Glucose-1,6-bisphosphate: A new gatekeeper of cerebral mitochondrial pyruvate uptake

IF 7 2区 医学 Q1 ENDOCRINOLOGY & METABOLISM
Motahareh Solina Safari , Priska Woerl , Carolin Garmsiri , Dido Weber , Marcel Kwiatkowski , Madlen Hotze , Louisa Kuenkel , Luisa Lang , Matthias Erlacher , Ellen Gelpi , Johannes A. Hainfellner , Gottfried Baier , Gabriele Baier-Bitterlich , Stephanie zur Nedden
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引用次数: 0

Abstract

Objective

Glucose-1,6-bisphosphate (G-1,6-BP), a byproduct of glycolysis that is synthesized by phosphoglucomutase 2 like 1 (PGM2L1), is particularly abundant in neurons. G-1,6-BP is sensitive to the glycolytic flux, due to its dependence on 1,3-bisphosphoglycerate as phosphate donor, and the energy state, due to its degradation by inosine monophosphate-activated phosphomannomutase 1. Since the exact role of this metabolite remains unclear, our aim was to elucidate the specific function of G-1,6-BP in the brain.

Methods

The effect of PGM2L1 on neuronal post-ischemic viability was assessed by siRNA-mediated knockdown of PGM2L1 in primary mouse neurons. Acute mouse brain slices were used to correlate the reduction in G-1,6-BP upon ischemia to changes in carbon metabolism by 13C6-glucose tracing. A drug affinity responsive target stability assay was used to test if G-1,6-BP interacts with the mitochondrial pyruvate carrier (MPC) subunits in mouse brain protein extracts. Human embryonic kidney cells expressing a MPC bioluminescence resonance energy transfer sensor were used to analyze how PGM2L1 overexpression affects MPC activity. The effect of G-1,6-BP on mitochondrial pyruvate uptake and oxygen consumption rates was analyzed in isolated mouse brain mitochondria. PGM2L1 and a predicted upstream kinase were overexpressed in a human neuroblastoma cell line and G-1,6-BP levels were measured.

Results

We found that G-1,6-BP in mouse brain slices was quickly degraded upon ischemia and reperfusion. Knockdown of PGM2L1 in mouse neurons reduced post-ischemic viability, indicating that PGM2L1 plays a neuroprotective role. The reduction in G-1,6-BP upon ischemia was not accompanied by alterations in glycolytic rates but we did see a reduced 13C6-glucose incorporation into citrate, suggesting a potential role in mitochondrial pyruvate uptake or metabolism. Indeed, G-1,6-BP interacted with both MPC subunits and overexpression of PGM2L1 increased MPC activity. G-1,6-BP, at concentrations found in the brain, enhanced mitochondrial pyruvate uptake and pyruvate-induced oxygen consumption rates. Overexpression of a predicted upstream kinase inhibited PGM2L1 activity, showing that besides metabolism, also signaling pathways can regulate G-1,6-BP levels.

Conclusions

We provide evidence that G-1,6-BP positively regulates mitochondrial pyruvate uptake and post-ischemic neuronal viability. These compelling data reveal a novel mechanism by which neurons can couple glycolysis-derived pyruvate to the tricarboxylic acid cycle. This process is sensitive to the glycolytic flux, the cell's energetic state, and upstream signaling cascades, offering many regulatory means to fine-tune this critical metabolic step.

1,6-二磷酸葡萄糖:大脑线粒体丙酮酸摄取的新看门人。
目的:葡萄糖-1,6-二磷酸(G-1,6-BP葡萄糖-1,6-二磷酸(G-1,6-BP)是糖酵解的副产物,由磷酸葡萄糖突变酶 2 样 1(PGM2L1)合成,在神经元中特别丰富。由于 G-1,6-BP 依赖 1,3-二磷酸甘油酯作为磷酸盐供体,因此它对糖酵解通量和能量状态都很敏感。由于这种代谢物的确切作用尚不清楚,我们的目的是阐明 G-1,6-BP 在大脑中的具体功能:方法:通过 siRNA 介导的小鼠原代神经元 PGM2L1 基因敲除,评估 PGM2L1 对神经元缺血后活力的影响。通过13C6-葡萄糖描记法将小鼠急性脑片缺血时G-1,6-BP的减少与碳代谢的变化联系起来。利用药物亲和力反应靶标稳定性测定法检测 G-1,6-BP 是否与小鼠脑蛋白提取物中的线粒体丙酮酸载体(MPC)亚基发生相互作用。表达 MPC 生物荧光共振能量转移传感器的人胚肾细胞被用来分析 PGM2L1 的过表达如何影响 MPC 的活性。在分离的小鼠脑线粒体中分析了 G-1,6-BP 对线粒体丙酮酸摄取和耗氧率的影响。在人神经母细胞瘤细胞系中过表达 PGM2L1 和一种预测的上游激酶,并测量 G-1,6-BP 的水平:结果:我们发现小鼠脑片中的G-1,6-BP在缺血和再灌注后迅速降解。小鼠神经元中 PGM2L1 的敲除降低了缺血后的存活率,表明 PGM2L1 起着神经保护作用。缺血时 G-1,6-BP 的减少并不伴随糖酵解率的改变,但我们确实看到 13C6 葡萄糖掺入柠檬酸盐的减少,这表明它可能在线粒体丙酮酸摄取或代谢中发挥作用。事实上,G-1,6-BP 与 MPC 的两个亚基都有相互作用,过量表达 PGM2L1 会增加 MPC 的活性。在大脑中发现的浓度下,G-1,6-BP 可提高线粒体的丙酮酸摄取量和丙酮酸诱导的氧消耗率。预测的上游激酶的过表达抑制了 PGM2L1 的活性,这表明除了新陈代谢外,信号通路也能调节 G-1,6-BP 的水平:我们提供的证据表明,G-1,6-BP 能积极调节线粒体丙酮酸摄取和缺血后神经元的存活能力。这些令人信服的数据揭示了神经元将糖酵解产生的丙酮酸与三羧酸循环耦合的新机制。这一过程对糖酵解通量、细胞能量状态和上游信号级联都很敏感,为微调这一关键代谢步骤提供了多种调节手段。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Molecular Metabolism
Molecular Metabolism ENDOCRINOLOGY & METABOLISM-
CiteScore
14.50
自引率
2.50%
发文量
219
审稿时长
43 days
期刊介绍: Molecular Metabolism is a leading journal dedicated to sharing groundbreaking discoveries in the field of energy homeostasis and the underlying factors of metabolic disorders. These disorders include obesity, diabetes, cardiovascular disease, and cancer. Our journal focuses on publishing research driven by hypotheses and conducted to the highest standards, aiming to provide a mechanistic understanding of energy homeostasis-related behavior, physiology, and dysfunction. We promote interdisciplinary science, covering a broad range of approaches from molecules to humans throughout the lifespan. Our goal is to contribute to transformative research in metabolism, which has the potential to revolutionize the field. By enabling progress in the prognosis, prevention, and ultimately the cure of metabolic disorders and their long-term complications, our journal seeks to better the future of health and well-being.
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