• Title of article

    Downregulated Expression of WWOX in Cervical Carcinoma: A Case-Control Study

  • Author/Authors

    Srivastava ، Shikha Cytogenetics Laboratory, Department of Zoology - Banaras Hindu University , Pratap Shahi ، Uday Department of Radiotherapy and Radiation Medicine - Institute of Medical Sciences - Banaras Hindu University , Divya ، Arti Indian Railways Cancer Institute and Research Centre , Gupta ، Sadhana Department of Obstetrics and Gynaecology - Institute of Medical Sciences - Banaras Hindu University , Singh ، Indu Apollo Clinic , Roy ، Jagat Kumar Cytogenetics Laboratory, Department of Zoology - Banaras Hindu University

  • From page
    273
  • To page
    287
  • Abstract
    Integration of human papilloma virus (HPV) in human genome is a random event, and fragile sites are one of the most susceptible sites for viral integrations. WWOX (WW-domain containing oxidoreductase) gene harbours the second most common fragile site, FRA16D, and can be an important candidate for HPV integration and cervical carcinogenesis. Our aim was to evaluate the potential role of WWOX in cervical carcinogenesis. Presence of HPV and its genotype was detected by PCR in normal cervix tissues and human cervical carcinoma. The expression of WWOX transcript and its protein was examined by RT-PCR, RNA in situ hybridization, and immunoblotting. Southern blotting and sequencing were used to determine the alternative transcripts of WWOX. Statistical analysis were performed by Mann Whitney U-test, Pearson correlation coefficient test at significance level of P value 0.05. Prevalence of HPV was observed in cervicitis (40%), cervical intraepithelial neoplasia patients (50%), and invasive cervical carcinoma patients (89.6%). Clinicopathological findings suggested a correlation of reduced level of WWOX protein and progression of cervical carcinoma deciphering its role in tumorigenesis. Furthermore, we observed aberrant WWOX transcript having deleted exon 6-8 region in invasive cervical cancer tissues as well as normal cervix samples. More than 60% of cervical carcinoma samples showed reduced protein level with an increase in wild type transcript level suggesting the involvement of a negative regulator, pAck1 (activated Cdc42- associated kinase) which might ubiquitinate WWOX protein leading to its degradation. Also, nuclear retention of WWOX transcript in invasive cervical carcinoma tissues suggests its regulation at post-transcriptional level. Our findings suggest that WWOX acts as a tumor suppressor in cervical carcinoma and could act as a potential therapeutic target for the disease.
  • Keywords
    Cervical cancer , clinical , pathological parameters , genotypes , cervical carcinoma patients , WWOX variants
  • Journal title
    International Journal of Molecular and Cellular Medicine(IJMCM)
  • Journal title
    International Journal of Molecular and Cellular Medicine(IJMCM)
  • Record number

    2578127