Melatonin:a multitasking indoleamine to modulate hippocampal neurogenesis

Neurodegeneration affects a large number of cell types including neurons,astrocytes or oligodendrocytes,and neural stem cells.Neural stem cells can generate new neuronal populations through proliferation,migration,and differentiation.This neurogenic potential may be a relevant factor to fight neurodegeneration and aging.In the last years,we can find growing evidence suggesting that melatonin may be a potential modulator of adult hippocampal neurogenesis.The lack of therapeutic strategies targeting neurogenesis led researchers to explore new molecules.Numerous preclinical studies with melatonin observed how melatonin can modulate and enhance molecular and signaling pathways involved in neurogenesis.We made a special focus on the connection between these modulation mechanisms and their implication in neurodegeneration,to summarize the current knowledge and highlight the therapeutic potential of melatonin.

The detrimental effects of lipopolysaccharideinduced neuroinflammation on adult hippocampal neurogenesis depend on the duration of the pro-inflammatory response

Adult hippocampal neurogenesis is a finely tuned process regulated by extrinsic factors. Neuroinflammation is a hallmark of several pathological conditions underlying dysregulation of neurogenesis. In animal models, lipopolysaccharide(LPS)-induced neuroinflammation leads to a neurogenic decrease mainly associated to the early inflammatory response. However, it is not well understood how the neuroinflammatory response progresses over time and if neurogenesis continues to be diminished during the late neuroinflammatory response. Moreover, it is unknown if repeated intermittent administration of LPS along time induces a greater reduction in neurogenesis. We administered one single intraperitoneal injection of LPS or saline or four repeated injections(one per week) of LPS or saline to young-adult mice. A cohort of new cells was labeled with three 5-bromo-2-deoxyuridine injections(one per day) 4 days after the last LPS injection. We evaluated systemic and neuroinflammation-associated parameters and compared the effects of the late neuroinflammatory response on neurogenesis induced by each protocol. Our results show that 1) a single LPS injection leads to a late pro-inflammatory response characterized by microglial activation, moderate astrocytic reaction and increased interleukin-6 levels. This response correlates in time with decreased neurogenesis and 2) a repeated intermittent injection of LPS does not elicit a late pro-inflammatory response although activated microglia persists. The latter profile is not accompanied by a continued longterm hippocampal neurogenic decrease. Hereby, we provide evidence that the neuroinflammatory response is a dynamic process that progresses in a milieu-dependent manner and does not necessarily lead to a neurogenic decrease, highlighting the complex interaction between the immune system and neurogenesis.

A new age in understanding adult hippocampal neurogenesis in Alzheimer’s disease

Several lines of evidence have established that proliferation and differentiation of neural stem cells into neurons within the sub-granular zone of the dentate gyrus,a process named adult hippocampal neurogenesis,contribute to maintaining healthy cognitive functions throughout life.The rate of adult hippocampal neurogenesis decreases with aging and a premature impairment of adult hippocampal neurogenesis has been observed both in animal models of Alzheimer’s disease and human post-mortem tissues.The causal relationship between adult hippocampal neurogenesis and the development of Alzheimer’s disease pathology has,however,not been established.This is partly due to the limitation of recapitulating the development of Alzheimer’s disease pathology in rodent models and the lack of translatable biomarkers to identify tractable targets in humans.While it is tempting to postulate that adult hippocampal neurogenesis could be leveraged to improve cognitive deficits in Alzheimer’s disease,consensual results have yet to be reached to fully explore this hypothesis.In this review,we discuss how the recent progress in identifying molecular pathways in adult hippocampal neurogenesis provides a good framework to initiate strategies for drug-based intervention in neurodegenerative diseases,especially in Alzheimer’s disease.We outline how discrepancies in pre-clinical disease models and experimental methodology have resulted in contradictory findings and propose a shift towards using more translatable approaches to model neurogenesis in Alzheimer’s disease.In particular,we review how exploring novel experimental paradigms including the use of human induced pluripotent stem cells and more complex cell culture systems,as well as standardizing protocols used to investigate evidence of neurogenesis in human tissues,could deliver deeper mechanistic insights that would kick-start innovative drug discovery efforts to promote healthy aging and cellular rejuvenation.

Adult hippocampal neurogenesis and its impairment in Alzheimer's disease

Adult neurogenesis is the creation of new neurons which integrate into the existing neural circuit of the adult brain.Recent evidence suggests that adult hippocampal neurogenesis(AHN)persists throughout life in mammals,including humans.These newborn neurons have been implicated to have a crucial role in brain functions such as learning and memory.Importantly,studies have also found that hippocampal neurogenesis is impaired in neurodegenerative and neuropsychiatric diseases.Alzheimer’s disease(AD)is one of the most common forms of dementia affecting millions of people.Cognitive dysfunction is a common symptom of AD patients and progressive memory loss has been attributed to the degeneration of the hippocampus.Therefore,there has been growing interest in identifying how hippocampal neurogenesis is affected in AD.However,the link between cognitive decline and changes in hippocampal neurogenesis in AD is poorly understood.In this review,we summarized the recent literature on AHN and its impairments in AD.

Active fraction combination from Liuwei Dihuang decoction improves adult hippocampal neurogenesis and neurogenic microenvironment in cranially irradiated mice

OBJECTIVE Cranial radiotherapy is clinically used in the treatment of brain tumors;however,the consequent cognitive and emotional dysfunctions seriously impair the life quality of patients.LW-AFC,an active fraction combination extracted from classical traditional Chinese medicine prescription Liuwei Dihuang decoction,can improve cognitive and emotional dysfunctions in many animal models;however,the protective effect of LW-AFC on cranial irradiation-induced cognitive and emotional dysfunctions has not been reported.Recent studies indicate that impairment of adult hippocampal neurogenesis(AHN)and alterations of the neurogenic microenvironment in the hippocampus constitute critical factors in cognitive and emotional dysfunctions following cranial irradiation.Here,our research further investigated the potential protective effects and mechanisms of LW-AFC on cranial irradiation-induced cognitive and emotional dysfunctions in mice.METHODS LW-AFC(1.6 g·kg^(-1))was intragastrically administered to mice for 14 d before cranial irradiation(7 Gyγ-ray).AHN was examined by quantifying the number of proliferative neural stem cells and immature neurons in the dorsal and ventral hippocampus.The contextual fear conditioning test,open field test,and tail suspension test were used to assess cognitive and emotional functions in mice.To detect the change of the neurogenic microenvironment,colorimetry and multiplex bead analysis were performed to measure the level of oxidative stress,neurotrophic and growth factors,and inflammation in the hippocampus.RESULTS LW-AFC exerted beneficial effects on the contextual fear memory,anxiety behavior,and depression behavior in irradiated mice.Moreover,LW-AFC increased the number of proliferative neural stem cells and immature neurons in the dorsal hippocampus,displaying a regional specificity of neurogenic response.For the neurogenic microenvironment,LW-AFC significantly increased the contents of superoxide dismutase,glutathione peroxidase,glutathione,and catalase and decreased the content of malondialdehyde in the hippocampus of irradiated mice,accompanied by the increase in brain-derived neurotrophic factor,insulin-like growth factor-1,and interleukin-4 content.Together,LW-AFC improved cognitive and emotional dysfunctions,promoted AHN preferentially in the dorsal hippocampus,and ameliorated disturbance in the neurogenic microenvironment in irradiated mice.CONCLUSION LW-AFC ameliorates cranial irradiation-induced cognitive and emotional dysfunctions,and the underlying mechanisms are mediated by promoting AHN in the dorsal hippocampus and improving the neurogenic microenvironment.LW-AFC might be a promising therapeutic agent to treat cognitive and emotional dysfunctions in patients receiving cranial radiotherapy.

Cholesterol or Fat Rich Diets Accelerate Natural Age-Decline on Adult Hippocampal Neurogenesis and Have an Impact in Memory and Like-Anxiety Behavior

Diet is an important health factor and it has been recently associated with neurodegenerative diseases and cognitive decline. Here it was investigated the effect of fatty acid or cholesterol rich diets with the possible acceleration of the biological decline in adult hippocampal neurogenesis associated with aging in middle-age rats, and its impact on anxiety and memory function. It was found that a diet of 10 weeks with saturated fatty acids and cholesterol has a detrimental effect on memory function, exerts like-anxiety behavior and diminishes the presence of new generated neurons in the hippocampus in six months old rats.

Impact of pediatric traumatic brain injury on hippocampal neurogenesis

Traumatic brain injury(TBI)is a major cause of mortality and morbidity in the pediatric population.With advances in medical care,the mortality rate of pediatric TBI has declined.However,more children and adolescents are living with TBI-related cognitive and emotional impairments,which negatively affects the quality of their life.Adult hippocampal neurogenesis plays an important role in cognition and mood regulation.Alterations in adult hippocampal neurogenesis are associated with a variety of neurological and neurodegenerative diseases,including TBI.Promoting endogenous hippocampal neurogenesis after TBI merits significant attention.However,TBI affects the function of neural stem/progenitor cells in the dentate gyrus of hippocampus,which results in aberrant migration and impaired dendrite development of adult-born neurons.Therefore,a better understanding of adult hippocampal neurogenesis after TBI can facilitate a more successful neuro-restoration of damage in immature brains.Secondary injuries,such as neuroinflammation and oxidative stress,exert a significant impact on hippocampal neurogenesis.Currently,a variety of therapeutic approaches have been proposed for ameliorating secondary TBI injuries.In this review,we discuss the uniqueness of pediatric TBI,adult hippocampal neurogenesis after pediatric TBI,and current efforts that promote neuroprotection to the developing brains,which can be leveraged to facilitate neuroregeneration.

运动训练对创伤后应激障碍小鼠焦虑和抑郁样行为的影响

目的:探讨运动缓解创伤后应激障碍(PTSD)焦虑抑郁样行为的作用及促进海马神经再生的中枢调控机制。方法:将雄性C57BL/6J小鼠随机分为对照组(Control)、PTSD建模组(PTSD)、建模后低强度运动组(PTSD+LE)和建模后高强度运动组(PTSD+HE)。采用条件性足部电击(CF)和单次-持续应激(SPS)相结合的方法,构建PTSD复合应激模型。利用旷场实验和悬尾实验分别评估小鼠的焦虑和抑郁样行为。通过免疫荧光双标实验观察小鼠海马DG区新生成熟神经元和增殖细胞。采用Western Blot检测小鼠海马脂联素受体1(AdipoR1)的表达情况。结果:旷场实验结果表明PTSD+HE组小鼠在中央区域的活动距离以及逗留时间明显长于PTSD组及PTSD+LE组(P<0.05);悬尾实验结果显示与PTSD组小鼠相比,不同程度运动训练组小鼠的不动时间明显减少(P<0.05),而且PTSD+HE组更显著(P<0.05)。此外,PTSD+HE组小鼠海马DG区的BrdU+、BrdU+/NeuN+与MCM2+细胞密度明显升高(P<0.05)。PTSD+HE组小鼠海马AdipoR1蛋白表达明显上调(P<0.05)。结论:PTSD小鼠焦虑和抑郁样行为与海马神经再生水平下降有关。运动可改善其焦虑和抑郁样行为,作用机制可能与促进AdipoR1表达、促进海马神经再生有关。

有氧运动对阿尔茨海默症小鼠成年海马神经发生的影响

背景:运动有助于改善阿尔茨海默症、痴呆症以及与年龄相关的认知能力,运动与这些健康益处之间的一个潜在中介可能是成年海马神经发生。因此,探索运动如何影响阿尔茨海默症小鼠的成年海马神经发生过程具有重要意义。目的:观察有氧运动对阿尔茨海默症小鼠成年海马神经发生的影响,探究有氧运动能否促进其成年海马神经发生。方法:将3月龄野生型(C57BL/6Jnju)及APP/PS1双转基因阿尔茨海默症小鼠随机分为4组:野生对照组、野生运动组、阿尔茨海默症对照组、阿尔茨海默症运动组,每组20只。对照组小鼠不进行运动,运动组小鼠进行5个月的有氧运动干预。运动干预结束后,采用Real-time PCR、免疫荧光及Western blot检测各组小鼠海马组织DCX、Ki67、βⅢ-tubulin及NeuN的表达。结果与结论:阿尔茨海默症对照组小鼠海马齿状回区DCX、βⅢ-tubulin及NeuN表达均显著低于野生对照组小鼠(P<0.05);阿尔茨海默症运动组小鼠海马齿状回区DCX、Ki67、βⅢ-tubulin及NeuN表达显著高于阿尔茨海默症对照组(P<0.05)。提示:长期有氧运动干预后,可以促进阿尔茨海默症小鼠成年海马神经发生过程中神经元增殖、迁移分化,显著增加神经元前体细胞、新生神经元数量。

不同强度运动改善PTSD小鼠恐惧记忆泛化及促海马神经再生效应研究

目的:探讨不同强度运动缓解创伤后应激障碍(PTSD)恐惧记忆泛化的作用及促海马神经再生中枢调控机制。方法:采用随机数字法将雄性C57 BL/6J小鼠分为对照(control)组、PTSD建模(PTSD)组、建模后高强度运动(PTSD-High)组和建模后低强度运动(PTSD-Low)组。采用条件性足部电击(CF)和单次-持续应激(SPS)相结合的方法,构建PTSD复合应激模型。利用条件性恐惧实验测试小鼠对恐惧记忆相似情境的辨别能力,评估小鼠恐惧记忆泛化程度,通过免疫荧光双标实验观察并量化小鼠海马DG区新生的未成熟神经元,使用ELISA测定血清脂联素的分泌水平。结果:(1)在条件性恐惧实验三个类似情境中,control组与PTSD-High组的不动时间均明显低于PTSD组。(2)免疫荧光双标染色图片显示,PTSD组小鼠海马DG区的新生神经元与未成熟神经元荧光信号降低,新生未成熟神经元纤维短而少。统计表明,与PTSD组相比,control、PTSD-High和PTSD-Low组小鼠新生未成熟神经元的细胞密度和树突分支点及长度均明显升高。(3)ELISA结果显示,control和PTSD-High组小鼠血清中脂联素水平均明显高于PTSD组和PTSD-Low组。结论:PTSD小鼠恐惧记忆泛化与海马神经再生水平下降有关。运动可能通过促进脂联素的分泌、促进海马神经再生改善恐惧记忆泛化。不同强度运动对比发现高强度运动改善效果更好。

Adult neural stem cells and schizophrenia

Schizophrenia(SCZ)is a devastating and complicated mental disorder accompanied by variable positive and negative symptoms and cognitive deficits.Although many genetic risk factors have been identified,SCZ is also considered as a neurodevelopmental disorder.Elucidation of the pathogenesis and the development of treatment is challenging because complex interactions occur between these genetic risk factors and environment in essential neurodevelopmental processes.Adult neural stem cells share a lot of similarities with embryonic neural stem cells and provide a promising model for studying neuronal development in adulthood.These adult neural stem cells also play an important role in cognitive functions including temporal and spatial memory encoding and context discrimination,which have been shown to be closely linked with many psychiatric disorders,such as SCZ.Here in this review,we focus on the SCZ risk genes and the key components in related signaling pathways in adult hippocampal neural stem cells and summarize their roles in adult neurogenesis and animal behaviors.We hope that this would be helpful for the understanding of the contribution of dysregulated adult neural stem cells in the pathogenesis of SCZ and for the identification of potential therapeutic targets,which could facilitate the development of novel medication and treatment.

成年海马神经再生改善模式分离鲁棒性

成年海马神经再生(adult hippocampal neurogenesis,AHN)被认为能有效参与齿状回(dentate gyrus,DG)网络来加强模式分离功能.目前虽然神经再生在模式分离中的潜在作用已在理论上得到了研究,但产生的新生颗粒细胞在信息处理和网络调节中的具体作用仍存在争议.针对上述问题,本文引入4-6周新生颗粒细胞作为独立的信息处理单元,提出了一种具有神经再生的DG网络计算模型.重点研究了不同输入刺激下新生颗粒细胞对模式分离的贡献.通过模拟实验,本文发现在不同强度的刺激下,新生颗粒细胞在齿状回网络中扮演着不同的角色.在低强度刺激下,新生颗粒细胞利用其易激活的神经元特性,可以恢复网络的信息表达能力,避免模式分离失败.在高强度刺激下,新生颗粒细胞作为一种中间神经元,能有效增强局部回路的反馈抑制作用,提高成熟颗粒细胞的稀疏性,最终增强模式分离功能.因此,该模型预测了在更精细和更广泛的输入下,成年海马神经再生在模式分离鲁棒性中的关键作用.

β‑Hydroxybutyric acid improves cognitive function in a model of heat stress by promoting adult hippocampal neurogenesis

Heat stress has multiple potential effects on the brain,such as neuroinflammation,neurogenesis defects,and cog-nitive impairment.β-hydroxybutyric acid(BHBA)has been demonstrated to play neuroprotective roles in various models of neurological diseases.In the present study,we investigated the efficacy of BHBA in alleviating heat stress-induced impairments of adult hippocampal neurogenesis and cognitive function,as well as the underlying mecha-nisms.Mice were exposed to 43℃for 15 min for 14 days after administration with saline,BHBA,or minocycline.Here,we showed for the first time that BHBA normalized memory ability in the heat stress-treated mice and attenuated heat stress-impaired hippocampal neurogenesis.Consistently,BHBA noticeably improved the synaptic plasticity in the heat stress-treated hippocampal neurons by inhibiting the decrease of synapse-associated proteins and the density of dendritic spines.Moreover,BHBA inhibited the expression of cleaved caspase-3 by suppressing endoplasmic reticu-lum(ER)stress,and increased the expression of brain-derived neurotrophic factor(BDNF)in the heat stress-treated hippocampus by activating the protein kinase B(Akt)/cAMP response element binding protein(CREB)and methyl-CpG binding protein 2(MeCP2)pathways.These findings indicate that BHBA is a potential agent for improving cogni-tive functions in heat stress-treated mice.The action may be mediated by ER stress,and Akt-CREB-BDNF and MeCP2 pathways to improve adult hippocampal neurogenesis and synaptic plasticity.

运动调节阿尔茨海默症成年海马神经发生的作用及机制

背景:研究发现,运动可以调节成年海马神经发生,并改善阿尔茨海默症患者的认知功能。然而,运动如何影响成年海马神经发生及改善阿尔茨海默症患者认知功能的机制并不清楚。目的:分析总结运动如何影响成年海马神经发生,以及成年海马神经发生在运动改善阿尔茨海默症中的作用机制。方法:以中文检索词(运动,神经发生,阿尔兹海默病,认知)及英文检索词(exercise,neurogenesis,AHN,Alzheimer’s disease,aging,cognition)分别检索CNKI、Web of Science数据库(包含WOS,DIIDW,INSPEC,KJD,MEDLINE,RSCI,SCIELO)等国内外数据库,检索时间截止至2020年12月,查询运动影响阿尔茨海默症及成年海马神经发生的相关研究,然后按照一定逻辑进行分析和综述。结果与结论:(1)运动可以通过增加星形胶质细胞的增殖和葡萄糖转运蛋白1、血管内皮生长因子、脑源性神经营养因子等的分泌来调节神经源龛的整体动态平衡,从而促进阿尔茨海默症患者成年海马神经发生过程;(2)然而这一过程会受到谷氨酸、γ-氨基丁酸、5-羟色胺、血管内皮生长因子、N-甲基-d-天冬氨酸、脑源性神经营养因子等介质、生长因子或神经营养因子的影响。

二十二碳六烯酸改善抑郁母鼠子代的认知功能研究

目的探讨二十二碳六烯酸(DHA)对由孕期抑郁引起的子代抑郁行为和认知能力的影响以及其可能的机制。方法通过长期束缚构建抑郁孕鼠模型。强迫游泳和悬尾实验用以检测小鼠抑郁状态,新物体和新位置识别实验用以检测小鼠的认知能力;免疫组化方法检测小鼠海马神经干细胞的生长情况。结果相较于对照组小鼠,束缚应激组的小鼠在强迫游泳和悬尾实验中不动时间增加(P<0.001);对新物体和新位置的物体探索时间降低(P<0.001);以及成年海马神经发生数目减少(P<0.001)。孕鼠在束缚应激期补充DHA后子鼠相较于没有补充DHA孕鼠的子鼠,在强迫游泳和悬尾实验中不动时间减少(P<0.001);对于新物体和新位置的物体的探索时间增加(P<0.001);成年海马神经发生数目增加(P<0.001)。结论孕期补充DHA可以降低母鼠孕期应激引起的子鼠抑郁状行为以及认知损伤,其机制可能和增加子鼠的成年海马神经发生有关。

癌症治疗对海马神经元生成的影响及其与认知功能和抑郁症间的关系

海马区齿状回颗粒下层是大脑神经元生成的主要区域,动物成年后神经干细胞仍不断的增殖和变异,形成新的神经元。成人海马神经元生成与空间意识、长期记忆、情感及情绪等功能相关。癌症治疗的目的是为了减少肿瘤细胞的分裂,然而,异常细胞分裂被中断的同时也抑制了成年神经干细胞的增殖和海马神经元的生成。癌症患者在治疗过程中常伴随着记忆功能的衰退及抑郁症状的出现。因此,本文主要综述癌症治疗对成人海马神经元生成的影响及与伴随出现的认知和情绪障碍间的潜在联系。

运动缓解创伤后应激障碍恐惧记忆泛化及成体海马神经再生机制研究进展

运动可通过成体海马神经再生(adult hippocampal neurogenesis,AHN)促进模式分离从而有效缓解创伤后应激障碍(post-traumatic stress disorder,PTSD)恐惧记忆泛化,即通过运动促进AHN可以减少PTSD患者的恐惧记忆对相似记忆的干扰,从而缓解PTSD患者的恐惧记忆泛化,这为运动干预有效治疗PTSD恐惧记忆泛化的可行性提供了理论支持。该文阐述了运动促进的AHN改善PTSD恐惧记忆泛化的研究进展,以期为PTSD基础研究及治疗提供新思路。

自主跑轮运动上调成年小鼠海马齿状回区细胞增殖及BDNF、IGF1和WNT4的表达水平

成年海马神经发生在调控学习记忆和情感过程中有重要作用。外界刺激因素,如自主运动能影响成年海马神经发生过程。自主运动能显著增强海马齿状回区的细胞增殖,并使新生神经元增多,但其具体机制仍不是十分清楚。本研究采用跑轮实验这种啮齿动物自主运动模型,使两月龄的C57BL/6成年小鼠跑轮15天后,用BrdU掺入实验观察海马齿状回区的细胞增殖情况。采用逆转录实时荧光定量PCR法(RT-qPCR)和蛋白免疫印迹法(Western blot)检测海马齿状回区、阿蒙角区和皮层区成年神经发生相关因子的mRNA和蛋白表达水平。结果显示,自主跑轮运动15天后的成年小鼠海马齿状回区增殖细胞数目显著上调;齿状回区Bdnf、Igf1的mRNA和蛋白表达水平显著升高,Wnt4的mRNA表达水平显著升高,提示15天自主运动可能通过特异地增加海马齿状回区BDNF、IGF1和WNT4的表达产生上调成年海马神经发生的作用。

促海马区成体神经发生药物的研究进展

阿尔兹海默病发病机制尚未阐明,目前临床上使用的药物均只能针对相应症状,不能逆转病情的发展进程,故采用新的治疗策略对阿尔兹海默病进行防治成为必然。海马区为实现学习、记忆和认知调节等功能提供了生理基础,与阿尔兹海默病的发生、发展密切相关。该区域存在成体神经发生现象,在某种意义上实现了大脑的可塑性,有望为阿尔兹海默病等神经退行性疾病的治疗开拓新的领域。本文从促进海马区成体神经发生的角度,提出了阿尔兹海默病的新的治疗方向,并总结了促成体神经发生药物的最新进展。