African Journal of
Biotechnology

  • Abbreviation: Afr. J. Biotechnol.
  • Language: English
  • ISSN: 1684-5315
  • DOI: 10.5897/AJB
  • Start Year: 2002
  • Published Articles: 12481

Full Length Research Paper

Polymorphisms of the DNA repair gene XPD (751) and XRCC1 (399) correlates with risk of hematological malignancies in Turkish population

Ali Özcan1#, Mustafa Pehlivan2#, AyÅŸe Gaye Tomatir3*, E. Karaca4, Cihangir Özkınay4, Filiz Özdemir1 and Sacide Pehlivan4,5
1Department of Biology, Ege University Faculty of Science, 35100 Izmir, Turkey. 2Department of Hematology, Gaziantep University Medical Faculty, 27100 Gaziantep, Turkey. 3Department of Medical Biology, Pamukkale University Medical Faculty, 20070 Denizli, Turkey. 4Genetic Diseases Research and Application Center, Ege University, 35100 Izmir, Turkey. 5Department of Medical Biology, Gaziantep University Medical Faculty, 27100 Gaziantep, Turkey. # These Authors contributed eaqually.
Email: [email protected]

  •  Accepted: 04 March 2011
  •  Published: 15 August 2011

Abstract

Polymorphisms that occur in DNA repair genes affect DNA repair capacity and constitute a risk factor in hematological malignancies. This study, was aimed to investigate whether xeroderma pigmentosum complementation group D (XPD) and x-ray repair cross-complementing group 1 (XRCC1) gene polymorphisms were involved in the susceptibility to different hematological malignancies. The genotype and allele frequencies were obtained by analyzing XPD gene codon 751 in a total of 80 patients and XRCC1 gene codon 399 polymorphism in a total of 100 patients with hematological malignancies and 100 healthy controls. Mean age was 45 (range: 16 to 75) and 46 (range: 16 to 82) in the patients groups and 39.5 (range: 18 to 67) in the control group, respectively. Additionally, distribution of genotypes and alleles were compared in the patient and control groups. In the comparison of genotype and allele frequencies in hematological malignancies and healthy controls, XPD-751Gln variant was arranged and compared according to age and sex and Gln/Gln genotype was reported to be a protector, which was decreased significantly in acute myeloblastic leukemia (AML) (p = 0.042). No relationship was determined between allele frequencies (p = 0.054). In XRCC1-399, it was shown that Gln/Gln genotype was decreased significantly in AML (p = 0.014) plus all hematological malignancies (p = 0.033) and that Gln allele was present at a lower ratio in AML (p = 0.046). The distribution of polymorphism of both genes was not statistically significant in terms of age and sex. In leukemia with early relapse, XPD 751 Lys/Lys genotype was determined at a statistically higher ratio (p = 0.042). In the evaluation of both genes together, a decrease was noted in Gln/Gln + Lys/Gln haplotype frequency in hematological malignancies (p = 0.048). In this study, it was demonstrated that a decrease in Gln/Gln genotype and Gln allele acted as a protector in XPD codon 751 and XRCC1 codon 399 polymorphisms in acute myeloblastic leukemia (AML) and that an increase in Lys/Lys genotype in acute leukemia was associated with early relapse.

 

Key words: DNA repair, XPD gene, XRCC1 gene, DNA, PCR-RFLP.

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This article is published under the terms of the Creative Commons Attribution License 4.0

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