From the Department of Medical Life Systems, Faculty of Life and Medical Sciences, Doshisha University, Kyoto 610-0394, Japan.
From the Department of Medical Life Systems, Faculty of Life and Medical Sciences, Doshisha University, Kyoto 610-0394, Japan.
Steroids. 2023 Jan;189:109136. doi: 10.1016/j.steroids.2022.109136. Epub 2022 Nov 11.
The brain-specific cholesterol metabolite 24(S)-hydroxycholesterol (24S-OHC) has been shown to cause neuronal cell death when subjected to esterification by acyl-CoA:cholesterol acyltransferase 1 (ACAT1). Accumulating 24S-OHC esters in the endoplasmic reticulum (ER) provoked ER membrane disruption and an integrated stress response (ISR), a signaling pathway that regulates adaptation to various stresses. We have previously reported that α-tocopherol (α-Toc) but not α-tocotrienol (α-Toc3), among vitamin E homologs, suppressed 24S-OHC-induced cell death without affecting ACAT1 activity in human neuroblastoma SH-SY5Y cells. However, the precise mechanisms underlying the inhibitory activity of α-Toc have yet to be elucidated. In the present study, we aimed to investigate the effects of α-Toc on the 24S-OHC-induced cell death machinery. We showed that α-Toc, but not α Toc3, suppressed 24S-OHC-induced ISR and downstream eukaryotic translation initiator factor 2α (eIF2α) phosphorylation. We also found that α-Toc inhibited stress granule formation and robust downregulation of nascent protein synthesis, which were induced by 24S-OHC treatment. Furthermore, disruption of ER membrane integrity was suppressed by α-Toc, but not by α-Toc3. Our findings suggest that the inhibitory effects of α-Toc on 24S-OHC-induced cell death may be attributed to its protective function against ER membrane disruption.
脑特异性胆固醇代谢产物 24(S)-羟基胆固醇(24S-OHC)在受到酰基辅酶 A:胆固醇酰基转移酶 1(ACAT1)酯化后,会导致神经元细胞死亡。内质网(ER)中 24S-OHC 酯的积累会引发 ER 膜破裂和综合应激反应(ISR),这是一种调节对各种应激适应的信号通路。我们之前曾报道,维生素 E 同系物中,α-生育酚(α-Toc)而不是α-生育三烯酚(α-Toc3)能够抑制 24S-OHC 诱导的细胞死亡,而不影响人神经母细胞瘤 SH-SY5Y 细胞中的 ACAT1 活性。然而,α-Toc 抑制活性的确切机制尚未阐明。在本研究中,我们旨在研究α-Toc 对 24S-OHC 诱导的细胞死亡机制的影响。我们表明,α-Toc 而非α-Toc3 抑制了 24S-OHC 诱导的 ISR 和下游真核起始因子 2α(eIF2α)磷酸化。我们还发现,α-Toc 抑制了 24S-OHC 处理诱导的应激颗粒形成和新生蛋白质合成的强烈下调。此外,α-Toc 抑制了 ER 膜完整性的破坏,但α-Toc3 没有。我们的研究结果表明,α-Toc 对 24S-OHC 诱导的细胞死亡的抑制作用可能归因于其对 ER 膜破裂的保护作用。