ULK1
自噬
调节器
激酶
细胞生物学
自噬体
化学
生物
癌症研究
生物化学
蛋白激酶A
安普克
基因
细胞凋亡
作者
Tiffany Tsang,Jessica M. Posimo,A. Andrea Gudiel,Michelle Cicchini,David M. Feldser,Donita C. Brady
标识
DOI:10.1038/s41556-020-0481-4
摘要
Although the transition metal copper (Cu) is an essential nutrient that is conventionally viewed as a static cofactor within enzyme active sites, a non-traditional role for Cu as a modulator of kinase signalling is emerging. Here, we found that Cu is required for the activity of the autophagic kinases ULK1 and ULK2 (ULK1/2) through a direct Cu–ULK1/2 interaction. Genetic loss of the Cu transporter Ctr1 or mutations in ULK1 that disrupt the binding of Cu reduced ULK1/2-dependent signalling and the formation of autophagosome complexes. Increased levels of intracellular Cu are associated with starvation-induced autophagy and are sufficient to enhance ULK1 kinase activity and, in turn, autophagic flux. The growth and survival of lung tumours driven by KRASG12D is diminished in the absence of Ctr1, is dependent on ULK1 Cu binding and is associated with reduced levels of autophagy and signalling. These findings suggest a molecular basis for exploiting Cu-chelation therapy to prevent autophagy signalling to limit proliferation and improve patient survival in cancer. Tsang et al. show that copper modulates the activity of autophagic kinases ULK1/2 to control autophagy, and is required for KRASG12D-driven tumour growth and cancer survival in response to starvation.
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