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https://doi.org/10.1038/cdd.2017.152
Title: | Oxidative stress promotes SIRT1 recruitment to the GADD34/PP1α complex to activate its deacetylase function | Authors: | Lee, Irene Chengjie Ho, Xue Yan George, Simi Elizabeth Goh, Catherine Wenhui Sundaram, Jeyapriya Rajameenakshi Pang, Karen Ka Lam Luo, Weiwei Yusoff, Permeen Sze, Newman Siu Kwan Shenolikar, Shirish |
Keywords: | Science & Technology Life Sciences & Biomedicine Biochemistry & Molecular Biology Cell Biology UNFOLDED PROTEIN RESPONSE ENDOPLASMIC-RETICULUM CELL-SURVIVAL DNA-DAMAGE INSULIN-RESISTANCE GADD34 PROTEIN 26S PROTEASOME PHOSPHORYLATION EIF2-ALPHA ACETYLATION |
Issue Date: | Feb-2018 | Publisher: | NATURE PUBLISHING GROUP | Citation: | Lee, Irene Chengjie, Ho, Xue Yan, George, Simi Elizabeth, Goh, Catherine Wenhui, Sundaram, Jeyapriya Rajameenakshi, Pang, Karen Ka Lam, Luo, Weiwei, Yusoff, Permeen, Sze, Newman Siu Kwan, Shenolikar, Shirish (2018-02). Oxidative stress promotes SIRT1 recruitment to the GADD34/PP1α complex to activate its deacetylase function. CELL DEATH AND DIFFERENTIATION 25 (2) : 255-267. ScholarBank@NUS Repository. https://doi.org/10.1038/cdd.2017.152 | Abstract: | Phosphorylation of the eukaryotic translation initiation factor, eIF2α, by stress-activated protein kinases and dephosphorylation by the growth arrest and DNA damage-inducible protein (GADD34)-containing phosphatase is a central node in the integrated stress response. Mass spectrometry demonstrated GADD34 acetylation at multiple lysines. Substituting K315 and K322 with alanines or glutamines did not impair GADD34's ability to recruit protein phosphatase 1α (PP1α) or eIF2α, suggesting that GADD34 acetylation did not modulate eIF2α phosphatase activity. Arsenite (Ars)-induced oxidative stress increased cellular GADD34 levels and enhanced Sirtuin 1 (SIRT1) recruitment to assemble a cytoplasmic complex containing GADD34, PP1α, eIF2α and SIRT1. Induction of GADD34 in WT MEFs paralleled the dephosphorylation of eIF2α (phosphoserine-51) and SIRT1 (phosphoserine-47). By comparison, eIF2α and SIRT1 were persistently phosphorylated in Ars-treated GADD34-/-MEFs. Expressing WT GADD34, but not a mutant unable to bind PP1α in GADD34-/-MEFs restored both eIF2α and SIRT1 dephosphorylation. SIRT1 dephosphorylation increased its deacetylase activity, measured in vitro and in cells. Loss of function of GADD34 or SIRT1 enhanced cellular p-eIF2α levels and attenuated cell death following Ars exposure. These results highlighted a novel role for the GADD34/PP1α complex in coordinating the dephosphorylation and reactivation of eIF2α and SIRT1 to determine cell fate following oxidative stress. | Source Title: | CELL DEATH AND DIFFERENTIATION | URI: | https://scholarbank.nus.edu.sg/handle/10635/248894 | ISSN: | 1350-9047 1476-5403 |
DOI: | 10.1038/cdd.2017.152 |
Appears in Collections: | Staff Publications Elements |
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