米替福新作为一种PPM1A激活剂,通过小胶质细胞/神经元的相互作用减轻tau蛋白病,从而改善小鼠的阿尔茨海默病样病理。
Miltefosine as a PPM1A activator improves AD-like pathology in mice by alleviating tauopathy via microglia/neurons crosstalk.
作者信息
Lv Jianlu, Shen Xingyi, Shen Xinya, Li Xiaoqian, Jin Zhuoying, Ouyang Xingnan, Lu Jian, Zhu Danyang, Wang Jiaying, Shen Xu
机构信息
Jiangsu Key Laboratory of Drug Target and Drug for Degenerative Diseases, Nanjing University of Chinese Medicine, Nanjing, 210023, China.
College of Pharmacy, Nanjing University of Chinese Medicine, Nanjing, 210023, China.
出版信息
Brain Behav Immun Health. 2022 Oct 29;26:100546. doi: 10.1016/j.bbih.2022.100546. eCollection 2022 Dec.
Alzheimer's disease (AD) is a progressively neurodegenerative disease without effective treatment. Here, we reported that the levels of expression and enzymatic activity of phosphatase magnesium-dependent 1A (PPM1A) were both repressed in brains of AD patient postmortems and 3 × Tg-AD mice, and treatment of adeno-associated virus (AAV)-ePHP-overexpression (OE)-PPM1A for brain-specific PPM1A overexpression or the new discovered PPM1A activator Miltefosine (MF, FDA approved oral anti-leishmanial drug) for PPM1A enzymatic activation improved the AD-like pathology in 3 × Tg-AD mice. The mechanism was intensively investigated by assay against the 3 × Tg-AD mice with brain-specific PPM1A knockdown (KD) through AAV-ePHP-KD-PPM1A injection. MF alleviated neuronal tauopathy involving microglia/neurons crosstalk by both promoting microglial phagocytosis of tau oligomers via PPM1A/Nuclear factor-κb (NF-κB)/C-X3-C Motif Chemokine Receptor 1 (CX3CR1) signaling and inhibiting neuronal tau hyperphosphorylation via PPM1A/NLR Family Pyrin Domain Containing 3 (NLRP3)/tau axis. MF suppressed microglial NLRP3 inflammasome activation by both inhibiting NLRP3 transcription via PPM1A/NF-κB/NLRP3 pathway in priming step and promoting PPM1A binding to NLRP3 to interfere NLRP3 inflammasome assembly in assembly step. Our results have highly addressed that PPM1A activation shows promise as a therapeutic strategy for AD and highlighted the potential of MF in treating this disease.
阿尔茨海默病(AD)是一种进行性神经退行性疾病,目前尚无有效治疗方法。在此,我们报告称,在AD患者尸检大脑和3×Tg-AD小鼠大脑中,镁依赖性磷酸酶1A(PPM1A)的表达水平和酶活性均受到抑制,通过腺相关病毒(AAV)-ePHP-过表达(OE)-PPM1A进行脑特异性PPM1A过表达治疗,或使用新发现的PPM1A激活剂米替福新(MF,美国食品药品监督管理局批准的口服抗利什曼原虫药物)激活PPM1A酶活性,均可改善3×Tg-AD小鼠的AD样病理特征。通过向3×Tg-AD小鼠脑内注射AAV-ePHP-KD-PPM1A进行脑特异性PPM1A基因敲低(KD)实验,深入研究了其作用机制。MF通过PPM1A/核因子-κB(NF-κB)/C-X3-C基序趋化因子受体1(CX3CR1)信号通路促进小胶质细胞对tau寡聚体的吞噬作用,并通过PPM1A/NLR家族含pyrin结构域3(NLRP3)/tau轴抑制神经元tau过度磷酸化,从而减轻涉及小胶质细胞/神经元相互作用的神经元tau病变。MF在启动步骤中通过PPM1A/NF-κB/NLRP3途径抑制NLRP3转录,并在组装步骤中促进PPM1A与NLRP3结合以干扰NLRP3炎性小体组装,从而抑制小胶质细胞NLRP3炎性小体激活。我们的研究结果充分表明,激活PPM1A有望成为AD的一种治疗策略,并突出了MF治疗该疾病的潜力。
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