Title of article :
P53/MDM2 CO-EXPRESSION CORRELATES WITH THE TUMOUR DIFFERENTIATION IN ORAL SQUAMOUS CELL CARCINOMA – A RETROSPECTIVE STUDY AND A SYSTEMATIC REVIEW
Author/Authors :
Choon, Y.F. university of malaya - Faculty of Dentistry - Department of Oral Pathology, Oral Medicine and Periodontology, Malaysia , Ramanathan, A. university of malaya - Oral Cancer Research and Coordinating Centre, Faculty of Dentistry - Department of Oral Pathology, Oral Medicine and Periodontology, Malaysia , Ali, H. university of malaya - Oral Cancer Research and Coordinating Centre, Faculty of Dentistry, Malaysia , Ghani, W.M.N. university of malaya - Oral Cancer Research and Coordinating Centre, Faculty of Dentistry, Malaysia , Cheong, S.C. university of malaya - Faculty of Dentistry - Department of Oral and Maxillofacial Surgery, Malaysia , Cheong, S.C. Cancer Research Initiatives Foundation (CARIF) - Oral Cancer Research Team, Sime Darby Medical Centre, Malaysia , Zain, R.B. university of malaya - Oral Cancer Research and Coordinating Centre, Faculty of Dentistry - Department of Oral Pathology, Oral Medicine and Periodontology, Malaysia
Abstract :
Background: MDM2 and p53 are involved in a negative feedback loop where p53 regulates MDM2 at the transcriptional level. MDM2, in turn, downregulates p53. This co-ordinated interaction between these proteins is set to play an important role in the regulation of cell cycle progression following DNA damage to cells. The over-expression of both p53 and MDM2 has been reported in various cancers. However there are only few studies discussing the co-expression of MDM2 with p53 in oral squamous cell carcinoma Aim: The purpose of this study was to determine the correlation of co-expression of p53, MDM2, and Ki-67 proteins with clinico-pathological factors in oral squamous cell carcinoma (OSCC) and to conduct a systematic review of the co-expression of p53/MDM2. Method: This is a retrospective descriptive study and a systematic review. Formalin-fixed paraff inembedded tissues from 45 OSCC cases were stained by immunohistochemistry (IHC) for p53, MDM2, and Ki-67 proteins. Results: Immuno-reactivity for p53, MDM2, and Ki-67 was seen in 75.6%, 97.8%, and 62.2% cases of OSCC respectively. The co-expression of p53 and MDM2 (p53/MDM2) was detected in 97.1%, however there was no signif icant correlation between p53 and MDM2 expression. Notably, p53/MDM2 coexpression was significantly associated with tumour differentiation (p-value = 0.045). The Ki-67LI was not signif icantly associated with neither MDM2 nor p53/MDM2 co-expression (p-value = 0.268, 0.916 respectively). Conclusion: The expression of MDM2 was not signif icantly associated with p53 expression suggesting that MDM2 expression is mediated by p53-independent pathways or mutated p53 could not induce the expression of MDM2 in this set of OSCCs. The only clinico-pathological parameter that correlates significantly with co-expression of p53/MDM2 is tumour differentiation where it is suggestive that the co-expression of these 2 proteins is indicative of aggressive tumour behavior.
Keywords :
Oral squamous cell carcinoma , MDM2 , p53 , Ki , 67 , immunohistochemistry , systematic review
Journal title :
Annals of Dentistry University of Malaya
Journal title :
Annals of Dentistry University of Malaya
