Abstract

Genotoxic stress, integral to an organisms life, is clearly implicated in many hazardous biological effects. However, mammalian cells have evolved intricate defense systems that orchestrate a cascade of cellular responses to genomic injury. During the previous grant period, the investigator has developed several sensitive, specific and unique approaches to monitor the induction and repair of genotoxic lesions within discrete DNA fragments. This continuation grant builds further and extends the scope of this work along a similar overall theme. The proposal is based on the premise that the origin, nature, and spatial distribution of genotoxic lesions in conjunction with the characteristic processing heterogeneity, specificity and competence of host repair system determine the cell's fate through a hierarchical order of downstream effectors controlling recovery. The specific hypotheses addressed are: (i) genomic stability and cellular recovery directly depend upon the extent of specific damage and corresponding repair mechanisms, (ii) the failure of repair of deleterious lesions at key gene sequences engenders crucial hotspot mutations and (iii) the p53 gene product actively participates in overall, gene- and site-specific repair.
The specific aims will focus on: (1) demonstrating that inherent repair heterogeneity, resulting in selective elimination of critical genotoxic damage from vital gene sequences, is adduct and target specific and occurs in a manner compatible with normal cell survival, (2) delineating the relationship of the spectrum and strand bias of induced mutations with the predominant persistent genotoxic lesions and strand specificity of repair at cognate genomic sites and (3) understanding the potential modulatory role of the p53 gene product in repair stimulation, mutation avoidance and elimination of mutant cell precursors by apoptosis. One representative subtle miscoding (O4-alkylthymine) and one bulky (anti-BPDE-guanine) adduct will be analyzed in human ras, p53 and factor IX gene targets. The p53 mediated post-damage cellular responses will be studied concomitantly with damage processing ability and mutagenesis in phenotypically and genotypically defined human cells. The integrated data of these systematic studies will provide crucial mechanistic insights pertinent to mutagenesis, oncogenesis and risk assessment of environmental hazards confronting human health.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Environmental Health Sciences (NIEHS)
Type
Research Project (R01)
Project #
5R01ES002388-13
Application #
2444200
Study Section
Special Emphasis Panel (ZRG4-ALTX-2)
Project Start
1981-09-01
Project End
1999-06-30
Budget Start
1997-07-01
Budget End
1998-06-30
Support Year
13
Fiscal Year
1997
Total Cost
Indirect Cost

  Institution

Name
Ohio State University
Department
Radiation-Diagnostic/Oncology
Type
Schools of Medicine
DUNS #
098987217
City
Columbus
State
OH
Country
United States
Zip Code
43210

  Publications

He, Jinshan; Zhu, Qianzheng; Wani, Gulzar et al. (2017) UV-induced proteolysis of RNA polymerase II is mediated by VCP/p97 segregase and timely orchestration by Cockayne syndrome B protein. Oncotarget 8:11004-11019
Zhu, Qianzheng; Wani, Altaf A (2017) Nucleotide Excision Repair: Finely Tuned Molecular Orchestra of Early Pre-incision Events. Photochem Photobiol 93:166-177
Zhu, Qianzheng; Wei, Shengcai; Sharma, Nidhi et al. (2017) Human CRL4DDB2 ubiquitin ligase preferentially regulates post-repair chromatin restoration of H3K56Ac through recruitment of histone chaperon CAF-1. Oncotarget 8:104525-104542
Rehmani, Nida; Zafar, Atif; Arif, Hussain et al. (2017) Copper-mediated DNA damage by the neurotransmitter dopamine and L-DOPA: A pro-oxidant mechanism. Toxicol In Vitro 40:336-346
He, Jinshan; Zhu, Qianzheng; Wani, Gulzar et al. (2016) Valosin-containing Protein (VCP)/p97 Segregase Mediates Proteolytic Processing of Cockayne Syndrome Group B (CSB) in Damaged Chromatin. J Biol Chem 291:7396-408
Han, Chunhua; Srivastava, Amit Kumar; Cui, Tiantian et al. (2016) Differential DNA lesion formation and repair in heterochromatin and euchromatin. Carcinogenesis 37:129-38
Ray, Alo; Blevins, Chessica; Wani, Gulzar et al. (2016) ATR- and ATM-Mediated DNA Damage Response Is Dependent on Excision Repair Assembly during G1 but Not in S Phase of Cell Cycle. PLoS One 11:e0159344
Han, Chunhua; Wani, Gulzar; Zhao, Ran et al. (2015) Cdt2-mediated XPG degradation promotes gap-filling DNA synthesis in nucleotide excision repair. Cell Cycle 14:1103-15
Zhao, Ran; Cui, Tiantian; Han, Chunhua et al. (2015) DDB2 modulates TGF-? signal transduction in human ovarian cancer cells by downregulating NEDD4L. Nucleic Acids Res 43:7838-49
Qian, J; Pentz, K; Zhu, Q et al. (2015) USP7 modulates UV-induced PCNA monoubiquitination by regulating DNA polymerase eta stability. Oncogene 34:4791-6

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