitro insertional mutagenesis with a selectable DNA fragment.

Authors: P Prentki; H M Krisch
Journal: Gene Date: 1984-09 Impact factor: 3.688

4. Model for homologous recombination during transfer of DNA into mouse L cells: role for DNA ends in the recombination process.

Authors: F L Lin; K Sperle; N Sternberg
Journal: Mol Cell Biol Date: 1984-06 Impact factor: 4.272

5. Nucleotide sequence and functional map of pE194, a plasmid that specifies inducible resistance to macrolide, lincosamide, and streptogramin type B antibodies.

Authors: S Horinouchi; B Weisblum
Journal: J Bacteriol Date: 1982-05 Impact factor: 3.490

6. On the formation of spontaneous deletions: the importance of short sequence homologies in the generation of large deletions.

Authors: A M Albertini; M Hofer; M P Calos; J H Miller
Journal: Cell Date: 1982-06 Impact factor: 41.582

7. Mechanism of intramolecular recyclization and deletion formation following transformation of Escherichia coli with linearized plasmid DNA.

Authors: E C Conley; V A Saunders; V Jackson; J R Saunders
Journal: Nucleic Acids Res Date: 1986-11-25 Impact factor: 16.971

8. Mechanistic study of E. coli DNA topoisomerase I: cleavage of oligonucleotides.

Authors: Y C Tse-Dinh; B G McCarron; R Arentzen; V Chowdhry
Journal: Nucleic Acids Res Date: 1983-12-20 Impact factor: 16.971

9. Identification of two Escherichia coli factor Y effector sites near the origins of replication of the plasmids (ColE1 and pBR322.

Authors: S L Zipursky; K J Marians
Journal: Proc Natl Acad Sci U S A Date: 1980-11 Impact factor: 11.205

10. Are single-stranded circles intermediates in plasmid DNA replication?

Authors: H te Riele; B Michel; S D Ehrlich
Journal: EMBO J Date: 1986-03 Impact factor: 11.598

32 in total

1. Cloning and sequencing of defective particles derived from the autonomous parvovirus minute virus of mice for the construction of vectors with minimal cis-acting sequences.

Authors: N Clément; B Avalosse; K El Bakkouri; T Velu; A Brandenburger
Journal: J Virol Date: 2001-02 Impact factor: 5.103

Deletions at stalled replication forks occur by two different pathways.

1. DNA replication fork pause sites dependent on transcription.

2. Bacterial DNA topoisomerase I can relax positively supercoiled DNA containing a single-stranded loop.

3. In vitro insertional mutagenesis with a selectable DNA fragment.

4. Model for homologous recombination during transfer of DNA into mouse L cells: role for DNA ends in the recombination process.

5. Nucleotide sequence and functional map of pE194, a plasmid that specifies inducible resistance to macrolide, lincosamide, and streptogramin type B antibodies.

6. On the formation of spontaneous deletions: the importance of short sequence homologies in the generation of large deletions.

7. Mechanism of intramolecular recyclization and deletion formation following transformation of Escherichia coli with linearized plasmid DNA.

8. Mechanistic study of E. coli DNA topoisomerase I: cleavage of oligonucleotides.

9. Identification of two Escherichia coli factor Y effector sites near the origins of replication of the plasmids (ColE1 and pBR322.

10. Are single-stranded circles intermediates in plasmid DNA replication?

1. Cloning and sequencing of defective particles derived from the autonomous parvovirus minute virus of mice for the construction of vectors with minimal cis-acting sequences.

2. Illegitimate recombination induced by overproduction of DnaB helicase in Escherichia coli.

3. Recombination enhancement by replication (RER) in Rhizobium etli.

4. Partial suppression of the fission yeast rqh1(-) phenotype by expression of a bacterial Holliday junction resolvase.

5. UvrA and UvrB suppress illegitimate recombination: synergistic action with RecQ helicase.

6. Ribosomal DNA replication fork barrier and HOT1 recombination hot spot: shared sequences but independent activities.

Review 7. Rescue of arrested replication forks by homologous recombination.

8. Instability of repetitive DNA sequences: the role of replication in multiple mechanisms.

9. Role of DnaB helicase in UV-induced illegitimate recombination in Escherichia coli.

10. Replication slippage involves DNA polymerase pausing and dissociation.