反映临床前模型中侵袭性的黑色素瘤肿瘤的免疫谱分析。
Immune profiling of melanoma tumors reflecting aggressiveness in a preclinical model.
作者信息
Fortis Sotirios P, Mahaira Louisa G, Anastasopoulou Eleftheria A, Voutsas Ioannis F, Perez Sonia A, Baxevanis Constantin N
机构信息
Cancer Immunology and Immunotherapy Center, "Saint Savas" Cancer Hospital, 171 Alexandras Avenue, 11522, Athens, Greece.
出版信息
Cancer Immunol Immunother. 2017 Dec;66(12):1631-1642. doi: 10.1007/s00262-017-2056-1. Epub 2017 Sep 4.
Abstract
Melanoma, like most solid tumors, is highly heterogeneous in terms of invasive, proliferative, and tumor-initiating potential. This heterogeneity is the outcome of differential gene expression resulting from conditions in the tumor microenvironment and the selective pressure of the immune system. To investigate possible signatures combining immune-related gene expression and lymphocyte infiltration, we established a preclinical model using B16.F1-derived clones, in the context of melanoma aggressiveness. Combinatorial analyses revealed that tumors concomitantly expressing low levels of Tnf-a, Pd-1, Il-10, Il-1ra, Ccl5, Ido, high Il-9, and with low infiltration by CD45, CD3, CD4 and CD8 cells and a high CD4:CD8 T cell ratio exhibited the most aggressive growth characteristics. Overall, these results support the notion that the intratumoral immunologic network molds aggressive melanoma phenotypes.
摘要
与大多数实体瘤一样,黑色素瘤在侵袭、增殖和肿瘤起始潜能方面具有高度异质性。这种异质性是肿瘤微环境条件和免疫系统选择性压力导致的基因表达差异的结果。为了研究结合免疫相关基因表达和淋巴细胞浸润的可能特征,我们在黑色素瘤侵袭性背景下,使用B16.F1衍生克隆建立了一个临床前模型。组合分析显示,同时表达低水平的Tnf-a、Pd-1、Il-10、Il-1ra、Ccl5、Ido,高水平的Il-9,且CD45、CD3、CD4和CD8细胞浸润低、CD4:CD8 T细胞比率高的肿瘤表现出最具侵袭性的生长特征。总体而言,这些结果支持肿瘤内免疫网络塑造侵袭性黑色素瘤表型这一观点。
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