ince Luciferase may stimulate a certain degree of immune recognition as a foreign protein, we continued to use both Renca-Luc and parental Renca in the following experiments, as each cell type presents unique advantages. Local administration of Ad5mTRAIL+CpG immunotherapy leads to regression of primary renal tumors Adenovirus-Encoded TRAIL Therapy of Metastatic RCC static RCC, mice were challenged with parental Renca cells and treated IR on d 7 with PBS or Ad5mTRAIL+CpG. Kidneys were harvested at d 12 for staining and flow cytometric analysis to determine the extent to which the therapy led to increased T cell infiltration into tumor-bearing kidneys. Administration of Ad5mTRAIL+CpG led to striking increases in the percentage of T cells in tumor-bearing kidneys. As shown, Cediranib chemical information approximately 96% of gated CD8 T cells and 100% of gated CD4 T cells were CD44high/CD62Llow, reflecting differentiation to an effector phenotype. We next asked if the influx of effector T cells into the kidney resulted in renal tumor regression. Mice were challenged IR with parental Renca, then on d 7 were given an IR dose of PBS, CpG alone, Ad5mTRAIL alone, or Ad5mTRAIL+CpG; or were left untreated. On d 23, tumor-challenged kidneys were excised and weighed to evaluate primary tumor growth. Three experimental groups showed significantly increased kidney weights as compared to tumor-free control kidneys. In contrast, kidneys from mice that received Ad5mTRAIL+CpG on d 7 remained statistically unchanged in weight through d 23 . These data indicate that tumors did not grow progressively in mice that received Ad5mTRAIL+CpG on d 7, as they did in mice that received PBS, CpG, or Ad5mTRAIL alone. We also found that IR administration of PBS on d 7 did not alter primary renal tumor outgrowth as compared to mice that received no IR injections on d 7, suggesting that physical trauma associated with a second IR injection did not alter the course of tumor outgrowth. Histological evaluations of tumor-challenged kidneys revealed that increased kidney weights were due to solid tumor growth and not merely to an influx of inflammatory cells. Thus, only the combination of Ad5mTRAIL+CpG was effective at controlling renal tumor outgrowth. Both CD4 and CD8 T cells can mediate tumor regression, and the relative contribution of each lymphocyte population may vary depending on the tumor model. PubMed ID:http://www.ncbi.nlm.nih.gov/pubmed/22180839 To identify the contributions of CD4 and CD8 T cells in protective antitumor immunity that resulted from Ad5mTRAIL+CpG administration, we performed IR tumor challenges with parental Renca cells as above, then depleted mice of either CD4 or CD8 cells prior to giving immunotherapy on d 7. Depletion of CD8 cells prior to Adenovirus-Encoded TRAIL Therapy of Metastatic RCC Ad5mTRAIL+CpG therapy resulted in a significant increase in primary renal tumor size, indicating that in the absence of CD8 cells, Ad5mTRAIL+CpG therapy was no longer effective. Depletion of CD4 cells led to a slight increase in primary renal tumor size as compared to non-depleted mice, but this difference was not statistically significant. The latter finding is in contrast to our previous results in the s.c. Renca model, wherein CD4 depletion actually enhanced the efficacy of Ad5mTRAIL+CpG therapy. Both gross and histological examination of kidneys showed that PBS-treated mice developed bulky renal tumors that obliterated normal kidney structure and greatly increased the overall kidney size. In contrast, kidneys from mice that received Adeno
Calcimimetic agent
Just another WordPress site