Valproate protects cells from ER stress-induced lipid accumulation and apoptosis by inhibiting glycogen synthase kinase-3

doi:10.1242/jcs.01562

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JCS ePress online publication date 7 Dec 2004
doi: 10.1242/jcs.01562

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Research Article

Valproate protects cells from ER stress-induced lipid accumulation and apoptosis by inhibiting glycogen synthase kinase-3

Anna J. Kim, Yuanyuan Shi, Richard C. Austin, and Geoff H. Werstuck^*
^* Author for correspondence (e-mail: gwerstuck{at}thrombosis.hhscr.org)

A wide range of agents and conditions are known to disruptthe ability of the endoplasmic reticulum (ER) to fold proteinsproperly, resulting in the onset of ER dysfunction/stress. Weand others have shown that ER stress can induce intracellularlipid accumulation through the activation of the sterol responsiveelement binding proteins (SREBPs) and initiate programmed celldeath by activation of caspases. It has been suggested thatER stress-induced lipid accumulation and cell death play a rolein the pathogenesis of disorders including Alzheimer's disease,Parkinson's disease, type-1 diabetes mellitus and hepatic steatosis.Here we show that exposure of HepG2 cells to the branch chainfatty acid, valproate, increases cellular resistance to ER stress-induceddysfunction. Two distinctly different potential mechanisms forthis protective effect were investigated. We show that exposureto valproate increases the expression of chaperones that assistin the folding of proteins in the ER including GRP78/BiP, GRP94,PDI and calreticulin as well as the cytosolic chaperone, HSP70.However, exposure of HepG2 cells to valproate does not decreasethe apparent ER stress response in cells challenged with tunicamycin,A23187 or glucosamine, suggesting that valproate-conferred protectionoccurs downstream of ER dysfunction. Finally, we demonstratethat valproate directly inhibits the glycogen synthase kinases(GSK)-3 ${alpha}$ / ${beta}$ . The ability of lithium, another inhibitor of GSK3 ${alpha}$ / ${beta}$ to protect cells from ER stress-induced lipid accumulation suggeststhat GSK3 plays a central role in signaling downstream effectsof ER stress. Strategies to protect cells from agents/conditionsthat induce ER stress may have potential in the treatment ofthe growing number of diseases and disorders linked to ER dysfunction.

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