Spleen-Derived CCL9 Recruits MDSC to Facilitate Tumor Growth in Orthotopic Hepatoma Mice.

IF 1.2 Q4 GENETICS & HEREDITY Global Medical Genetics Pub Date : 2023-12-01 DOI:10.1055/s-0043-1777327
Baohua Li, Wenjuan Li, Yingxue Liang, Chen Zhang, Guangyao Kong, Zongfang Li
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Abstract

Objectives  Spleen is involved in multiple diseases, the role of the spleen and spleen-derived factors in hepatocellular carcinoma (HCC) is still not clarified. Methods  In the current study, a murine H22 orthotopic hepatoma model was established. Three groups were divided: normal mice, tumor-bearing mice with spleen-preserving, and tumor-bearing mice with splenectomy. Spleen and tumor weights were recorded by weeks 1 and 2. The proportion of myeloid-derived suppressor cell (MDSC) in peripheral blood and tumor tissue was detected using flow cytometry. Protein chip assay was used to compare the differential cytokines between normal liver supernatant and tumor supernatant. The common upregulated cytokines both in spleen and tumor were focused and analyzed using gene expression profiling interactive analysis (GEPIA) database. Enzyme-linked immunosorbent assay was performed to verify the chip result, and to examine CCL9 expression before and after splenectomy. Spleen MDSC was sorted using flow cytometry, and chemotaxis assay was performed to demonstrate whether CCL9 attracted spleen MDSC. Results  The spleen enlarged during tumor progression, and compared with splenectomy group, there were faster tumor growth, shorter survival time, and higher proportions of MDSC in spleen-preserving group. Protein chip assay and GEPIA database revealed CCL9 was the most promising chemokine involved in HCC upregulated both in spleen and tumor tissue. CCL9 attracted MDSC in vitro, the level of CCL9 in tumor tissue was downregulated, and the percentage of MDSC was decreased after splenectomy. Conclusion  The results demonstrate that CCL9 may be derived from spleen; it facilitated HCC growth via the chemotaxis of MDSC, targeting CCL9 may be a promising strategy in HCC treatment.

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脾源CCL9募集MDSC促进原位肝癌小鼠肿瘤生长
目的脾参与多种疾病,脾及脾源性因子在肝细胞癌(HCC)中的作用尚不清楚。方法建立小鼠H22原位肝癌模型。将正常小鼠、保脾荷瘤小鼠和脾切除荷瘤小鼠分为三组。于第1周和第2周记录脾脏和肿瘤重量。采用流式细胞术检测外周血和肿瘤组织中髓源性抑制细胞(MDSC)的比例。用蛋白芯片法比较正常肝脏上清与肿瘤上清细胞因子的差异。利用基因表达谱交互分析(GEPIA)数据库对脾脏和肿瘤中常见的上调细胞因子进行了集中分析。采用酶联免疫吸附法验证芯片结果,并检测脾切除术前后CCL9的表达。采用流式细胞术对脾脏MDSC进行分选,并进行趋化性实验验证CCL9是否吸引脾脏MDSC。结果肿瘤进展过程中脾脏肿大,与脾切除组相比,保脾组肿瘤生长更快,生存时间更短,MDSC比例更高。蛋白芯片分析和GEPIA数据库显示CCL9是最有希望参与HCC的趋化因子,在脾脏和肿瘤组织中均上调。体外CCL9诱导MDSC,肿瘤组织中CCL9水平下调,脾切除术后MDSC百分比降低。结论CCL9可能来源于脾脏;它通过MDSC的趋化性促进HCC的生长,靶向CCL9可能是HCC治疗的一种有前途的策略。
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来源期刊
Global Medical Genetics
Global Medical Genetics GENETICS & HEREDITY-
自引率
11.80%
发文量
30
审稿时长
14 weeks
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