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[Cancer Research 65, 10079-10087, November 1, 2005]
© 2005 American Association for Cancer Research


Immunology

High Frequencies of Functional Tumor-Reactive T Cells in Bone Marrow and Blood of Pancreatic Cancer Patients

Friedrich H. Schmitz-Winnenthal1, Christine Volk1, Kaspar Z'graggen1,3, Luis Galindo1, Daniel Nummer2, Yvonne Ziouta2, Marianna Bucur2, Jürgen Weitz1, Volker Schirrmacher2, Markus W. Büchler1 and Philipp Beckhove2

1 Department of General Surgery, the University Hospital of Heidelberg; 2 Department of Cellular Immunology, Tumor Immunology Program, the German Cancer Research Center, Heidelberg, Germany; and 3 Berner Viszeralchirurgie Hirslanden, Klinik Beau-Site, Bern, Switzerland

Requests for reprints: Philipp Beckhove, Department of Cellular Immunology, Tumor Immunology Program, the German Cancer Research Center, INF 280, 69120 Heidelberg, Germany. Phone: 49-6221-423-745; Fax: 49-6221-423-702; E-mail: p.beckhove{at}dkfz.de.

Pancreatic cancer is characterized by aggressive growth and treatment resistance. New approaches include immunotherapeutic strategies but the type and extent of spontaneous immune responses against tumor antigens remains unclear. A dominance of TH2 cytokines in patients' sera reported previously suggests systemic tumor-induced immunosuppression, potentially inhibiting the induction of tumor-reactive T cells. We characterized the localization, frequencies, and functional potential of spontaneously induced memory T cells specific for individual tumor antigens or the tumor-associated antigen mucin-1 in the peripheral blood and bone marrow of 41 pancreatic cancer patients. We found high numbers of tumor-reactive T cells in all bone marrow samples and in 50% of the blood samples. These cells secreted the TH1 cytokine IFN-{gamma} rather than TH2 cytokines upon stimulation with tumor antigens. Although consistently induced during pancreatic cancer, T cells specific for pancreatic antigens were not detected during chronic pancreatitis, suggesting that their evaluation may be of diagnostic use in both diseases. Freshly isolated T cells from cancer patients recognized autologous tumor cells and rejected them in vitro and in a xenotransplant model in vivo, suggesting their therapeutic potential. Thus, tumor antigen–specific T cell responses occur regularly during pancreatic cancer disease and lead to enrichment of tumor cell–reactive memory T cells in the bone marrow. The bone marrow can therefore be considered an important organ for antitumor immune responses in pancreatic cancer.




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Copyright © 2005 by the American Association for Cancer Research.