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Selective immunosuppression resulting from exposure to the carcinogenic congener of benzopyrene in B6C3F1 mice.

机译:B6C3F1小鼠暴露于苯并re致癌同类物而产生的选择性免疫抑制。

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摘要

B6C3F1 mice were exposed to two congeners of benzopyrene, either the carcinogen benzo(a)pyrene (B(a)P) or the non-carcinogen benzo(e)pyrene (B(e)P. Exposure of mice to B(a)P resulted in a reduced number of IgM and IgG antibody plaque forming cells (PFC) to the T-dependent (TD) antigen SRBC and IgM PFC's to the T-independent (TI) antigen LPS. The IgM response to hapten conjugated TI antigens was examined using TNP-LPS for reactivity of less mature B cells (B1) and TNP-Ficoll for more mature B cells (B2). Exposure to B(a)P severely depressed the TNP-Ficoll PFC response by up to 77% without altering the TNP-LPS response. These data indicated that exposure to B(a)P alters differentiation and antibody production in mature B cells to both TD and B2 TI antigens. No change in PFC was observed following exposure to B(e)P. Mishell-Dutton co-cultures confirmed that B cells were affected and that T helper cells or suppressor Mphi were not involved. Parameters of cell-mediated immunocompetence including delayed cutaneous hypersensitivity to KLH, allograft or tumour cell rejection and susceptibility to Listeria monocytogens were unaltered in B(a)P treated mice.
机译:B6C3F1小鼠暴露于苯并py的两个同类物,即致癌物苯并(a)py(B(a)P)或非致癌物苯并(e)re(B(e)P)。 P导致针对T依赖性(TD)抗原SRBC的IgM和IgG抗体斑块形成细胞(PFC)的数量减少,而针对T非依赖性(TI)抗原LPS的IgM PFC的数量减少。使用TNP-LPS对较不成熟的B细胞(B1)和TNP-Ficoll对较成熟的B细胞(B2)的反应进行了检测。暴露于B(a)P会使TNP-Ficoll PFC反应严重降低了77%,而没有改变这些数据表明,暴露于B(a)P会改变成熟B细胞对TD和B2 TI抗原的分化和抗体产生,而暴露于B(e)P则未观察到PFC的变化。 -Dutton共培养证实B细胞受到影响,而T辅助细胞或抑制性Mphi不受影响。由于延迟对KLH的皮肤超敏反应,同种异体移植或肿瘤细胞排斥以及对单核细胞增生李斯特菌的敏感性在B(a)P治疗的小鼠中未改变。

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