Hernandez Abbi R, Hernandez Caesar M, Campos Keila, Truckenbrod Leah, Federico Quinten, Moon Brianna, McQuail Joseph A, Maurer Andrew P, Bizon Jennifer L, Burke Sara N
Department of Neuroscience, McKnight Brain Institute, University of Florida, Gainesville, FL, United States.
Institute on Aging, University of Florida, Gainesville, FL, United States.
Front Aging Neurosci. 2018 Dec 3;10:391. doi: 10.3389/fnagi.2018.00391. eCollection 2018.
Age-related cognitive decline has been linked to a diverse set of neurobiological mechanisms, including bidirectional changes in proteins critical for neuron function. Importantly, these alterations are not uniform across the brain. For example, the hippocampus (HPC) and prefrontal cortex (PFC) show distinct patterns of dysfunction in advanced age. Because higher cognitive functions require large-scale interactions across prefrontal cortical and hippocampal networks, selectively targeting an alteration within one region may not broadly restore function to improve cognition. One mechanism for decline that the PFC and HPC share, however, is a reduced ability to utilize glucose for energy metabolism. Although this suggests that therapeutic strategies bypassing the need for neuronal glycolysis may be beneficial for treating cognitive aging, this approach has not been empirically tested. Thus, the current study used a ketogenic diet (KD) as a global metabolic strategy for improving brain function in young and aged rats. After 12 weeks, rats were trained to perform a spatial alternation task through an asymmetrical maze, in which one arm was closed and the other was open. Both young and aged KD-fed rats showed resilience against the anxiogenic open arm, training to alternation criterion performance faster than control animals. Following alternation testing, rats were trained to perform a cognitive dual task that required working memory while simultaneously performing a bi-conditional association task (WM/BAT), which requires PFC-HPC interactions. All KD-fed rats also demonstrated improved performance on WM/BAT. At the completion of behavioral testing, tissue punches were collected from the PFC for biochemical analysis. KD-fed rats had biochemical alterations within PFC that were dissociable from previous results in the HPC. Specifically, MCT1 and MCT4, which transport ketone bodies, were significantly increased in KD-fed rats compared to controls. GLUT1, which transports glucose across the blood brain barrier, was decreased in KD-fed rats. Contrary to previous observations within the HPC, the vesicular glutamate transporter (VGLUT1) did not change with age or diet within the PFC. The vesicular GABA transporter (VGAT), however, was increased within PFC similar to HPC. These data suggest that KDs could be optimal for enhancing large-scale network function that is critical for higher cognition.
与年龄相关的认知衰退与多种神经生物学机制有关,包括对神经元功能至关重要的蛋白质的双向变化。重要的是,这些改变在大脑中并不一致。例如,海马体(HPC)和前额叶皮层(PFC)在老年时表现出不同的功能障碍模式。由于更高的认知功能需要前额叶皮层和海马体网络之间的大规模相互作用,选择性地针对一个区域内的改变可能无法广泛恢复功能以改善认知。然而,PFC和HPC共有的一种衰退机制是利用葡萄糖进行能量代谢的能力下降。虽然这表明绕过神经元糖酵解需求的治疗策略可能对治疗认知衰老有益,但这种方法尚未经过实证检验。因此,当前的研究使用生酮饮食(KD)作为一种整体代谢策略来改善年轻和老年大鼠的脑功能。12周后,训练大鼠通过不对称迷宫执行空间交替任务,其中一个臂是封闭的,另一个是开放的。年轻和老年KD喂养的大鼠对引起焦虑的开放臂都表现出恢复力,训练到交替标准表现的速度比对照动物快。交替测试后,训练大鼠执行一项认知双重任务,该任务需要工作记忆,同时执行一项双条件关联任务(WM/BAT),这需要PFC-HPC相互作用。所有KD喂养的大鼠在WM/BAT上也表现出改善。行为测试完成后,从前额叶皮层收集组织切片进行生化分析。KD喂养的大鼠在前额叶皮层内有生化改变,这些改变与先前在海马体中的结果不同。具体而言,与对照组相比,KD喂养的大鼠中运输酮体的MCT1和MCT4显著增加。将葡萄糖转运过血脑屏障的GLUT1在KD喂养的大鼠中减少。与先前在海马体中的观察结果相反,前额叶皮层内的囊泡谷氨酸转运体(VGLUT1)不会随年龄或饮食而变化。然而,囊泡GABA转运体(VGAT)在前额叶皮层内增加,类似于海马体。这些数据表明,生酮饮食可能最适合增强对更高认知至关重要的大规模网络功能。
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