| Literature DB >> 30042492 |
Lidia Avalle1, Annalisa Camporeale1, Giampaolo Morciano2,3,4, Natascia Caroccia2, Elena Ghetti1, Valeria Orecchia1, Daniele Viavattene1, Carlotta Giorgi2, Paolo Pinton5,6, Valeria Poli7.
Abstract
STAT3 is an oncogenic transcription factor exerting its functions both as a canonical transcriptional activator and as a non-canonical regulator of energy metabolism and mitochondrial functions. While both activities are required for cell transformation downstream of different oncogenic stimuli, they rely on different post-translational activating events, namely phosphorylation on either Y705 (nuclear activities) or S727 (mitochondrial functions). Here, we report the discovery of the unexpected STAT3 localization to the endoplasmic reticulum (ER), from where it modulates ER-mitochondria Ca2+ release by interacting with the Ca2+ channel IP3R3 and facilitating its degradation. The release of Ca2+ is of paramount importance for life/death cell decisions, as excessive Ca2+ causes mitochondrial Ca2+ overload, the opening of the mitochondrial permeability transition pore, and the initiation of the intrinsic apoptotic program. Indeed, STAT3 silencing enhances ER Ca2+ release and sensitivity to apoptosis following oxidative stress in STAT3-dependent mammary tumor cells, correlating with increased IP3R3 levels. Accordingly, basal-like mammary tumors, which frequently display constitutively active STAT3, show an inverse correlation between IP3R3 and STAT3 protein levels. These results suggest that STAT3-mediated IP3R3 downregulation in the ER crucially contributes to its anti-apoptotic functions via modulation of Ca2+ fluxes.Entities:
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Year: 2018 PMID: 30042492 PMCID: PMC6214529 DOI: 10.1038/s41418-018-0171-y
Source DB: PubMed Journal: Cell Death Differ ISSN: 1350-9047 Impact factor: 15.828