A variant within the DNA repair gene XRCC3 is associated with the development of melanoma skin cancer. Winsey, S. L., Haldar, N. A., Marsh, H. P., Bunce, M., Marshall, S. E., Harris, A. L., Wojnarowska, F., & Welsh, K. I. Cancer Research, 60(20):5612–5616, October, 2000.
abstract   bibtex   
Exposure to UV radiation is a major risk factor for the development of malignant melanoma. DNA damage caused by UV radiation is thought to play a major role in carcinogenesis induction. Multiprotein pathways involved in repairing UV-DNA damage are the base excision, the nucleotide excision, and the homologous double-stranded DNA repair pathways. This study used a sequence-specific primer PCR (PCR-SSP) genotyping method to investigate the association between polymorphisms in DNA repair genes from these pathways with the development of malignant melanoma. The patient cohort was comprised of 125 individuals with malignant melanoma with lesions or staging suggesting a high risk of relapse or metastatic disease. The control population consisted of 211 individuals. We found the presence of a T allele in exon 7 (position 18067) of the XRCC3 gene was significantly associated with melanoma development (P = 0.004; odds ratio, 2.36; relative risk, 1.74). This gene codes for a protein involved in the homologous pathway of double-stranded DNA repair, thought to repair chromosomal fragmentation, translocations, and deletions. These results may provide further insights into the pathogenesis and the mechanism of UV-radiation induced carcinogenesis as well as having a role in prevention.
@article{winsey_variant_2000,
	title = {A variant within the {DNA} repair gene {XRCC3} is associated with the development of melanoma skin cancer},
	volume = {60},
	issn = {0008-5472},
	abstract = {Exposure to UV radiation is a major risk factor for the development of malignant melanoma. DNA damage caused by UV radiation is thought to play a major role in carcinogenesis induction. Multiprotein pathways involved in repairing UV-DNA damage are the base excision, the nucleotide excision, and the homologous double-stranded DNA repair pathways. This study used a sequence-specific primer PCR (PCR-SSP) genotyping method to investigate the association between polymorphisms in DNA repair genes from these pathways with the development of malignant melanoma. The patient cohort was comprised of 125 individuals with malignant melanoma with lesions or staging suggesting a high risk of relapse or metastatic disease. The control population consisted of 211 individuals. We found the presence of a T allele in exon 7 (position 18067) of the XRCC3 gene was significantly associated with melanoma development (P = 0.004; odds ratio, 2.36; relative risk, 1.74). This gene codes for a protein involved in the homologous pathway of double-stranded DNA repair, thought to repair chromosomal fragmentation, translocations, and deletions. These results may provide further insights into the pathogenesis and the mechanism of UV-radiation induced carcinogenesis as well as having a role in prevention.},
	language = {eng},
	number = {20},
	journal = {Cancer Research},
	author = {Winsey, S. L. and Haldar, N. A. and Marsh, H. P. and Bunce, M. and Marshall, S. E. and Harris, A. L. and Wojnarowska, F. and Welsh, K. I.},
	month = oct,
	year = {2000},
	keywords = {Adult, Aged, Aged, 80 and over, Cohort Studies, DNA Repair, DNA-Binding Proteins, Exons, Female, Genetic Predisposition to Disease, Genotype, Humans, Male, Melanoma, Middle Aged, Phenotype, Polymerase Chain Reaction, Polymorphism, Genetic, Skin Neoplasms},
	pages = {5612--5616},
}
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