Association between newly identified variant form of DNA polymerase beta^Δ208–304 and ovarian cancer

Article type: Research Article

Authors: Khanra, Kalyani^a | Panda, Kakali^a | Bhattacharya, Chandan^b | Mitra, AK^c | Sarkar, Ranu^d | Banerjee, Sipra^e | Bhattacharyya, Nandan^{a; *}

Affiliations: [a] Department of Biotechnology, Haldia Institute of Technology, WB, India | [b] Bidhan Chandra Krishi Vishyavidyalaya, Regional Research Station, Jhargram, West Bengal, India | [c] Haldia Seva Sadan, Debhog, Haldia, Purba Medinipur, PIN, India | [d] Department of Pathology, NRS Medical College, Kolkata, India | [e] Department of Cancer Biology, Cleveland Clinic Foundation, Cleveland, OH, USA

Correspondence: [*] Corresponding author: Prof. Nandan Bhattacharyya, School of Food and Biotechnology; Haldia Institute of Technology, P.O.-HIT, PIN-721657, West Bengal, India. Tel.: +91 94344 53188; Fax: +91 3224252800; E-mail: [email protected].

Abstract: Background:Base excision repair (BER) is a key pathway for maintaining genomic stability. A key enzyme in the BER pathway is DNA polymerase beta (polβ), which removes the deoxyribose phosphate group (dRP) and fills in the gap with a nucleotide after the DNA lesion is excised. It has been shown that more than thirty percent of breast, bladder, esophageal, colon, and gastric cancer samples studied so far have exhibited DNA polymerase beta mutation. Aim:To examine the association between polβ polymorphism and ovarian cancer, case control study was performed using one hundred fifty two cancer samples and non-metastatic normal samples from the same patients in Indian population. Design:The polβ polymorphism was studied in ovarian carcinoma tissues samples initially by RT-PCR followed by sequencing and then by western blot analysis. Result:A new type of variant was detected along with the WT allele (polβΔ208−304). Stage IV samples have shown a significant factor for cancer progression in ovarian cancer patients of India [OR=3.58; 95% CI (1.6–7.9); and p=0.001]. The association study involving serous type and the variant showed a tendency towards ovarian carcinogenesis [OR=1.57; 95% CI (0.8–3.1); p=0.19]. The western blot analysis result indicates that the specific deletion appears to be associated with disease progression. Conclusion:The result reveals that this variant form of polβ is a predisposing factor for stage IV ovarian cancer samples in Indian population.

Keywords: DNA polymerase β, polymorphism, ovarian cancer, India

DOI: 10.3233/CBM-2012-00275

Journal: Cancer Biomarkers, vol. 11, no. 4, pp. 155-160, 2012