8, 2.2 and 3-fold (P < 0.05) increase in cleaved caspase-3-positive cells over that of control group. These results confirmed the apoptotic effect of Mesothelin shRNA in tumors, which could have been mediated by the caspase-3 pathway. Our results shown buy C188-9 in Capan-2 cells with wt-p53, mesothelin regulated PUMA, bax and bcl-2 through wt-p53 dependent pathway. In Capan-1, MIA PaCa-2 and ASPC-1 cells with mt-p53, mesothelin regulated PUMA, bax and bcl-2 through wt-p53 independent pathway (Figure 6D). Discussion Mesothelin is a glycoprotein to be largely restricted to mesothelial cells or to epithelial cells of the trachea,
tonsils, fallopian tube, and kidneys [21]. Mesothelin has been reported to be a tumour-associated marker in several types of human cancers, including ovarian carcinomas and adenocarcinomas arising from the pancreatico-biliary tract, endometrium, and lungs [22]. Mesothelin has also been reported to interact with CA125 to mediate cell adhesion [23]. Although the biological functions of mesothelin remain largely unknown, there is evidence that mesothelin has the potential as a new cancer biomarker [10] and as a target molecule for gene therapy [24]. Some investigators have reported that mesothelin can be a new
Belinostat supplier marker for the diagnosis of ovarian carcinoma [25] and as a target in mesothelin-expressing tumours [18], including pancreatic cancer [11]. However,the signal transduction pathways induced by mesothelin resulting in cell survival is unclear. In the present study, we have shown that mesothelin was overexpressed in the human pancreatic cancer cell lines. Increased mesothelin is associated with increased cell proliferation of pancreatic cancer cells in vitro and contributes to tumor progression in the nude mouse xenograft model. Silencing of mesothelin expression significantly decreased cell proliferation and promoted apoptosis in pancreatic cancer cells in vitro and inhibited tumor see more growth in vivo. We also shown mesothelin mediated cell survival Prostatic acid phosphatase and apoptosis by
p53-dependent and independent conditions. p53 is a critical regulator of the response to DNA damage and oncogenic stress. Loss of p53 function, through mutation or deletion, is a frequent occurrence in human malignancies. Previous experimental works have converged to indicate that the wt-p53 protein would act as a negative regulator of cell growth [26–28] and a suppressor of transformation and tumonigenesis [29]. In the study reported here, we chose HPAC cells which expressed wt-p53 with less endogenous mesothelin, and Capan-2 cells which expressed wt-p53 with moderate endogenous mesothelin. We found that mesothelin overexpression in HPAC and Capan-2 cells is associated with increased cell proliferation followed by decreased wt-p53. p53 re-inhibition by siRNA in stable mesothelin sliencing Capan-2 and HPAC cells promoted cell survival and proliferation.