For the analyses using the t test for independent samples and the

For the analyses using the t test for independent samples and the Pearsons test, the NPM1 expression in tumor sam ples was calibrated by their matched non neoplastic counterpart. selleck kinase inhibitor In all analyses, P 0. 05 was considered significant. Results NPM1 protein expression was significantly reduced in GC samples compared to matched non neoplastic gastric samples. The protein level of NPM1 was reduced at least 1. 5 fold in 35% of GC samples, and no tumor presented an increase in expression of 50% compared to their paired non Inhibitors,Modulators,Libraries neoplastic gastric tissue. In all cases, the NPM1 immunoreactivity was detected in neoplastic and non neoplastic cells, including in in testinal metaplastic, gastritis and inflammatory cells. NPM1 was mainly expressed in nucleus and nucleolus. Only one case presented cytoplasmatic staining in the parietal cells.

The staining in tensity and the percentage of immunoreactive cells varied among the studied cases. In nuclei of tumor cells, NPM1 immunoreactivity score ranged from 0 to 2, with 41. 7% cases presenting score 0. In nucleoli of tumor cells, 5 of 12 cases presented score 0 and 7 of 12 presented score 2. The score of NPM1 immunore Inhibitors,Modulators,Libraries activity in the nucleoli of tumor cells was inversely cor related with the protein expression by Western blot. The NPM1 mRNA expression did not differ between GC and matched non neoplastic gastric samples. The NPM1 mRNA level was reduced at least 1. 5 fold in 45. 5% of samples and increased in 27. 3% of samples. A moderate inverse correlation was ob served between the relative quantifications of NPM1 protein and mRNA levels.

The intestinal type GC presented higher NPM1 mRNA levels than diffuse type GC. The mRNA Batimastat expression was at least 50% reduced in all diffuse type. In the intestinal type, the mRNA expression was less than 1. 5 fold in 25% of cases and greater than 1. 5 fold in 37. 5% in relation to their matched Inhibitors,Modulators,Libraries non neoplastic counterpart. On the other hand, the NPM1 protein level did not differ between diffuse type and intestinal type GC. However, intestinal type GC presented a significant reduc tion of NPM1 protein expression compared to matched non neoplastic gastric samples. In addition, the protein level of NPM1 was reduced at least 1. 5 fold in 46. 2% of intestinal type GC and in no case of diffuse type GC. Tumors from patients with known distant metastasis showed reduced NPM1 protein Inhibitors,Modulators,Libraries expression compared to tumors from patients without distant metastasis.

No association selleck chemical between NPM1 expression and any other clinicopathological characteris tics was found. Discussion NPM1 is a multifunctional protein. The first proposed role of NPM1 was in the regulation of cell growth, proliferation and transformation because its expression increases in response to mitogenic stimuli and is up regulated in highly proliferative and malignant cells. However, se veral recent studies have demonstrated that NPM1 has both proliferative and growth suppressive roles in the cell.

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