CD86
癌症研究
基因敲除
免疫系统
医学
黑色素瘤
转染
免疫学
生物
T细胞
细胞培养
遗传学
作者
Shimei Yuan,Huan Li,Min Yang,He Zha,Hui Sun,Xue-ru Li,Aifang Li,Yue Gu,Liang Duan,Jinyong Luo,Chongyan Li,Yan Wang,Zhibiao Wang,Tong‐Chuan He,Lan Zhou
出处
期刊:Oncotarget
[Impact Journals LLC]
日期:2015-10-16
卷期号:6 (35): 37626-37637
被引量:38
标识
DOI:10.18632/oncotarget.5285
摘要
HIFU has been demonstrated to enhance anti-tumor immunity, however, the mechanism of which has not been well elucidated. Emerging evidence indicates that miRNAs play important roles in immune response. In this study, we used the B16F10 melanoma allograft mouse model to investigate the role of miRNAs in HIFU-enhanced anti-tumor immunity. We found that HIFU treatment decreased circulating B16F10 cells and pulmonary metastasis nodules while increased IFN-γ and TNF-α in the peripheral blood and cumulative mouse survival, which was associated with inhibition of miR-134 expression and activation of CD86 expression in tumor tissues. Further, we determined that miR-134 directly binds to the 3'UTR of CD86 mRNA to suppress its expression in B16F10 cells. When B16F10 cells transfected with miR-134 were co-cultured with normal splenic lymphocytes, the secretion of IFN-γ and TNF-α from lymphocytes was reduced and B16F10 cell survival was increased. HIFU exposure efficiently decreased miR-134 while increased CD86 expression in B16F10 cells in vitro. CD86 knockdown with siRNA markedly rescued the viability of HIFU-treated B16F10 cells that co-cultured with lymphocytes. Altogether, our results suggest that HIFU down-regulates miR-134 to release the inhibition of miR-134 on CD86 in melanoma cells, thereby enhancing anti-tumor immune response.
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