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肿瘤微环境是否会改变犬传染性性病肿瘤的肿瘤发生及临床反应?

Does the tumour microenvironment alter tumorigenesis and clinical response in transmissible venereal tumour in dogs?

作者信息

Ballestero Fêo H, Montoya Flórez L, Yamatogi R S, Prado Duzanski A, Araújo J P, Oliveira R A, Rocha N S

机构信息

Department of Veterinary Clinics, Faculty of Veterinary Medicine, UNESP, Botucatu, Brazil.

Veterinary Pathology Research Group, Faculty of Agricultural Sciences, Universidad de Caldas, Manizales, Colombia.

出版信息

Vet Comp Oncol. 2018 Sep;16(3):370-378. doi: 10.1111/vco.12388. Epub 2018 Mar 5.

Abstract

The canine transmissible venereal tumour (CTVT) is a transmissible cancer that is spread naturally between dogs, with the ability to develop and evade the immune system, despite strict immune surveillance of the host. Furthermore, molecular signalling between cells of the immune system and the tumour microenvironment appear to influence the behaviour and development of the tumour. Thus, this study aimed to quantify the expression of genes related to the immune system such as IL-6, IFN-γ, and TGF-β, as well as angiogenic factors (VEGF, CXCR4), in CTVT cells in vivo and in vitro (primary culture), correlating with the clinical response of the animals treated with vincristine. As expected, the most prevalent subtype was plasmacytoid cells, although lymphocytic cells were also found, indicating the possibility of polyclonality. When we compared the gene expressions of IFN-γ and IL-6, we mostly found low expression, concluding that MHC expression was probably not occurring in tumour cells, and no activation of immune cells to eliminate the tumour. The TGF-β gene was normal in the majority of animals but demonstrated decreased expression in vincristine resistant animals, leading to the hypothesis that the concentration of tumour-derived TGF-β was affecting and even suppressing the real TGF-β expression, favouring tumour proliferation and progression in these cases. VEGF expression was extremely high, demonstrating its angiogenic role in tumour growth, while CXCR4 was decreased, possibly because of CTVT's low metastatic potential. Thus, we concluded that the tumour microenvironment, together with the immune system of the host, influences CTVT, presumably altering its tumorigenesis and the animal's clinical response to treatment.

摘要

犬传染性性病肿瘤(CTVT)是一种可在犬之间自然传播的传染性癌症,尽管宿主有严格的免疫监视,但它仍有能力发展并逃避免疫系统。此外,免疫系统细胞与肿瘤微环境之间的分子信号似乎会影响肿瘤的行为和发展。因此,本研究旨在量化体内和体外(原代培养)CTVT细胞中与免疫系统相关的基因(如IL-6、IFN-γ和TGF-β)以及血管生成因子(VEGF、CXCR4)的表达,并将其与长春新碱治疗动物的临床反应相关联。正如预期的那样,最常见的亚型是浆细胞样细胞,不过也发现了淋巴细胞,这表明存在多克隆性的可能性。当我们比较IFN-γ和IL-6的基因表达时,大多发现表达水平较低,由此推断肿瘤细胞中可能未发生MHC表达,免疫细胞也未被激活以消除肿瘤。大多数动物的TGF-β基因正常,但在长春新碱耐药的动物中其表达降低,这导致一种假设,即肿瘤来源的TGF-β浓度正在影响甚至抑制真正的TGF-β表达,在这些情况下有利于肿瘤的增殖和进展。VEGF表达极高,表明其在肿瘤生长中的血管生成作用,而CXCR4表达降低,可能是因为CTVT的转移潜能较低。因此,我们得出结论,肿瘤微环境与宿主的免疫系统共同影响CTVT,大概会改变其肿瘤发生过程以及动物对治疗的临床反应。

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