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Literature DB >> 10735873

Intrinsic polymerase activities of UmuD'(2)C and MucA'(2)B are responsible for their different mutagenic properties during bypass of a T-T cis-syn cyclobutane dimer.

P I O'Grady¹, A Borden, D Vandewiele, A Ozgenc, R Woodgate, C W Lawrence.

Abstract

In wild-type Escherichia coli, translesion replication is largely dependent upon the UmuD'(2)C complex (DNA polymerase V [polV]) or its plasmid-encoded homologs, such as MucA'(2)B. Interestingly, both the efficiency of translesion replication of a T-T cis-syn dimer and the spectra of mutations observed are different in Umu- and Muc-expressing strains. We have investigated whether the polIII core is responsible for these differences by measuring the frequency of dimer bypass, the error rate of bypass, and the resulting mutation spectrum in mutants carrying a deletion of dnaQ (epsilon subunit) or holE (theta subunit) or carrying the dnaQ allele mutD5, which is deficient in proofreading but is competent in the structural function of epsilon, or the dnaE antimutator allele spq-2. The chromosomal copy of the umuDC operon was deleted in each strain, and the UmuDC, UmuD'C, MucAB, or MucA'B proteins were expressed from a low-copy-number plasmid. With only few exceptions, we found that the characteristically different mutation spectra resulting from Umu- and Muc-mediated bypass are maintained in all of the strains investigated, indicating that differences in the activity or structure of the polIII core are not responsible for the observed phenotype. We also demonstrate that the MucA'(2)B complex is more efficient in promoting translesion replication than the UmuD'(2)C proteins and show that, contrary to expectation, the T-T dimer is bypassed more accurately by MucA'(2)B than by UmuD'(2)C. These results are consistent with the view that in a wild-type cell, the polV-like enzymes are responsible for the spectra of mutations generated during translesion replication and that polIII may simply be required to fix the misincorporations as mutations by completing chromosomal replication. Our observations also show that the mutagenic properties of a lesion can depend strongly on the particular enzyme employed in bypass.

Entities: Gene Species

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Year: 2000 PMID： 10735873 PMCID： PMC111279 DOI： 10.1128/JB.182.8.2285-2291.2000

Source DB: PubMed Journal: J Bacteriol ISSN： 0021-9193 Impact factor: 3.490

39 in total

1. Novel human and mouse homologs of Saccharomyces cerevisiae DNA polymerase eta.

Authors: J P McDonald; V Rapić-Otrin; J A Epstein; B C Broughton; X Wang; A R Lehmann; D J Wolgemuth; R Woodgate
Journal: Genomics Date: 1999-08-15 Impact factor: 5.736

2. Lon-mediated proteolysis of the Escherichia coli UmuD mutagenesis protein: in vitro degradation and identification of residues required for proteolysis.

Authors: M Gonzalez; E G Frank; A S Levine; R Woodgate
Journal: Genes Dev Date: 1998-12-15 Impact factor: 11.361

3. Efficient translesion replication in the absence of Escherichia coli Umu proteins and 3'-5' exonuclease proofreading function.

Authors: D Vandewiele; A Borden; P I O'Grady; R Woodgate; C W Lawrence
Journal: Proc Natl Acad Sci U S A Date: 1998-12-22 Impact factor: 11.205

4. Frequency and spectrum of mutations produced by a single cis-syn thymine-thymine cyclobutane dimer in a single-stranded vector.

Authors: S K Banerjee; R B Christensen; C W Lawrence; J E LeClerc
Journal: Proc Natl Acad Sci U S A Date: 1988-11 Impact factor: 11.205

5. Roles of E. coli DNA polymerases IV and V in lesion-targeted and untargeted SOS mutagenesis.

Authors: M Tang; P Pham; X Shen; J S Taylor; M O'Donnell; R Woodgate; M F Goodman
Journal: Nature Date: 2000-04-27 Impact factor: 49.962

6. The mutagenesis protein UmuC is a DNA polymerase activated by UmuD', RecA, and SSB and is specialized for translesion replication.

Authors: N B Reuven; G Arad; A Maor-Shoshani; Z Livneh
Journal: J Biol Chem Date: 1999-11-05 Impact factor: 5.157

7. Isolation and characterization of mutants of Escherichia coli deficient in induction of mutations by ultraviolet light.

Authors: T Kato; Y Shinoura
Journal: Mol Gen Genet Date: 1977-11-14

8. UmuD'(2)C is an error-prone DNA polymerase, Escherichia coli pol V.

Authors: M Tang; X Shen; E G Frank; M O'Donnell; R Woodgate; M F Goodman
Journal: Proc Natl Acad Sci U S A Date: 1999-08-03 Impact factor: 11.205

9. Mutagenic DNA repair in Escherichia coli. III. Requirement for a function of DNA polymerase III in ultraviolet-light mutagenesis.

Authors: B A Bridges; R P Mottershead
Journal: Mol Gen Genet Date: 1976-02-27

10. Mechanism of ultraviolet-induced mutagenesis: extent and fidelity of in vitro DNA synthesis on irradiated templates.

Authors: G Villani; S Boiteux; M Radman
Journal: Proc Natl Acad Sci U S A Date: 1978-07 Impact factor: 11.205

5 in total

1. Escherichia coli DNA polymerase III can replicate efficiently past a T-T cis-syn cyclobutane dimer if DNA polymerase V and the 3' to 5' exonuclease proofreading function encoded by dnaQ are inactivated.

Authors: Angela Borden; Paul I O'Grady; Dominique Vandewiele; Antonio R Fernández de Henestrosa; Christopher W Lawrence; Roger Woodgate
Journal: J Bacteriol Date: 2002-05 Impact factor: 3.490

2. The aflatoxin B(1) formamidopyrimidine adduct plays a major role in causing the types of mutations observed in human hepatocellular carcinoma.

Authors: Maryann E Smela; Michelle L Hamm; Paul T Henderson; Constance M Harris; Thomas M Harris; John M Essigmann
Journal: Proc Natl Acad Sci U S A Date: 2002-05-14 Impact factor: 11.205