Downregulation of cytoplasmic DNases is implicated in cytoplasmic DNA accumulation and SASP in senescent cells.
Akiko TakahashiTze Mun LooRyo OkadaFumitaka KamachiYoshihiro WatanabeMasahiro WakitaSugiko WatanabeShimpei KawamotoKenichi MiyataGlen N BarberNaoko OhtaniEiji HaraPublished in: Nature communications (2018)
Accumulating evidence indicates that the senescence-associated secretory phenotype (SASP) contributes to many aspects of physiology and disease. Thus, controlling the SASP will have tremendous impacts on our health. However, our understanding of SASP regulation is far from complete. Here, we show that cytoplasmic accumulation of nuclear DNA plays key roles in the onset of SASP. Although both DNase2 and TREX1 rapidly remove the cytoplasmic DNA fragments emanating from the nucleus in pre-senescent cells, the expression of these DNases is downregulated in senescent cells, resulting in the cytoplasmic accumulation of nuclear DNA. This causes the aberrant activation of cGAS-STING cytoplasmic DNA sensors, provoking SASP through induction of interferon-β. Notably, the blockage of this pathway prevents SASP in senescent hepatic stellate cells, accompanied by a decline of obesity-associated hepatocellular carcinoma development in mice. These findings provide valuable new insights into the roles and mechanisms of SASP and possibilities for their control.
Keyphrases
- induced apoptosis
- circulating tumor
- cell cycle arrest
- cell free
- single molecule
- type diabetes
- healthcare
- signaling pathway
- cell death
- public health
- metabolic syndrome
- oxidative stress
- dna damage
- cell proliferation
- long non coding rna
- endothelial cells
- dendritic cells
- high fat diet induced
- body mass index
- pi k akt
- stress induced
- health promotion