Pagliassotti Michael J, Estrada Andrea L, Hudson William M, Wei Yuren, Wang Dong, Seals Douglas R, Zigler Melanie L, LaRocca Thomas J
Department of Food Science and Human Nutrition, Colorado State University, Fort Collins, CO 80523-1571, USA.
Department of Food Science and Human Nutrition, Colorado State University, Fort Collins, CO 80523-1571, USA.
J Nutr Biochem. 2017 Jul;45:15-23. doi: 10.1016/j.jnutbio.2017.02.022. Epub 2017 Apr 6.
The accumulation of damaged proteins can perturb cellular homeostasis and provoke aging and cellular damage. Quality control systems, such as the unfolded protein response (UPR), inflammatory signaling and protein degradation, mitigate the residence time of damaged proteins. In the present study, we have examined the UPR and inflammatory signaling in the liver of young (6 months) and old (28 months) mice (n=8/group), and the ability of trehalose, a compound linked to increased protein stability and autophagy, to counteract age-induced effects on these systems. When used, trehalose was provided for 4 weeks in the drinking water immediately prior to sacrifice (n=7/group). Livers from old mice were characterized by activation of the UPR, increased inflammatory signaling and indices of liver injury. Trehalose treatment reduced the activation of the UPR and inflammatory signaling, and reduced liver injury. Reductions in proteins involved in autophagy and proteasome activity observed in old mice were restored following trehalose treatment. The autophagy marker, LC3B-II, was increased in old mice treated with trehalose. Metabolomics analyses demonstrated that reductions in hexosamine biosynthetic pathway metabolites and nicotinamide in old mice were restored following trehalose treatment. Trehalose appears to be an effective intervention to reduce age-associated liver injury and mitigate the need for activation of quality control systems that respond to disruption of proteostasis.
受损蛋白质的积累会扰乱细胞内稳态,引发衰老和细胞损伤。质量控制系统,如未折叠蛋白反应(UPR)、炎症信号传导和蛋白质降解,会缩短受损蛋白质的驻留时间。在本研究中,我们检测了年轻(约6个月)和年老(约28个月)小鼠(每组n = 8)肝脏中的UPR和炎症信号传导,以及海藻糖(一种与提高蛋白质稳定性和自噬相关的化合物)抵消年龄对这些系统影响的能力。使用海藻糖时,在处死前4周通过饮用水提供(每组n = 7)。老年小鼠的肝脏表现为UPR激活、炎症信号传导增加和肝损伤指标升高。海藻糖处理降低了UPR和炎症信号传导的激活,并减轻了肝损伤。海藻糖处理后,老年小鼠中观察到的参与自噬和蛋白酶体活性的蛋白质减少得到恢复。用海藻糖处理的老年小鼠中自噬标志物LC3B-II增加。代谢组学分析表明,海藻糖处理后,老年小鼠中己糖胺生物合成途径代谢物和烟酰胺的减少得到恢复。海藻糖似乎是一种有效的干预措施,可减少与年龄相关的肝损伤,并减轻对响应蛋白质稳态破坏的质量控制系统激活的需求。