多巴胺信号调节小胶质细胞 NLRP3 炎症小体的激活:对帕金森病的影响。
Dopamine signaling modulates microglial NLRP3 inflammasome activation: implications for Parkinson's disease.
机构信息
Department of Clinical Chemistry, Amsterdam Neuroscience, Neurochemistry Laboratory, Amsterdam UMC, Vrije Universiteit Amsterdam, De Boelelaan 1117, 1081 HV, Amsterdam, The Netherlands.
Department of Biology, University of Padua, Padua, Italy.
出版信息
J Neuroinflammation. 2022 Feb 16;19(1):50. doi: 10.1186/s12974-022-02410-4.
BACKGROUND
Parkinson's disease (PD) is characterized by the loss of nigral dopaminergic neurons leading to impaired striatal dopamine signaling, α-synuclein- (α-syn-) rich inclusions, and neuroinflammation. Degenerating neurons are surrounded by activated microglia with increased secretion of interleukin-1β (IL-1β), driven largely by the NLRP3 inflammasome. A critical role for microglial NLRP3 inflammasome activation in the progression of both dopaminergic neurodegeneration and α-syn pathology has been demonstrated in parkinsonism mouse models. Fibrillar α-syn activates this inflammasome in mouse and human macrophages, and we have shown previously that the same holds true for primary human microglia. Dopamine blocks microglial NLRP3 inflammasome activation in the MPTP model, but its effects in this framework, highly relevant to PD, remain unexplored in primary human microglia and in other in vivo parkinsonism models.
METHODS
Biochemical techniques including quantification of IL-1β secretion and confocal microscopy were employed to gain insight into dopamine signaling-mediated inhibition of the NLRP3 inflammasome mechanism in primary human microglia and the SYN120 transgenic mouse model. Dopamine and related metabolites were applied to human microglia together with various inflammasome activating stimuli. The involvement of the receptors through which these catecholamines were predicted to act were assessed with agonists in both species.
RESULTS
We show in primary human microglia that dopamine, L-DOPA, and high extracellular K, but not norepinephrine and epinephrine, block canonical, non-canonical, and α-syn-mediated NLRP3 inflammasome-driven IL-1β secretion. This suggests that dopamine acts as an inflammasome inhibitor in human microglia. Accordingly, we provide evidence that dopamine exerts its inhibitory effect through dopamine receptor D1 and D2 (DRD1 and DRD2) signaling. We also show that aged mice transgenic for human C-terminally truncated (1-120) α-syn (SYN120 tg mice) display increased NLRP3 inflammasome activation in comparison to WT mice that is diminished upon DRD1 agonism.
CONCLUSIONS
Dopamine inhibits canonical, non-canonical, and α-syn-mediated activation of the NLRP3 inflammasome in primary human microglia, as does high extracellular K. We suggest that dopamine serves as an endogenous repressor of the K efflux-dependent microglial NLRP3 inflammasome activation that contributes to dopaminergic neurodegeneration in PD, and that this reciprocation may account for the specific vulnerability of these neurons to disease pathology.
背景
帕金森病(PD)的特征是黑质多巴胺能神经元丧失,导致纹状体多巴胺信号转导受损、α-突触核蛋白(α-syn)丰富的内含物和神经炎症。退化的神经元被激活的小胶质细胞包围,小胶质细胞的白细胞介素-1β(IL-1β)分泌增加,主要由 NLRP3 炎性小体驱动。在帕金森病小鼠模型中,小胶质细胞 NLRP3 炎性小体的激活在多巴胺能神经退行性变和 α-syn 病理的进展中起着关键作用。纤维状 α-syn 在小鼠和人巨噬细胞中激活了这种炎性小体,我们之前已经表明,原代人小胶质细胞也是如此。多巴胺在 MPTP 模型中阻断小胶质细胞 NLRP3 炎性小体的激活,但在这个与 PD 高度相关的框架中,其在原代人小胶质细胞和其他体内帕金森病模型中的作用仍未得到探索。
方法
采用生化技术,包括 IL-1β 分泌的定量和共聚焦显微镜,研究多巴胺信号转导对原代人小胶质细胞和 SYN120 转基因小鼠模型中 NLRP3 炎性小体抑制的机制。将多巴胺和相关代谢物与各种炎性小体激活刺激物一起应用于人小胶质细胞。通过在两种物种中使用激动剂来评估这些儿茶酚胺作用的受体。
结果
我们在原代人小胶质细胞中表明,多巴胺、L-DOPA 和高细胞外 K+,而不是去甲肾上腺素和肾上腺素,阻断了经典的、非经典的和 α-syn 介导的 NLRP3 炎性小体驱动的 IL-1β 分泌。这表明多巴胺在人小胶质细胞中作为炎性小体抑制剂发挥作用。因此,我们提供了证据表明,多巴胺通过多巴胺受体 D1 和 D2(DRD1 和 DRD2)信号发挥其抑制作用。我们还表明,与 WT 小鼠相比,携带人 C 端截断(1-120)α-syn(SYN120 tg 小鼠)的老年转基因小鼠显示出 NLRP3 炎性小体激活增加,而 DRD1 激动剂可减少这种激活。
结论
多巴胺抑制原代人小胶质细胞中经典的、非经典的和 α-syn 介导的 NLRP3 炎性小体的激活,以及高细胞外 K+。我们认为,多巴胺作为 K 外流依赖性小胶质细胞 NLRP3 炎性小体激活的内源性抑制剂,有助于 PD 中的多巴胺能神经退行性变,这种相互作用可能解释了这些神经元对疾病病理的特定易感性。
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