胰岛素样生长因子1受体
下调和上调
癌症研究
肺癌
癌症
肿瘤坏死因子α
医学
生物
免疫学
受体
病理
内科学
生长因子
生物化学
基因
作者
Gu‐Choul Shin,Hyeong Min Lee,Nayeon Kim,Sang‐Uk Seo,Kwang Pyo Kim,Kyun‐Hwan Kim
标识
DOI:10.1038/s12276-023-01147-1
摘要
Abstract Tumor necrosis factor superfamily (TNFSF) resistance contributes to the development and progression of tumors and resistance to various cancer therapies. Tumor-intrinsic alterations involved in the adaptation to the TNFSF response remain largely unknown. Here, we demonstrate that protein kinase C substrate 80K-H (PRKCSH) abundance in lung cancers boosts oncogenic IGF1R activation, leading to TNFSF resistance. PRKCSH abundance is correlated with IGF1R upregulation in lung cancer tissues. Specifically, PRKCSH interacts with IGF1R and extends its half-life. The PRKCSH-IGF1R axis in tumor cells impairs caspase-8 activation, increases Mcl-1 expression, and inhibits caspase-9, leading to an imbalance between cell death and survival. PRKCSH deficiency augmented the antitumor effects of natural killer (NK) cells, representative TNFSF effector cells, in a tumor xenograft IL-2Rg-deficient NOD/SCID (NIG) mouse model. Our data suggest that PRKCSH plays a critical role in TNFSF resistance and may be a potential target to improve the efficacy of NK cell-based cancer therapy.
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