Literature DB >> 24962573

The C-terminal domain of the DNA polymerase catalytic subunit regulates the primase and polymerase activities of the human DNA polymerase α-primase complex.

Yinbo Zhang1, Andrey G Baranovskiy2, Tahir H Tahirov3, Youri I Pavlov4.   

Abstract

The initiation of DNA synthesis during replication of the human genome is accomplished primarily by the DNA polymerase α-primase complex, which makes the RNA-DNA primers accessible to processive DNA pols. The structural information needed to understand the mechanism of regulation of this complex biochemical reaction is incomplete. The presence of two enzymes in one complex poses the question of how these two enzymes cooperate during priming of DNA synthesis. Yeast two-hybrid and direct pulldown assays revealed that the N-terminal domain of the large subunit of primase (p58N) directly interacts with the C-terminal domain of the catalytic subunit of polα (p180C). We found that a complex of the C-terminal domain of the catalytic subunit of polα with the second subunit (p180C-p70) stimulated primase activity, whereas the whole catalytically active heterodimer of polα (p180ΔN-p70) inhibited RNA synthesis by primase. Conversely, the polα catalytic domain without the C-terminal part (p180ΔN-core) possessed a much higher propensity to extend the RNA primer than the two-subunit polα (p180ΔN-p70), suggesting that p180C and/or p70 are involved in the negative regulation of DNA pol activity. We conclude that the interaction between p180C, p70, and p58 regulates the proper primase and polymerase function. The composition of the template DNA is another important factor determining the activity of the complex. We have found that polα activity strongly depends on the sequence of the template and that homopyrimidine runs create a strong barrier for DNA synthesis by polα.
© 2014 by The American Society for Biochemistry and Molecular Biology, Inc.

Entities:  

Keywords:  C-terminal Domain; DNA Polymerase; DNA Polymerase Activity; DNA Polymerase α-Primase; DNA Primase; DNA Replication; DNA Replication Initiation; Primase Activity; Protein-Protein Interaction; RNA

Mesh:

Substances:

Year:  2014        PMID: 24962573      PMCID: PMC4139218          DOI: 10.1074/jbc.M114.570333

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  62 in total

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  19 in total

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Journal:  J Biol Chem       Date:  2015-12-28       Impact factor: 5.157

2.  Crystal Structure of the Human Pol α B Subunit in Complex with the C-terminal Domain of the Catalytic Subunit.

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3.  Crystal structure of the human primase.

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Journal:  J Biol Chem       Date:  2014-12-30       Impact factor: 5.157

Review 4.  Emerging critical roles of Fe-S clusters in DNA replication and repair.

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5.  Crystal structure of the human Polϵ B-subunit in complex with the C-terminal domain of the catalytic subunit.

Authors:  Andrey G Baranovskiy; Jianyou Gu; Nigar D Babayeva; Igor Kurinov; Youri I Pavlov; Tahir H Tahirov
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6.  Monitoring the Retention of Human Proliferating Cell Nuclear Antigen at Primer/Template Junctions by Proteins That Bind Single-Stranded DNA.

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7.  Comment on "The [4Fe4S] cluster of human DNA primase functions as a redox switch using DNA charge transport".

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8.  Activity and fidelity of human DNA polymerase α depend on primer structure.

Authors:  Andrey G Baranovskiy; Vincent N Duong; Nigar D Babayeva; Yinbo Zhang; Youri I Pavlov; Karen S Anderson; Tahir H Tahirov
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9.  Mechanism of Concerted RNA-DNA Primer Synthesis by the Human Primosome.

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