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Journal ArticleDOI

Correlation between the sensitivity or resistance to IL‐2 and the response to cyclophosphamide of 4 tumors transplantable in the same murine host

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TLDR
The results indicate an inverse correlation between sensitivity to IL‐2 and response to CTX and emphasize the importance of initial host‐tumor interaction in determining the type of response toIL‐2 or CTX.
Abstract
We have studied the anti-tumor response to cyclophosphamide (CTX) in DBA/2 mice transplanted s.c. with 4 tumors exhibiting different responses to IL-2: ESb lymphoma and Friend leukemia cells (non-responsive or poorly responsive, respectively), pI I-R-Eb and Eb lymphoma cells (both highly responsive to IL-2). CTX injections on days 7, 14 and 21 resulted in a significant anti-tumor response in mice transplanted s.c. with Friend leukemia cells or ESb cells, whereas no anti-tumor effect was observed in mice injected with Eb or pI I-R-Eb cells. All 4 tumor cell lines were equally sensitive to the cytotoxic effects of mafosfamide, an in vitro active analogue of CTX. To define the host mechanisms responsible for the lack of an anti-tumor effect of CTX in mice transplanted with IL-2-responsive tumors, we studied several aspects of the spontaneous or IL-2-induced anti-tumor response in mice transplanted with pI I-R-Eb cells. Injection of monoclonal antibodies (MAbs) to IFN-γ completely abolished the anti-tumor effects of IL-2. Using a Winn assay, clear-cut anti-tumor activity was found in spleen cells from mice transplanted with the IL-2-responsive tumors. This activity was abolished by CTX, which also abrogated the anti-tumor response to IL-2 in mice injected with pI I-R-Eb cells. Our results indicate an inverse correlation between sensitivity to IL-2 and response to CTX and emphasize the importance of initial host-tumor interaction in determining the type of response to IL-2 or CTX. © 1995 Wiley-Liss, Inc.

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Journal ArticleDOI

Cyclophosphamide induces type I interferon and augments the number of CD44hi T lymphocytes in mice: implications for strategies of chemoimmunotherapy of cancer

TL;DR: It is demonstrated that CTX is an inducer of type I IFN in vivo and enhances the number of T cells exhibiting the CD44(hi) memory phenotype and provides a new rationale for combined treatments with CTX and adoptive immunotherapy in cancer patients.
Journal ArticleDOI

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

TL;DR: The 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.
Journal ArticleDOI

Influence of hyaluronic acid or phorbol 12-myristate 13-acetate on the migration capacity of a murine lymphoma cell line (Eb) and its metastatic variant (ESb)

TL;DR: In the highly metastatic cell line ESb, which had a low spontaneous locomoting activity, migration could clearly be stimulated by hyaluronic acid whereas only a small increase was found after incubation with phorbol myristate acetate (PMA), the observed stimulation could be attributed to an increase in recruitment of locomoting cells and not to changes in migration parameters of motile individual cells.
References
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Journal ArticleDOI

Augmentation of delayed-type hypersensitivity by doses of cyclophosphamide which do not affect antibody responses.

TL;DR: The results suggest that antibody feedback is not the sole regulator of delayed reactions; the possibility that suppressor T cells may also be involved is discussed.
Journal ArticleDOI

Monoclonal antibody to murine gamma interferon inhibits lymphokine-induced antiviral and macrophage tumoricidal activities

TL;DR: It was found that in relation to the quantity of antibody needed to completely neutralize antiviral activity, much higher concentrations of MAb were required to abolish the capacity of lymphokine preparations to induce macrophage tumoricidal activity in vitro.
Journal ArticleDOI

Effect of cyclophosphamide on immunological control mechanisms.

TL;DR: Cyclophosphamide (CY) given before immunization causes greatly increased delayed hypersensitivity skin reactions and has been found to reverse immunological tolerance where this form of unresponsiveness is due to suppressor cells.
Journal Article

Cyclophosphamide-induced Immunologically Mediated Regression of a Cyclophosphamide-resistant Murine Tumor: A Consequence of Eliminating Precursor L3T4+ Suppressor T-Cells

TL;DR: The results represent a striking example of the negative regulatory influence of suppressor T-cells on the immune response to an immunogenic tumor.
Journal ArticleDOI

Tumor metastases and cell-mediated immunity in a model system in DBA/2 mice. I. Tumor invasiveness in vitro and metastasis formation in vivo.

TL;DR: A syngeneic model system for the study of tumor metastases and cell‐mediated immunity is described and it is revealed that ESb but not Eb tumor cells had the ability to attach to and invade normal tissue and showed higher malignancy in vivo.
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