| Literature DB >> 30527665 |
Xin Jin1, Donglin Ding2, Yuqian Yan2, Hui Li2, Bo Wang1, Linlin Ma3, Zhenqing Ye4, Tao Ma2, Qiang Wu5, Daniel N Rodrigues6, Manish Kohli7, Rafael Jimenez8, Liguo Wang4, David W Goodrich9, Johann de Bono6, Haidong Dong10, Heshui Wu11, Runzhi Zhu12, Haojie Huang13.
Abstract
Aberrant expression of programmed death ligand-1 (PD-L1) in tumor cells promotes cancer progression by suppressing cancer immunity. The retinoblastoma protein RB is a tumor suppressor known to regulate the cell cycle, DNA damage response, and differentiation. Here, we demonstrate that RB interacts with nuclear factor κB (NF-κB) protein p65 and that their interaction is primarily dependent on CDK4/6-mediated serine-249/threonine-252 (S249/T252) phosphorylation of RB. RNA-seq analysis shows a subset of NF-κB pathway genes including PD-L1 are selectively upregulated by RB knockdown or CDK4/6 inhibitor. S249/T252-phosphorylated RB inversely correlates with PD-L1 expression in patient samples. Expression of a RB-derived S249/T252 phosphorylation-mimetic peptide suppresses radiotherapy-induced upregulation of PD-L1 and augments therapeutic efficacy of radiation in vivo. Our findings reveal a previously unrecognized tumor suppressor function of hyperphosphorylated RB in suppressing NF-κB activity and PD-L1 expression and suggest that the RB-NF-κB axis can be exploited to overcome cancer immune evasion triggered by conventional or targeted therapies.Entities:
Keywords: CDK4/6 inhibitor; CHD1; MAP3K7; NF-κB; PD-L1; RB; immunotherapy; phosphorylation; prostate cancer; radiotherapy
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Year: 2018 PMID: 30527665 PMCID: PMC8968458 DOI: 10.1016/j.molcel.2018.10.034
Source DB: PubMed Journal: Mol Cell ISSN: 1097-2765 Impact factor: 17.970