Background: Disturbances in the expressions of centrosomal proteins (CEPs) and regulatory proteins that\ncontrol G1-Sphase transition, like cyclins could participate in dysregulation of cell cycle control that has been\nincriminated in the pathogenesis of several malignancies. Centrosomal protein 55 (CEP55) has an important role\nin participation in the final stage of cell division, and cell cycle progression. CEP55 and Cyclin D1 expressions were\ndetected in several tumors but their prognostic and predictive roles in epithelial ovarian carcinoma (EOC) are still\nstudied.\nAim of the study: Explore tissue expressions of CEPP55 and Cyclin D1 in EOC correlating their expression with\npathological, clinical and prognostic parameters.\nMethods: CEP55 and Cyclin D1 expressions were evaluated in tissue biopsies that are retrieved from 60\ncases of epithelial ovarian carcinoma using immunohistochemistry, patients that were followed up for 3 years. The\nrelationship between their level of expressions and degree of differentiation, spread of the tumor, disease recurrence,\nresponse to therapy and survival were studied.\nResults: CEP55 expression in EOC was positively correlated with loss of differentiation of the tumor, presence of\nL.N (p<0.001), and distant metastases (p=0.012) and advanced stage of the tumor (p=0.007), cyclin D1 expression\nin EOC was positively correlated with loss of differentiation and advanced stage of the tumor, presence of L.N\n(p<0.001), and distant metastases (p=0.009). CEPP 55 and Cyclin D1 were positively correlated with each other.\nLow CEPP 55 and Cyclin D1 expressions were strongly correlated with optimal surgical eradication of the tumor,\nincreased 3-year overall survival (OS) and low incidence of tumor recurrence after therapy (P<0.001).\nConclusion: High levels of expression of CEPP 55 and Cyclin D1and are markers of poor prognosis in EOC\npatients.
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