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Citations to this article

Importance of cyclophosphamide-induced bystander effect on T cells for a successful tumor eradication in response to adoptive immunotherapy in mice.
E Proietti, … , D Carlei, F Belardelli
E Proietti, … , D Carlei, F Belardelli
Published January 15, 1998
Citation Information: J Clin Invest. 1998;101(2):429-441. https://doi.org/10.1172/JCI1348.
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Research Article

Importance of cyclophosphamide-induced bystander effect on T cells for a successful tumor eradication in response to adoptive immunotherapy in mice.

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Abstract

Cyclophosphamide (CTX) increases the antitumor effectiveness of adoptive immunotherapy in mice, and combined immunotherapy regimens are now used in some clinical trials. However, the mechanisms underlying the synergistic antitumor responses are still unclear. The purpose of this study was (a) to evaluate the antitumor response to CTX and adoptive immunotherapy in mice bearing four different syngeneic tumors (two responsive in vivo to CTX and two resistant); and (b) to define the mechanism(s) of the CTX-immunotherapy synergism. Tumor-bearing DBA/2 mice were treated with a single injection of CTX followed by an intravenous infusion of tumor-immune spleen cells. In all the four tumor models, a single CTX injection resulted in an impressive antitumor response to the subsequent injection of spleen cells from mice immunized with homologous tumor cells independently of the in vivo response to CTX alone. Detailed analysis of the antitumor mechanisms in mice transplanted with metastatic Friend leukemia cells revealed that (a) the effectiveness of this combined therapy was dependent neither on the CTX-induced reduction of tumor burden nor on CTX-induced inhibition of some putative tumor-induced suppressor cells; (b) the CTX/immune cells' regimen strongly protected the mice from subsequent injection of FLC, provided the animals were also preinoculated with inactivated homologous tumor together with the immune spleen cells; (c) CD4(+) T immune lymphocytes were the major cell type responsible for the antitumor activity; (d) the combined therapy was ineffective in mice treated with antiasialo-GM1 or anti-IFN-alpha/beta antibodies; (e) spleen and/ or bone marrow cells from CTX-treated mice produced soluble factors that assisted in proliferation of the spleen cells. Altogether, these results indicate that CTX acts via bystander effects, possibly through production of T cell growth factors occurring during the rebound events after drug administration, which may sustain the proliferation, survival, and activity of the transferred immune T lymphocytes. Thus, our findings indicate the need for reappraisal of the mechanisms underlying the synergistic effects of CTX and adoptive immunotherapy, and may provide new insights into the definition of new and more effective strategies with chemotherapy and adoptive immunotherapy for cancer patients.

Authors

E Proietti, G Greco, B Garrone, S Baccarini, C Mauri, M Venditti, D Carlei, F Belardelli

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TP Yeo, RH Hruban, SD Leach, RE Wilentz, TA Sohn, SE Kern, CA Iacobuzio-Donahue, A Maitra, M Goggins, MI Canto, RA Abrams, D Laheru, EM Jaffee, M Hidalgo, CJ Yeo
Current Problems in Cancer 2002
Chemo-immunotherapy and chemo-adoptive immunotherapy of cancer
GG Gomez, RB Hutchison, CA Kruse
Cancer Treatment Reviews 2001
Bryostatin/Ionomycin-Activated T Cells Mediate Regression of Established Tumors
CS Chin, LJ Graham, GG Hamad, KR George, HD Bear
Journal of Surgical Research 2001
Surgical Research
J Rozga, AA Demetriou
Surgical Research 2001
Cyclophosphamide Induces the Development of Early Myeloid Cells Suppressing Tumor Cell Growth by a Nitric Oxide-Dependent Mechanism
B Peláez, JA Campillo, JA López-Asenjo, JL Subiza
Journal of immunology (Baltimore, Md. : 1950) 2001
Anti-Tumor Immunity Provided by a Synthetic Multiple Antigenic Glycopeptide Displaying a Tri-Tn Glycotope
R Lo-Man, S Vichier-Guerre, S Bay, E Dériaud, D Cantacuzène, C Leclerc
Journal of immunology (Baltimore, Md. : 1950) 2001
Cyclophosphamide enhances anti-tumor effect of wild-type p53-specific CTL
MP Vierboom, GM Bos, M Ooms, R Offringa, CJ Melief
International Journal of Cancer 2000
High- and low-dose interferon alfa-2b in high-risk melanoma: first analysis of intergroup trial E1690/S9111/C9190
F Belardelli, M Ferrantini, E Proietti, JM Kirkwood
Journal of Clinical Oncology 2000
Cyclophosphamide induces type I interferon and augments the number of CD44hi T lymphocytes in mice: implications for strategies of chemoimmunotherapy of cancer
G Schiavoni, F Mattei, TD Pucchio, SM Santini, L Bracci, F Belardelli, E Proietti
Blood 2000
Relatively low-dose cyclophosphamide is likely to induce apoptotic cell death in rat thymus through Fas/Fas ligand pathway
GJ Wang, L Cai
Mutation Research/Fundamental and Molecular Mechanisms of Mutagenesis 1999

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