Showing papers on "Protein kinase complex published in 2013"
TL;DR: The Atg1/ULK1 complex plays a central role in starvation-induced autophagy, integrating signals from upstream sensors such as MTOR and AMPK and transducing them to the downstreamautophagy pathway, and examples of potential ULK1-independent autophapy have emerged, indicating that under certain specific contexts, the ULK 1 complex might be dispensable for autophagic activation.
Abstract: The Atg1/ULK1 complex plays a central role in starvation-induced autophagy, integrating signals from upstream sensors such as MTOR and AMPK and transducing them to the downstream autophagy pathway. Much progress has been made in the last few years in understanding the mechanisms by which the complex is regulated through protein-protein interactions and post-translational modifications, providing insights into how the cell modulates autophagy, particularly in response to nutrient status. However, how the ULK1 complex transduces upstream signals to the downstream central autophagy pathway is still unclear. Although the protein kinase activity of ULK1 is required for its autophagic function, its protein substrate(s) responsible for autophagy activation has not been identified. Furthermore, examples of potential ULK1-independent autophagy have emerged, indicating that under certain specific contexts, the ULK1 complex might be dispensable for autophagy activation. This raises the question of how the autophagic machinery is activated independent of the ULK1 complex and what are the biological functions of such noncanonical autophagy pathways.
411 citations
TL;DR: Novel insights are shed on the mechanism of hypoxia‐induced activation of the ATR pathway by reporting that ATRIP is a direct target of HIF‐1 and silencing the expression of ATRIP by RNA interference abolished Hypoxia induced ATR activation and CHK1 phosphorylation in cancer cells.
12 citations