De la Fuente López Marjorie, Landskron Glauben, Parada Daniela, Dubois-Camacho Karen, Simian Daniela, Martinez Maripaz, Romero Diego, Roa Juan Carlos, Chahuán Isidora, Gutiérrez Rocío, Lopez-K Francisco, Alvarez Karin, Kronberg Udo, López Sebastian, Sanguinetti Antonella, Moreno Natalia, Abedrapo Mario, González María-Julieta, Quera Rodrigo, Hermoso-R Marcela A
1 Academic Research Unit, Clínica Las Condes, Santiago, Chile.
2 Innate Immunity Laboratory, Disciplinary Program of Immunology, Institute of Biomedical Sciences, Faculty of Medicine, Universidad de Chile, Santiago, Chile.
Tumour Biol. 2018 Nov;40(11):1010428318810059. doi: 10.1177/1010428318810059.
A complex network of chemokines can influence cancer progression with the recruitment and activation of hematopoietic cells, including macrophages to the supporting tumor stroma promoting carcinogenesis and metastasis. The aim of this study was to investigate the relation between tissue and plasma chemokine levels involved in macrophage recruitment with tumor-associated macrophage profile markers and clinicopathological features such as tumor-node-metastases stage, desmoplasia, tumor necrosis factor-α, and vascular endothelial growth factor plasma content. Plasma and tumor/healthy mucosa were obtained from Chilean patients undergoing colon cancer surgery. Chemokines were evaluated from tissue lysates (CCL2, CCL3, CCL4, CCL5, and CX3CL1) by Luminex. Statistical analysis was performed using Wilcoxon match-paired test ( p < 0.05). Macrophage markers (CD68, CD163, and iNOS) were evaluated by immunohistochemistry samples derived from colorectal cancer patients. Correlation analysis between chemokines and macrophage markers and clinicopathological features were performed using Spearman's test. Plasmatic levels of chemokines and inflammatory mediators' vascular endothelial growth factor and tumor necrosis factor-α were evaluated by Luminex. Tumor levels of CCL2 (mean ± standard deviation = 530.1 ± 613.9 pg/mg), CCL3 (102.7 ± 106.0 pg/mg), and CCL4 (64.98 ± 48.09 pg/mg) were higher than those found in healthy tissue (182.1 ± 116.5, 26.79 ± 22.40, and 27.06 ± 23.69 pg/mg, respectively p < 0.05). The tumor characterization allowed us to identify a positive correlation between CCL4 and the pro-tumor macrophages marker CD163 ( p = 0.0443), and a negative correlation of iNOS with desmoplastic reaction ( p = 0.0467). Moreover, we identified that tumors with immature desmoplasia have a higher CD163 density compared to those with a mature/intermediated stromal tissue ( p = 0.0288). Plasmatic CCL4 has shown a positive correlation with inflammatory mediators (tumor necrosis factor-α and vascular endothelial growth factor) that have previously been associated with poor prognosis in patients. In conclusion High expression of CCL4 in colon cancer could induce the infiltration of tumor-associated macrophages and specifically a pro-tumor macrophage profile (CD163 cells). Moreover, plasmatic chemokines could be considered inflammatory mediators associated to CRC progression as well as tumor necrosis factor-α and vascular endothelial growth factor. These data reinforce the idea of chemokines as potential therapeutic targets or biomarker in CRC.
趋化因子的复杂网络可通过募集和激活造血细胞(包括巨噬细胞)至支持性肿瘤基质,从而影响癌症进展,促进致癌作用和转移。本研究的目的是调查参与巨噬细胞募集的组织和血浆趋化因子水平与肿瘤相关巨噬细胞谱标记物以及临床病理特征(如肿瘤-淋巴结-转移分期、促纤维增生、肿瘤坏死因子-α和血管内皮生长因子血浆含量)之间的关系。从接受结肠癌手术的智利患者获取血浆和肿瘤/健康黏膜。通过Luminex技术从组织裂解液(CCL2、CCL3、CCL4、CCL5和CX3CL1)中评估趋化因子。使用Wilcoxon配对检验进行统计分析(p < 0.05)。通过免疫组织化学对来自结直肠癌患者的样本评估巨噬细胞标记物(CD68、CD163和诱导型一氧化氮合酶)。使用Spearman检验进行趋化因子与巨噬细胞标记物及临床病理特征之间的相关性分析。通过Luminex技术评估趋化因子和炎症介质血管内皮生长因子及肿瘤坏死因子-α的血浆水平。肿瘤组织中CCL2(平均值±标准差 = 530.1±613.9 pg/mg)、CCL3(102.7±106.0 pg/mg)和CCL4(64.98±48.09 pg/mg)的水平高于健康组织(分别为182.1±116.5、26.79±22.40和27.06±23.69 pg/mg,p < 0.05)。肿瘤特征分析使我们能够确定CCL4与促肿瘤巨噬细胞标记物CD163之间呈正相关(p = 0.0443),诱导型一氧化氮合酶与促纤维增生反应呈负相关(p = 0.0467)。此外,我们发现与成熟/中间基质组织的肿瘤相比,具有未成熟促纤维增生的肿瘤具有更高的CD163密度(p = 0.0288)。血浆CCL4与先前与患者预后不良相关的炎症介质(肿瘤坏死因子-α和血管内皮生长因子)呈正相关。总之,结肠癌中CCL4的高表达可诱导肿瘤相关巨噬细胞浸润,特别是促肿瘤巨噬细胞谱(CD163细胞)。此外,血浆趋化因子可被视为与结直肠癌进展相关的炎症介质以及肿瘤坏死因子-α和血管内皮生长因子。这些数据强化了趋化因子作为结直肠癌潜在治疗靶点或生物标志物的观点。
