Abstract

Recent studies have suggested that successful antitumor responses consisted of a combination of T cell-mediated and non-T cell-mediated mechanisms. We have used transplantable mouse renal and autochthonous mammary carcinoma models to demonstrate that the systemic administration of the combination of IL-2 + IL-12 yields enhanced antitumor effects against even well-established metastatic cancers. Further, the local injection of replication-defective pox viruses (pv) modified to express Il-12 also induces potent antitumor effects against transplantable renal and lung tumors. The mechanism for these effects is complex, and depends on the presence of CD8 positive T cells for induction of the response. However, the effector phase occurs in the absence of a large accumulation of T cells at the tumor site; but does coincide with the development of anti-neovascular effects, enhanced induction of chemokines and Th1 cytokines, reduced production of Th2 cytokines, and a reversal of the tumor-induced inhibition of nitric oxide production. In addition, the systemic (IV) administration of pv IL-12 + systemic IL-2 is able to reduce the number of pre-existing hepatic metastases by about 95%. Additional studies have shown that the recruitment of antitumor effector NK and T cells to tumors may be impaired because of inappropriate expression of the requisite adhesion molecules in tumor neovasculature. However, our studies also have shown for the first time that the cytokine-induced redistribution of NK cell to parenchymal organs that are often the site of metastases formation are critically dependent on the interaction of the VCAM-1/VLA-4 adhesion/ligand pair. Further, the results have shown that IL-2 and IL-12 differentially regulate the recruitment of NK vs T cells to the liver. Overall, these results demonstrate that the successful induction and mediation of antitumor effects results from complex events that depend on both T cell-mediated and T cell-dependent, non-T cell-mediated processes. By understanding the relative contributions of these different, but related processes, we should gain new insight into biological mechanisms that can be exploited for the treatment of cancer.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Intramural Research (Z01)
Project #
1Z01BC009262-14
Application #
2463762
Study Section
Special Emphasis Panel (LEI)
Project Start
Project End
Budget Start
Budget End
Support Year
14
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
National Cancer Institute Division of Basic Sciences
Department
Type
DUNS #
City
State
Country
United States
Zip Code

  Publications

Kudo-Saito, Chie; Wansley, Elizabeth K; Gruys, M Eilene et al. (2007) Combination therapy of an orthotopic renal cell carcinoma model using intratumoral vector-mediated costimulation and systemic interleukin-2. Clin Cancer Res 13:1936-46
Kummar, Shivaani; Kinders, Robert; Rubinstein, Larry et al. (2007) Compressing drug development timelines in oncology using phase '0'trials. Nat Rev Cancer 7:131-9
Peter, Marcus E; Budd, Ralph C; Desbarats, Julie et al. (2007) The CD95 receptor: apoptosis revisited. Cell 129:447-50
Weiss, Jonathan M; Subleski, Jeff J; Wigginton, Jon M et al. (2007) Immunotherapy of cancer by IL-12-based cytokine combinations. Expert Opin Biol Ther 7:1705-21
Yazawa, H; Murakami, T; Li, H-M et al. (2006) Hydrodynamics-based gene delivery of naked DNA encoding fetal liver kinase-1 gene effectively suppresses the growth of pre-existing tumors. Cancer Gene Ther 13:993-1001
Shorts, Lynnette; Weiss, Jonathan M; Lee, Jong-Keuk et al. (2006) Stimulation through CD40 on mouse and human renal cell carcinomas triggers cytokine production, leukocyte recruitment, and antitumor responses that can be independent of host CD40 expression. J Immunol 176:6543-52
Ortaldo, John R; Winkler-Pickett, Robin T; Bere Jr, Earl W et al. (2005) In vivo hydrodynamic delivery of cDNA encoding IL-2: rapid, sustained redistribution, activation of mouse NK cells, and therapeutic potential in the absence of NKT cells. J Immunol 175:693-9
Welniak, Lisbeth A; Shorts, Lynnette; Subleski, Jeff et al. (2004) Tumor regression by anti-CD40 and interleukin-2: role of CD40 in hematopoietic cells and organ-specific effects. Biol Blood Marrow Transplant 10:534-9
Ortaldo, John R; Young, Howard A; Winkler-Pickett, Robin T et al. (2004) Dissociation of NKT stimulation, cytokine induction, and NK activation in vivo by the use of distinct TCR-binding ceramides. J Immunol 172:943-53
Hussain, S Perwez; Trivers, Glennwood E; Hofseth, Lorne J et al. (2004) Nitric oxide, a mediator of inflammation, suppresses tumorigenesis. Cancer Res 64:6849-53

Showing the most recent 10 out of 18 publications