Role of T suppressor cells in the cycling of the immune response against a murine fibrosarcoma

Payelle, B; Lespinats, G; Tlouzeau, Sylvie

doi:10.1002/ijc.2910340117

Cited by 4 publications

(2 citation statements)

References 28 publications

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“…Drebin et al, however, demonstrated that Lyt-1-.2.3 ÷ Ts are generated as early as 24 h after the s.c. tumor inoculation (33). Furthermore, it has been demonstrated by several authors (34)(35)(36)(37)(38)(39)(40) that Ts are largely Lyt-2 cells, although they carry small numbers of Lyt-1 determinants. Presumably, suppression by Lyt-1-.2.3 + Ts is an example of T-cell-mediated unresponsiveness (passive suppression), in contrast to active T-cell-mediated suppression.…”

Section: Discussionmentioning

confidence: 99%

Temporal changes of suppressor T lymphocytes and cytotoxic T lymphocytes in syngeneic murine malignant gliomas

et al. 1986

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The temporal activities of suppressor T lymphocytes (Ts) and cytotoxic T lymphocytes (CTL) were investigated in a syngeneic murine malignant glioma (a methylcholanthrene-induced ependymoblastoma of C57BL/6 mouse origin, 203-glioma). After the s.c. tumor inoculation, it was suggested that both Ts and CTL were generated with target specificity against 203-glioma cells, because neither Ts nor CTL activity were seen against syngeneic EL 4 (benzpyrene-induced thymoma), allogeneic P815 (methylcholanthrene-induced mastocytoma of DBA/2 mouse origin) or YAC-1 (Moloney leukemia-induced T-cell lymphoma of A/Sn mouse origin), but only against 203-glioma. It was found that the generation of Ts preceded that of CTL and that the turnover was faster; furthermore, Ts were generated in the thymus and spleen, while CTL were distributed in regional lymph nodes and spleen. Surface marker analysis revealed that only Lyt-1-.2.3+ T-cells participated in suppressor responses in contrast to both Lyt-1-.2.3+ and Lyt-1+.2.3+ T-cells participating in cytotoxic responses. The effects of adult thymectomy (ATx) on the changes of the immunized T-cell subsets were also investigated. In mice thymectomized 3 weeks previously, the Ts activity was abrogated, whereas the CTL activity increased markedly and Lyt-1+.2.3+ T-cells were not detected. The results suggest that CTL or their precursors bearing Lyt-1+.2.3+ phenotype and Ts bearing Lyt-1-.2.3+ phenotype are short-lived lymphocytes. Accordingly, it is suggested that in tumor-bearing mice short-lived Ts are generated earliest with target specificity and, due to the reciprocal relationships between Ts and CTL activities, may have a modulating influence on CTL; furthermore, ATx may alter the patterns of generation of the precursor T-cells and Ts.

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Section: Discussionmentioning

confidence: 99%

Temporal changes of suppressor T lymphocytes and cytotoxic T lymphocytes in syngeneic murine malignant gliomas

et al. 1986

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“…For example, the expression of H-2D, in association with tumor-associated target antigens, might bx&rt a regulatory effect on the specific immune response against the tumor. This might occur through interactions with suppressive immune components such as suppressor T cells (49) or by induction of CTL's capable of recognizing T-cell receptor structures on CTL's specific for the tumor (50). Such specific immune suppression could explain the lack of immunogenicity associated with these subclones (51).…”

Section: Enhancement and Activation Of Class I Sequences In Tumorsmentioning

confidence: 98%

Histocompatibility Antigens on Murine Tumors

Goodenow

Vogel

Linsk

1985

Science

156

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Recent advances in tumor immunology suggest that the expression of the histocompatibility antigens, encoded by the major histocompatibility complex, is important in controlling the metastatic growth of certain murine tumors. The anomalous expression of histocompatibility antigens in many neoplasms appears to be associated with the ability of these cells to evade the immune system and progress to metastasis. This review examines some of the underlying molecular and immunobiological interactions that might determine the metastatic outcome of cellular transformation.

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Suppressor Cells and Malignancy

Naor¹,

Duke‐Cohan²

1986

Advances in Immunity and Cancer Therapy

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Role of T suppressor cells in the cycling of the immune response against a murine fibrosarcoma

Cited by 4 publications

References 28 publications

Temporal changes of suppressor T lymphocytes and cytotoxic T lymphocytes in syngeneic murine malignant gliomas

Temporal changes of suppressor T lymphocytes and cytotoxic T lymphocytes in syngeneic murine malignant gliomas

Histocompatibility Antigens on Murine Tumors

Suppressor Cells and Malignancy

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