线粒体
先天免疫系统
炎症
细胞生物学
癌症研究
RNA沉默
生物
小RNA
胰腺导管腺癌
RNA干扰
胰腺癌
癌症
信号转导
核糖核酸
细胞凋亡
程序性细胞死亡
转录组
癌细胞
免疫
化学
细胞
基因沉默
小干扰RNA
下调和上调
基因表达
基因
肿瘤坏死因子α
细胞生长
癌变
腺癌
作者
Andrew T. Milcarek,Minjeong Yeon,Camilla Esposito,Prerna Kulkarni,Andrew V. Kossenkov,Jozef Madžo,Anneliese M. Faustino,Hsin-Yao Tang,Alessandra Maria Storaci,A. Palleschi,M Locatelli,Valentina Vaira,Mary Iacocca,Andrea Ward,Arvind Sabesan,Nicholas J. Petrelli,Michela Perego,Dario C. Altieri
标识
DOI:10.1073/pnas.2528281123
摘要
Mitochondria activate inflammation and innate immunity to protect against infections, but the role in cancer is unknown. Here, we report that patients with pancreatic ductal adenocarcinoma (PDAC) with reduced levels of the mitochondrial scaffold, Mic60, or inner mitochondrial membrane protein, exhibit increased inflammation, high NFκB activity and production of TNFα. This is mediated by double-stranded RNA (dsRNA) released from structurally defective, Mic60-low mitochondria, which engages TLR3/RIG-I sensing, activates NFκB gene expression and reprograms transcriptional and signaling networks to promote PDAC proliferation. Preclinical targeting of mitochondrial dsRNA signaling triggers rapid cell death and inhibition of tumor growth, selectively in Mic60-knockdown PDAC, without overt toxicity, in vivo. Therefore, dsRNA released from defective mitochondria generates protumorigenic inflammation and provides an actionable therapeutic target in selected PDAC patients.
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