Graduate Institute of Medicine, College of Medicine, Kaohsiung Medical University, Kaohsiung, Taiwan.
Institute for Translational Research in Biomedicine, Kaohsiung Chang Gung Memorial Hospital, Kaohsiung, Taiwan.
Cell Commun Signal. 2023 Jun 14;21(1):140. doi: 10.1186/s12964-023-01158-5.
We previously reported that miR-195 exerts neuroprotection by inhibiting Sema3A and cerebral miR-195 levels decreased with age, both of which urged us to explore the role of miR-195 and miR-195-regulated Sema3 family members in age-associated dementia.
miR-195a KO mice were used to assess the effect of miR-195 on aging and cognitive functions. Sema3D was predicted as a miR-195 target by TargetScan and then verified by luciferase reporter assay, while effects of Sema3D and miR-195 on neural senescence were assessed by beta-galactosidase and dendritic spine density. Cerebral Sema3D was over-expressed by lentivirus and suppressed by si-RNA, and effects of over-expression of Sema3D and knockdown of miR-195 on cognitive functions were assessed by Morris Water Maze, Y-maze, and open field test. The effect of Sema3D on lifespan was assessed in Drosophila. Sema3D inhibitor was developed using homology modeling and virtual screening. One-way and two-way repeated measures ANOVA were applied to assess longitudinal data on mouse cognitive tests.
Cognitive impairment and reduced density of dendritic spine were observed in miR-195a knockout mice. Sema3D was identified to be a direct target of miR-195 and a possible contributor to age-associated neurodegeneration as Sema3D levels showed age-dependent increase in rodent brains. Injection of Sema3D-expressing lentivirus caused significant memory deficits while silencing hippocampal Sema3D improved cognition. Repeated injections of Sema3D-expressing lentivirus to elevate cerebral Sema3D for 10 weeks revealed a time-dependent decline of working memory. More importantly, analysis of the data on the Gene Expression Omnibus database showed that Sema3D levels were significantly higher in dementia patients than normal controls (p < 0.001). Over-expression of homolog Sema3D gene in the nervous system of Drosophila reduced locomotor activity and lifespan by 25%. Mechanistically, Sema3D might reduce stemness and number of neural stem cells and potentially disrupt neuronal autophagy. Rapamycin restored density of dendritic spines in the hippocampus from mice injected with Sema3D lentivirus. Our novel small molecule increased viability of Sema3D-treated neurons and might improve autophagy efficiency, which suggested Sema3D could be a potential drug target. Video Abstract CONCLUSION: Our results highlight the importance of Sema3D in age-associated dementia. Sema3D could be a novel drug target for dementia treatment.
我们之前的研究表明 miR-195 通过抑制 Sema3A 发挥神经保护作用,并且随着年龄的增长,大脑中的 miR-195 水平降低,这促使我们探索 miR-195 和受其调控的 Sema3 家族成员在与年龄相关的痴呆症中的作用。
使用 miR-195a 敲除小鼠评估 miR-195 对衰老和认知功能的影响。TargetScan 预测 Sema3D 是 miR-195 的靶标,然后通过荧光素酶报告基因实验验证,同时通过β-半乳糖苷酶和树突棘密度评估 Sema3D 和 miR-195 对神经衰老的影响。通过慢病毒过表达和 siRNA 抑制来上调大脑中的 Sema3D,通过 Morris 水迷宫、Y 迷宫和旷场试验评估 Sema3D 过表达和 miR-195 敲低对认知功能的影响。使用同源建模和虚拟筛选开发 Sema3D 抑制剂。采用单向和双向重复测量方差分析评估小鼠认知测试的纵向数据。
在 miR-195a 敲除小鼠中观察到认知障碍和树突棘密度降低。Sema3D 被鉴定为 miR-195 的直接靶标,并且可能是与年龄相关的神经退行性变的一个促成因素,因为 Sema3D 水平在啮齿动物大脑中表现出与年龄相关的增加。注射 Sema3D 表达的慢病毒会导致明显的记忆缺陷,而抑制海马体中的 Sema3D 则改善了认知功能。重复注射 Sema3D 表达的慢病毒以 10 周的时间升高大脑中的 Sema3D,结果显示工作记忆随时间推移而下降。更重要的是,对基因表达综合数据库中数据的分析表明,痴呆症患者的 Sema3D 水平明显高于正常对照组(p < 0.001)。在果蝇的神经系统中过表达同源 Sema3D 基因会使运动活性和寿命降低 25%。从机制上讲,Sema3D 可能会降低神经干细胞的干性和数量,并可能破坏神经元自噬。雷帕霉素恢复了 Sema3D 慢病毒注射小鼠海马体树突棘的密度。我们的新型小分子增加了 Sema3D 处理神经元的存活率,并可能提高自噬效率,这表明 Sema3D 可能是一个潜在的药物靶点。
我们的研究结果强调了 Sema3D 在与年龄相关的痴呆症中的重要性。Sema3D 可能成为治疗痴呆症的新型药物靶点。
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