| Literature DB >> 29786073 |
Seung Hee Jung1,2, Minyoung Lee3, Hyun A Park1,2, Hyung Chul Lee1,2, Donghee Kang1,2, Hyun Jung Hwang1,2, Chanho Park2, Dong-Min Yu4, Yu Ri Jung3, Mi-Na Hong3, Yong-Nyun Kim5, Heon Joo Park2,6, Young-Gyu Ko4, Jae-Seon Lee7,8.
Abstract
Cellular senescence refers to an irreversible growth arrest that is triggered by various intrinsic and extrinsic stresses. Many recent studies have demonstrated that cellular senescence plays a crucial role in the regression of tumors exposed to ionizing radiation (IR), but the underlying mechanism remains unknown. Here we show that the activation of integrin β4 is essential for IR-induced cellular senescence. IR treatment results in the phosphorylation of integrin β4 at tyrosine residue 1510, leading to activation of the integrin α6β4-Src-AKT signaling pathway. We further reveal that the IR-induced phosphorylation of integrin β4 is regulated by the cholesterol content and membrane fluidity. We also find that IR-induced p53-caspase signaling is independent of integrin α6β4-Src-AKT signaling. Finally, we show that siRNA- or inhibitor-mediated blockade of integrin α6β4-Src-AKT signaling switches the post-irradiation fate from senescence to apoptosis, under p53 activated condition, in both cancer cells and tumor tissues of xenograft mice. On the basis of our finding that, integrin α6β4 is specifically activated and acts primarily to induce premature senescence in irradiated cancer cells, we propose that this integrin may be a valuable target and biomarker for radiotherapy.Entities:
Mesh:
Substances:
Year: 2018 PMID: 29786073 PMCID: PMC6329762 DOI: 10.1038/s41418-018-0114-7
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 15.828