Expression of p53 family members and CD44 in oral squamous cell carcinoma (OSCC) in relation to tumorigenesis

Pauline Bidaud¹, Jacques Chasle^1,2, François Sichel¹, Stéphane Rousseau¹, Pascal Petit², Didier Pottier¹, Jean-Michel Picquenot³, Marie-Yolande Louis⁴ and Mathilde Lechevrel<sup>1

1</sup>GRECAN-IFR146 ICORE, François Baclesse Center and University of Caen, Caen, France, ²Department of Anatomopathology, François Baclesse Center, Caen, France, ³Department of Anatomopathology, Henri Becquerel Center, Rouen, France and ⁴Department of Maxillofacial surgery, François Baclesse Center, Caen, France.

Offprint requests to: Dr Mathilde Lechevrel, GRECAN Centre François Baclesse, 3, avenue du Général Harris, B.P. 5026, 14076 CAEN Cedex 05, France. e-mail: mathilde.lechevrel@unicaen.fr


Summary. Oral squamous cell carcinomas (OSCCs) are described as the result of a multistep tumorigenesis process. In order to develop useful diagnosis of pre-malignant lesions, expression of p53 family members and the cancer stem cell (CSCs) marker, CD44v6, were studied in histologically normal oral epithelium, precancerous lesions and succeeding invasive OSCCs. p53 was expressed focally in normal epithelium adjacent to tumors, while expression was high in intra-epithelial neoplasia and moderate in OSCC. p63 nuclear staining was important in basal and suprabasal layers of histologically normal oral mucosa and in immature compartments of premalignant lesions and cancer. In epithelium without neoplasia, intense p73 staining was observed in the basal layer, while focal expression was present in suprabasal layers. Most immature dysplastic areas showed either high or moderate staining, whereas those in OSCCs expressed low and moderate p73 level expression. CD44v6 was only expressed in poorly differentiated areas of epithelium, altered or not. p53, p63 and p73 positive stainings were statistically related in intra-epithelial neoplasia to tumours. Analysis of TP53 mutations in 17% of tumours principally revealed G>A and A>G transitions. No relation was observed between this mutational profile and different immunostainings. In conclusion, our results support that immunostaining of p53 family members might be helpful in diagnosis and monitoring of high-risk pre-malignant lesions of oral epithelium. The combination of staining patterns of p63, p73α and CD44v6 enabled us to isolate phenotypic undifferentiated or transient amplifying areas, reflecting the immaturity of the tumour cell lineage. While CD44v6 expression is an interesting marker of such epithelial cells, it is not specific enough to be useful alone and other phenotypic markers are needed. Histol Histopathol 25, 331-339 (2010)

Key words: OSCC, p53, p63, p73, CD44

DOI: 10.14670/HH-25.331