ABHD6 drives endocytosis of AMPA receptors to regulate synaptic plasticity and learning flexibility

IF 6.7 2区 医学 Q1 NEUROSCIENCES Progress in Neurobiology Pub Date : 2023-12-28 DOI:10.1016/j.pneurobio.2023.102559
Mengping Wei , Lei Yang , Feng Su , Ying Liu , Xinyi Zhao , Lin Luo , Xinyue Sun , Sen Liu , Zhaoqi Dong , Yong Zhang , Yun Stone Shi , Jing Liang , Chen Zhang
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Abstract

Trafficking of α‐Amino‐3–hydroxy‐5–methylisoxazole‐4–propionic acid (AMPA) receptors (AMPARs), mediated by AMPAR interacting proteins, enabled neurons to maintain tuning capabilities at rest or active state. α/β-Hydrolase domain-containing 6 (ABHD6), an endocannabinoid hydrolase, was an AMPAR auxiliary subunit found to negatively regulate the surface delivery of AMPARs. While ABHD6 was found to prevent AMPAR tetramerization in endoplasmic reticulum, ABHD6 was also reported to localize at postsynaptic site. Yet, the role of ABHD6 interacting with AMPAR at postsynaptic site, and the physiological significance of ABHD6 regulating AMPAR trafficking remains elusive. Here, we generated the ABHD6 knockout (ABHD6KO) mice and found that deletion of ABHD6 selectively enhanced AMPAR-mediated basal synaptic responses and the surface expression of postsynaptic AMPARs. Furthermore, we found that loss of ABHD6 impaired hippocampal long-term depression (LTD) and synaptic downscaling in hippocampal synapses. AMPAR internalization assays revealed that ABHD6 was essential for neuronal activity-dependent endocytosis of surface AMPARs, which is independent of ABHD6's hydrolase activity. The defects of AMPAR endocytosis and LTD are expressed as deficits in learning flexibility in ABHD6KO mice. Collectively, we demonstrated that ABHD6 is an endocytic accessory protein promoting AMPAR endocytosis, thereby contributes to the formation of LTD, synaptic downscaling and reversal learning.

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ABHD6 驱动 AMPA 受体的内吞,调节突触可塑性和学习灵活性
α-氨基-3-羟基-5-甲基异恶唑-4-丙酸(AMPAR)受体(AMPARs)在AMPAR相互作用蛋白的介导下进行迁移,使神经元能够在静息或活跃状态下保持调谐能力。含α/β-水解酶结构域的6(ABHD6)是一种内源性大麻素水解酶,它是一种AMPAR辅助亚基,被发现对AMPAR的表面传递有负面调节作用。虽然 ABHD6 被发现能阻止 AMPAR 在内质网中的四聚化,但 ABHD6 也被报道定位在突触后部位。然而,ABHD6 在突触后位点与 AMPAR 相互作用的作用以及 ABHD6 调节 AMPAR 转运的生理意义仍未确定。在这里,我们产生了 ABHD6 基因敲除(ABHD6KO)小鼠,并发现 ABHD6 的缺失选择性地增强了 AMPAR 介导的基础突触反应和突触后 AMPAR 的表面表达。此外,我们还发现 ABHD6 的缺失会损害海马突触的长期抑制(LTD)和突触降尺度。AMPAR内化实验显示,ABHD6对于神经元活动依赖性的表面AMPAR内吞至关重要,这与ABHD6的水解酶活性无关。ABHD6KO小鼠的AMPAR内吞和LTD缺陷表现为学习灵活性的缺陷。总之,我们证明了ABHD6是一种促进AMPAR内吞的内吞辅助蛋白,因此有助于LTD的形成、突触降尺度和逆转学习。
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来源期刊
Progress in Neurobiology
Progress in Neurobiology 医学-神经科学
CiteScore
12.80
自引率
1.50%
发文量
107
审稿时长
33 days
期刊介绍: Progress in Neurobiology is an international journal that publishes groundbreaking original research, comprehensive review articles and opinion pieces written by leading researchers. The journal welcomes contributions from the broad field of neuroscience that apply neurophysiological, biochemical, pharmacological, molecular biological, anatomical, computational and behavioral analyses to problems of molecular, cellular, developmental, systems, and clinical neuroscience.
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