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Mouse Model of Devil Facial Tumour Disease Establishes That an Effective Immune Response Can be Generated Against the Cancer Cells

机译:魔鬼面部肿瘤疾病的小鼠模型建立可以针对癌细胞生成有效的免疫反应

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摘要

The largest carnivorous marsupial in Australia, the Tasmanian devil (Sarcophilus harrisii) is facing extinction in the wild due to a transmissible cancer known as Devil Facial Tumour Disease (DFTD). DFTD is a clonal cell line transmitted from host to host with 100% mortality and no known immunity. While it was first considered that low genetic diversity of the population of devils enabled the allograft transmission of DFTD recent evidence reveals that genetically diverse animals succumb to the disease. The lack of an immune response against the DFTD tumor cells may be due to a lack of immunogenicity of the tumor cells. This could facilitate transmission between devils. To test immunogenicity, mice were injected with viable DFTD cells and anti-DFTD immune responses analyzed. A range of antibody isotypes against DFTD cells was detected, indicating that as DFTD cells can induce an immune response they are immunogenic. This was supported by cytokine production, when splenocytes from mice injected with DFTD cells were cultured in vitro with DFTD cells and the supernatant analyzed. There was a significant production of IFN-γ and TNF-α following the first injection with DFTD cells and a significant production of IL-6 and IL-10 following the second injection. Splenocytes from naïve or immunized mice killed DFTD cells in in vitro cytotoxicity assays. Thus, they are also targets for immunological destruction. We conclude that as an immune response can be generated against DFTD cells they would be suitable targets for a vaccine.
机译:塔斯马尼亚恶魔(Sarcophilus harrisii)是澳大利亚最大的食肉有袋动物,由于一种称为恶魔面部肿瘤病(DFTD)的可传播癌症而在野外面临灭绝。 DFTD是一种在宿主之间传播的克隆细胞系,死亡率为100%,并且没有已知的免疫力。虽然最初被认为是恶魔种群的低遗传多样性使得DFTD的同种异体移植得以传播,但最近的证据表明,遗传多样性的动物会死于该病。缺乏针对DFTD肿瘤细胞的免疫应答可能是由于缺乏肿瘤细胞的免疫原性。这可以促进魔鬼之间的传递。为了测试免疫原性,给小鼠注射活的DFTD细胞并分析抗DFTD免疫应答。检测到针对DFTD细胞的一系列抗体同种型,表明DFTD细胞可以诱导免疫反应,因此具有免疫原性。当用DFTD细胞体外培养来自注射了DFTD细胞的小鼠的脾细胞并分析上清液时,这由细胞因子产生来支持。第一次注射DFTD细胞后,IFN-γ和TNF-α大量产生,第二次注射后IL-6和IL-10大量产生。在体外细胞毒性试验中,来自幼稚或免疫小鼠的脾细胞杀死了DFTD细胞。因此,它们也是免疫破坏的靶标。我们得出结论,由于可以针对DFTD细胞产生免疫应答,因此它们将成为疫苗的合适靶标。

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