Regulatory regions responsive to oxidative stress in the promoter of the human DNA glycosylase gene NEIL2

doi:10.1093/mutage/gep058

Mutagenesis Advance Access published online on November 27, 2009
Mutagenesis, doi:10.1093/mutage/gep058

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Regulatory regions responsive to oxidative stress in the promoter of the human DNA glycosylase gene NEIL2

Carla J. Kinslow, Randa A. El-Zein¹, Catherine M. Rondelli, Courtney E. Hill, Jeffrey K. Wickliffe² and Sherif Z. Abdel-Rahman^*

Department of Obstetrics and Gynecology, The University of Texas Medical Branch, Galveston, TX 77555-1062, USA ¹Department of Epidemiology, University of Texas M.D. Anderson Cancer Center, Houston, TX, USA ²Tulane University Health Sciences Center, School of Public Health and Tropical Medicine, New Orleans, LA, USA

Reactive oxygen species (ROS) generated endogenously or fromexogenous sources produce mutagenic DNA lesions. If not repaired,these lesions could lead to genomic instability and, potentially,to cancer development. NEIL2 (EC 4.2.99.18 [EC] ), a mammalian baseexcision repair (BER) protein and ortholog of the bacterialFpg/Nei, excises oxidized DNA lesions from bubble or single-strandedstructures, suggesting its involvement in transcription-coupledDNA repair. Perturbation in NEIL2 expression may, therefore,significantly impact BER capacity and promote genomic instability.To characterize the genetic and environmental factors regulatingNEIL2 gene expression, we mapped the human NEIL2 transcriptionalstart site and partially characterized the promoter region ofthe gene using a luciferase reporter assay. We identified astrong positive regulatory region from nucleotide –206to +90 and found that expression from this region was contingenton its being isolated from an adjacent strong negative regulatoryregion located downstream (+49 to +710 bp), suggesting thatNEIL2 transcription is influenced by both these regions. Wealso found that oxidative stress, induced by glucose oxidasetreatment, reduced the positive regulatory region expressionlevels, suggesting that ROS may play a significant role in regulatingNEIL2 transcription. In an initial attempt to characterize theunderlying mechanisms, we used in silico analysis to identifyputative cis-acting binding sites for ROS-responsive transcriptionfactors within this region and then used site-directed mutagenesisto investigate their role. A single-base change in the regionencompassing nucleotides –206 to +90 abolished the effectof oxidative stress that was observed in the absence of themutation. Our study is the first to provide an initial partialcharacterization of the NEIL2 promoter and opens the door forfuture research aimed at understanding the role of genetic andenvironmental factors in regulating NEIL2 expression.

^* To whom correspondence should be addressed. Tel: +1 409 772 9111; Fax: +1 409 772 2261; Email: sabdelra{at}utmb.edu

Received on June 29, 2009; revised on October 2, 2009; accepted on November 4, 2009.

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