Stimulation of NEIL2-mediated Oxidized Base Excision Repair via YB-1 Interaction during Oxidative Stress

Das, Soumita; Chattopadhyay, Ranajoy; Bhakat, Kishor K.; Boldogh, István; Kohno, Kimitoshi; Prasad, Rajendra; Wilson, Samuel H.; Hazra, Tapas K.

doi:10.1074/jbc.m704672200

Cited by 125 publications

(108 citation statements)

References 52 publications

(24 reference statements)

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“…For example, we have shown ROS-mediated activation of NEIL1 and APE1 [183,184]. We have shown that ROS enhances NEIL2 complex formation [161]. ROS also enhances modification of OGG1 [180] and possibly other BER proteins.…”

Section: Summary and Future Perspectivesmentioning

confidence: 88%

“…Formation of the multiprotein complexes for oxidative damage repair is enhanced by ROS [51,161]. It was previously shown that NEILs carry out SN-BER mediated by PNK, Pol β, Lig IIIα and XRCC1 by stably interacting with Pol β, Lig IIIα and XRCC1 [51,115].…”

Section: Repair Interactome -A New Paradigm In Bermentioning

confidence: 99%

“…NEIL2 interacts with YB-1, a Y-box binding protein, and it was suggested that YB-1 may be required for the fine-tuning of repair [161]. NTH1 was also shown to interact with and be stimulated by YB-1 [175].…”

Section: Dna Glycosylases Interact With Non-ber Proteinsmentioning

confidence: 99%

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Early steps in the DNA base excision/single-strand interruption repair pathway in mammalian cells

2008

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Base excision repair (BER) is an evolutionarily conserved process for maintaining genomic integrity by eliminating several dozen damaged (oxidized or alkylated) or inappropriate bases that are generated endogenously or induced by genotoxicants, predominantly, reactive oxygen species (ROS). BER involves 4-5 steps starting with base excision by a DNA glycosylase, followed by a common pathway usually involving an AP-endonuclease (APE) to generate 3′ OH terminus at the damage site, followed by repair synthesis with a DNA polymerase and nick sealing by a DNA ligase. This pathway is also responsible for repairing DNA single-strand breaks with blocked termini directly generated by ROS. Nearly all glycosylases, far fewer than their substrate lesions particularly for oxidized bases, have broad and overlapping substrate range, and could serve as back-up enzymes in vivo. In contrast, mammalian cells encode only one APE, APE1, unlike two APEs in lower organisms. In spite of overall similarity, BER with distinct subpathways in the mammals is more complex than in E. coli. The glycosylases form complexes with downstream proteins to carry out efficient repair via distinct subpathways one of which, responsible for repair of strand breaks with 3′ phosphate termini generated by the NEIL family glycosylases or by ROS, requires the phosphatase activity of polynucleotide kinase instead of APE1. Different complexes may utilize distinct DNA polymerases and ligases. Mammalian glycosylases have nonconserved extensions at one of the termini, dispensable for enzymatic activity but needed for interaction with other BER and non-BER proteins for complex formation and organelle targeting. The mammalian enzymes are sometimes covalently modified which may affect activity and complex formation. The focus of this review is on the early steps in mammalian BER for oxidized damage.

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Section: Summary and Future Perspectivesmentioning

confidence: 88%

Section: Repair Interactome -A New Paradigm In Bermentioning

confidence: 99%

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Early steps in the DNA base excision/single-strand interruption repair pathway in mammalian cells

2008

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“…Contrary to the common perception that the repair of oxidatively damaged bases in DNA via the BER pathway involves only a few conserved repair proteins, a more complex picture of BER is now emerging in that BER comprises several alternative subpathways that utilize distinct sets of repair enzymes and other proteins (16,19,21,35,46). We have been exploring the role of noncanonical proteins in oxidized base repair and have characterized the proteins present in immunoprecipitates of early BER enzymes including DGs.…”

Section: Discussionmentioning

confidence: 99%

Enhancement of NEIL1 Protein-initiated Oxidized DNA Base Excision Repair by Heterogeneous Nuclear Ribonucleoprotein U (hnRNP-U) via Direct Interaction

Hegde

Banerjee

Hegde

et al. 2012

Journal of Biological Chemistry

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Background: Oxidized bases in mammalian genome are repaired via base excision repair (BER) process that utilizes both common repair and noncanonical proteins. Results: hnRNP-U stimulates NEIL1-initiated BER via direct interaction and is required for enhancing oxidative stress-induced repair. Conclusion: NEIL1's interaction with hnRNP-U is critical for regulating oxidized genome damage repair after oxidative stress. Significance: The RNA-binding protein hnRNP-U plays a role in maintaining genomic integrity.

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“…Actually, several noncanonical factors have been demonstrated to participate BER, even though their in vivo functions are yet to be fully unraveled. The list of non-BER proteins includes for instance: YB-1 [which has been shown to interact with the endonuclease VIII-like 2 (NEIL2) glycosylase (35), the endonuclease III-like glycosylase (NTH1) and APE1 (29)], NEIL2 [which was also found to interact with the RNA-binding protein hnRNP-U (6)], HMGB1 [which has been implicated in single-strand break (SSB) repair involving Polb (90)] and the tumor suppressor p53, which was also shown to play a role in DNA damage repair through direct binding to APE1 and Polb (168). The list of these non-BER proteins is still growing, supporting the notion that BER in vivo is far more complex than the simple model that we can reconstitute in vitro.…”

Section: Relevance Of the Unfolded Domains In Ber Proteinsmentioning

confidence: 99%

Emerging Roles of the Nucleolus in Regulating the DNA Damage Response: The Noncanonical DNA Repair Enzyme APE1/Ref-1 as a Paradigmatical Example

Antoniali

Lirussi

Poletto

et al. 2014

Antioxidants & Redox Signaling

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Significance: An emerging concept in DNA repair mechanisms is the evidence that some key enzymes, besides their role in the maintenance of genome stability, display also unexpected noncanonical functions associated with RNA metabolism in specific subcellular districts (e.g., nucleoli). During the evolution of these key enzymes, the acquisition of unfolded domains significantly amplified the possibility to interact with different partners and substrates, possibly explaining their phylogenetic gain of functions. Recent Advances: After nucleolar stress or DNA damage, many DNA repair proteins can freely relocalize from nucleoli to the nucleoplasm. This process may represent a surveillance mechanism to monitor the synthesis and correct assembly of ribosomal units affecting cell cycle progression or inducing p53-mediated apoptosis or senescence. Critical Issues: A paradigm for this kind of regulation is represented by some enzymes of the DNA base excision repair (BER) pathway, such as apurinic/apyrimidinic endonuclease 1 (APE1). In this review, the role of the nucleolus and the noncanonical functions of the APE1 protein are discussed in light of their possible implications in human pathologies. Future Directions: A productive cross-talk between DNA repair enzymes and proteins involved in RNA metabolism seems reasonable as the nucleolus is emerging as a dynamic functional hub that coordinates cell growth arrest and DNA repair mechanisms. These findings will drive further analyses on other BER proteins and might imply that nucleic acid processing enzymes are more versatile than originally thought having evolved DNA-targeted functions after a previous life in the early RNA world. Antioxid. Redox Signal. 20, 621-639.

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Stimulation of NEIL2-mediated Oxidized Base Excision Repair via YB-1 Interaction during Oxidative Stress

Cited by 125 publications

References 52 publications

Early steps in the DNA base excision/single-strand interruption repair pathway in mammalian cells

Early steps in the DNA base excision/single-strand interruption repair pathway in mammalian cells

Enhancement of NEIL1 Protein-initiated Oxidized DNA Base Excision Repair by Heterogeneous Nuclear Ribonucleoprotein U (hnRNP-U) via Direct Interaction

Emerging Roles of the Nucleolus in Regulating the DNA Damage Response: The Noncanonical DNA Repair Enzyme APE1/Ref-1 as a Paradigmatical Example

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