Investigation of the differential genetic expression in reply to the effect of the anti-inflammatory protein Anexina A1 in the cervical carcinoma

Abstract

The cervical cancer is the second type of more frequent cancer in women world-wide, being the fourth cause of death for cancer in developing countries. Cervical carcinogenesis is related with genetic alterations, infection for Human PapilomaVirus (HPV), angiogenesis and inflammatory processes. The idea of that the inflammation is involved in tumorigenesis is supported by the comment of that the cancer appears frequently in areas of chronic inflammation. On the other hand, the inflammatory reply is controlled for the action of anti-inflammatory mediators, who act to keep the homeostasis of the immunological reply to prevent the tecidual injury. Among these mediators we detach the annexin A1 (ANXA1), protein of 37 kDa, that is express for the tumoral cells and acts as modulating of the inflammatory process. However, the molecular mechanisms for which the ANXA1 modulates the cellular answers in the inflammatory processes are not yet completely determined. The available data suggest that this protein family can have, beyond its important role in the inflammatory process, a significant involvement in the cancer, through signaling cascades that include genes related with the cellular cycle, the differentiation and apoptosis. Ahead of these considerations, we will investigate, in vitro, the influence of this anti-inflammatory one in the SiHa cells on the morphology, cellular proliferation and localization and in the proteic and gene expression, observing as the ANXA1 modulates the expression of these genes and as these alterations can participate of the tumorigenic process. For this, the cell line SiHa will be used (derived from the cervical squamous cell carcinoma), treated with ANXA1 for 1, 2, 4, 24, 48 and 72 hours. Specifically, it will be investigated the effect of this addition in the gene expression, by rapid subtractive hybridization (RaSH) and the differentially expressed genes distinguishing, will be validated by techniques of quantitative PCR, then, will be investigated the ways of cellular signaling, of which the ANXA1 participates, important for the tumorigenic process.