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病毒诱导肿瘤及其免疫治疗的模型研究(作者译)

[Model studies on virus-induced tumors and their immunological treatment (author's transl)].

作者信息

Schäfer W

出版信息

Klin Wochenschr. 1977 Sep 1;55(17):835-46. doi: 10.1007/BF01491299.

Abstract

After a review of the general biological properties of C-type oncorna viruses, results are presented on the structure of an exogenous murine leukemia virus (FLV) and on the serobiological properties of its structural proteins. Our findings suggested a major role of the viral surface glycoprotein gp71 in immunological defense mechanisms. This was confirmed by vaccination experiments with isolated gp71 in mice. The induced immunity was highly specific and not operative against endogenous murine C-viruses belonging to other serotypes. Surprisingly the latter were found to be activated by the vaccination with gp71 of FLV. In heterologous animal species isolated FLV-gp71 induced the formation of broadly reacting antibodies. They were found to be effective in the therapy of infections with FLV in mice as well as with feline leukaemia virus in cats. Most impressive results were obtained with an antiserum prepared against feline leukaemia virus in a goat. This serum completely suppressed sarcomas induced by infection with feline sarcoma virus.

摘要

在回顾了C型肿瘤病毒的一般生物学特性之后,本文给出了关于外源性小鼠白血病病毒(FLV)的结构及其结构蛋白的血清生物学特性的研究结果。我们的研究结果表明,病毒表面糖蛋白gp71在免疫防御机制中起主要作用。这一点通过在小鼠中用分离出的gp71进行疫苗接种实验得到了证实。诱导产生的免疫力具有高度特异性,对属于其他血清型的内源性小鼠C病毒不起作用。令人惊讶的是,发现后者可被用FLV的gp71进行的疫苗接种激活。在异种动物中,分离出的FLV-gp71诱导产生了广泛反应的抗体。发现它们在治疗小鼠的FLV感染以及猫的猫白血病病毒感染方面有效。用在山羊体内制备的抗猫白血病病毒抗血清获得了最令人印象深刻的结果。这种血清完全抑制了由猫肉瘤病毒感染诱导产生的肉瘤。

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