Specific Function of DNA Ligase I in Simian Virus 40 DNA Replication by Human Cell-free Extracts Is Mediated by the Amino-terminal Non-catalytic Domain

Mackenney, Victoria J.; Barnes, Deborah E.; Lindahl, Tomas

doi:10.1074/jbc.272.17.11550

Cited by 68 publications

(64 citation statements)

References 30 publications

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“…In agreement with published studies, DNA replication efficiency was dependent upon having enough ligation activity and the ability of hLigI to interact with PCNA (16 -18, 33, 57-59). Expression of wild type hLigI mostly corrected the replication defect of hLigI-deficient 46BRLigI m/m extract (17,18,40). These results are also consistent with PCNA coordinating the action of hLigI during Okazaki fragment processing and ligation and the essential role of PCNA in efficient fork progression (17,40).…”

Section: Discussionsupporting

confidence: 76%

“…Expression of wild type hLigI mostly corrected the replication defect of hLigI-deficient 46BRLigI m/m extract (17,18,40). These results are also consistent with PCNA coordinating the action of hLigI during Okazaki fragment processing and ligation and the essential role of PCNA in efficient fork progression (17,40). At the same time, replication was slightly hindered by the presence of CTG/CAG repeats in the template, an effect further exacerbated by hLigI-altered backgrounds.…”

Section: Discussionsupporting

confidence: 74%

“…This increase was dependent upon the presence of a functional PCNA interaction motif but not linked to ligation activity (31). (ii) An excess of hLigI, either full-length or its aminoterminal region (required for PCNA interaction) but not the catalytic domain, inhibited in vitro SV40 DNA replication by HeLa cell extracts (40). This disruption by the non-catalytic domain of hLigI was interpreted to be because of an imbalanced availability of hLigI-interacting partners, like PCNA.…”

Section: Discussionmentioning

confidence: 99%

“…1) (18). Because it has been suggested that the steady state levels of hLigI protein may affect replication or repair pathways (40) and hLigI is frequently overexpressed in human malignant processes (48), we also examined its levels in the three 46BRLigI cell lines (18). Interestingly, different levels of hLigI were observed ( Fig.…”

Section: Different Hligi Protein Backgrounds In 46brligi Extracts-mentioning

confidence: 99%

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CTG/CAG Repeat Instability Is Modulated by the Levels of Human DNA Ligase I and Its Interaction with Proliferating Cell Nuclear Antigen

Castel

Tomkinson

Pearson

2009

Journal of Biological Chemistry

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Mechanisms contributing to disease-associated trinucleotide repeat instability are poorly understood. DNA ligation is an essential step common to replication and repair, both potential sources of repeat instability. Using derivatives of DNA ligase I (hLigI)-deficient human cells (46BR.1G1), we assessed the effect of hLigI activity, overexpression, and its interaction with proliferating cell nuclear antigen (PCNA) upon the ability to replicate and repair trinucleotide repeats. Compared with LigI ؉/؉ , replication progression through repeats was poor, and repair tracts were broadened beyond the slipped-repeat for all mutant extracts. Increased repeat instability was linked only to hLigI overexpression and expression of a mutant hLigI incapable of interacting with PCNA. The endogenous mutant version of hLigI with reduced ligation activity did not alter instability. We distinguished the DNA processes through which hLigI contributes to trinucleotide instability. The highest levels of repeat instability were observed under the hLigI overexpression and were linked to reduced slipped-DNAs repair efficiencies. Therefore, the replication-mediated instability can partly be attributed to errors during replication but also to the poor repair of slipped-DNAs formed during this process. However, repair efficiencies were unaffected by expression of a PCNA interaction mutant of hLigI, limiting this instability to the replication process. The addition of purified proteins suggests that disruption of LigI and PCNA interactions influences trinucleotide repeat instability. The variable levels of age-and tissue-specific trinucleotide repeat instability observed in myotonic dystrophy patients and transgenic mice may be influenced by varying steady state levels of DNA ligase I in these tissues and during different developmental windows.More than 40 hereditary diseases are caused by gene-specific repeat instability (1). Changes at trinucleotide repeats (TNRs) 3 constitute the largest component of this group, causing at least 15 different human diseases, including myotonic dystrophy (DM1), Huntington disease, and fragile X syndrome (FRAXA). Repeat changes in humans are expansion-biased and occur both in parent-to-offspring transmissions and in somatic tissues. The formation of unusual DNA structures during DNA replication and/or aberrant repair of these intermediates has been postulated as the likely source for the development of repeat tract changes (1-3), although the exact molecular mechanisms are unclear. Various proteins have been identified as players in the mutagenic process of TNR instability, including FEN1 (4 -6), OGG1 (7), and some mismatch repair factors, such as MSH2, MSH3, and PMS2 (8 -13). All processes suggested to be involved in repeat instability require a nick located within or proximal to the repeat tract, which ultimately must be ligated. Importantly, many proposed mechanisms of repeat instability involve slippage at the nick (1, 2, 7).Ligation is an essential step in DNA replication, repair, and recombination (14, 1...

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Section: Discussionsupporting

confidence: 76%

Section: Discussionsupporting

confidence: 74%

Section: Discussionmentioning

confidence: 99%

Section: Different Hligi Protein Backgrounds In 46brligi Extracts-mentioning

confidence: 99%

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CTG/CAG Repeat Instability Is Modulated by the Levels of Human DNA Ligase I and Its Interaction with Proliferating Cell Nuclear Antigen

Castel

Tomkinson

Pearson

2009

Journal of Biological Chemistry

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“…LigI is the major replicative ligase with limited functions in some DNA repair pathways (1)(2)(3)(4). LigIV joins DNA double-stranded breaks in the nonhomologous end joining and during V(D)J recombination in the developing immune system (5).…”

mentioning

confidence: 99%