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Depressed Cell-Mediated Immunity in Newborn Rabbits Bearing Fibroma Virus-Induced Tumors

机译:患有纤维瘤病毒诱导的肿瘤的新生兔的细胞介导的免疫抑制

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Tumors were induced in adult and newborn rabbits by inoculation of fibroma virus. Whereas tumors completely regressed in adult rabbits by 3 weeks after virus inoculation, newborn rabbits supported tumor growth for 3 to 4 weeks. In the latter case, some animals died at this time, others survived with a gradual regression of the tumors over an additional period of 5 to 6 weeks. Virus neutralization studies demonstrated antibodies to fibroma virus in the serum from both adult and newborn tumor-bearing rabbits. Newborn rabbits with progressively growing tumors failed to elicit a delayed cutaneous hypersensitivity reaction to fibroma antigens, whereas adult rabbits showed strong reactions as early as 7 days after tumor induction. Similarly, macrophage migration inhibition tests revealed that the lymphocytes from newborn rabbits with progressively growing tumors were only weakly reactive to fibroma antigens, as compared to lymphocytes from adult tumorbearing rabbits. In contrast, newborn rabbits that survived and regressed the tumors demonstrated strong cell-mediated immunity both by skin testing and migration inhibition. Virus growth studies in cell culture demonstrated that fibroma was unable to replicate in peritoneal macrophages from either newborn or adult rabbits. No differences were observed in growth of the virus in macrophages from tumor-bearing rabbits. The significance of these observations is discussed in respect of the possible role of cell-mediated immunity in fibroma tumor regression.
机译:接种纤维瘤病毒可在成年和新生兔中诱发肿瘤。接种病毒后3周,成年兔的肿瘤完全消退,而新生兔则支持肿瘤生长3至4周。在后一种情况下,一些动物此时死亡,另一些动物存活了下来,并在5到6周的额外时间内肿瘤逐渐消退。病毒中和研究表明,成年和新生荷瘤兔血清中的纤维瘤病毒抗体。肿瘤逐渐生长的新生兔子未能引起对纤维瘤抗原的延迟皮肤超敏反应,而成年兔子早在肿瘤诱导后7天就表现出强烈反应。同样,巨噬细胞迁移抑制试验表明,与成年荷瘤兔的淋巴细胞相比,肿瘤逐渐生长的新生兔的淋巴细胞对纤维瘤抗原的反应较弱。相反,存活并消退了肿瘤的新生兔子通过皮肤测试和迁移抑制均表现出强大的细胞介导的免疫力。细胞培养中的病毒生长研究表明,纤维瘤无法在新生或成年兔的腹膜巨噬细胞中复制。在荷瘤兔的巨噬细胞中病毒的生长没有观察到差异。关于细胞介导的免疫在纤维瘤肿瘤消退中的可能作用,讨论了这些观察结果的意义。

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