突触蛋白在学习记忆过程中的作用

学习和记忆是脑的高级功能。学习指人和动物获得外界知识的神经过程;记忆指将获得的知识储存和读出的神经过程。突触蛋白(synapsin)是一种与突触结构和功能密切相关的膜蛋白,在突触的可塑性以及长时程增强(long-timepotentiation,LTP)中起着重要作用。而突触可塑性是突触对内外环境变化作出反应的能力,是学习记忆的神经生物学基础。LTP一直被认为是学习记忆的神经基础之一,是突触可塑性的功能指标,也是研究学习记忆的理想模型。该文介绍突触蛋白在学习记忆过程中的作用及机制、突触蛋白在学习记忆研究中的应用。     

突触可塑性与脑疾病的神经发育基础

大脑神经回路高度有序的神经元活动是高级脑功能的基础,神经元之间的突触联结是神经回路的关键功能节点。神经突触根据神经元活动调整其传递效能的能力,亦即突触可塑性,被认为是神经回路发育和学习与记忆功能的基础。其异常则可能导致如抑郁症和阿尔茨海默病等精神、神经疾病。将介绍这两种疾病与突触可塑性的关系,聚焦于相关分子和细胞机制以及新的研究、治疗手段等进展。     

脑内ATF4对学习记忆的调节作用

转录激活因子4(ATF4)属于碱性亮氨酸拉链结构域蛋白中的ATF/CREB转录因子家族,ATF4在脑内广泛表达,在应激、痛觉、突触可塑性和神经退行性变等中发挥重要作用。学习与记忆是脑的高级功能之一,学习是获取新信息的过程,记忆是将信息进行编码、储存及提取的过程,二者被认为是认知活动的基础。突触可塑性是突触在形态、结构和功能上的可变性和可修饰性,与神经系统的发育和学习记忆等脑的高级功能密切相关。突触可塑性的长时程增强和长时程抑制是学习和记忆形成的基础。近年来研究发现, ATF4与突触可塑性和学习记忆密切相关,其在神经退行性变、脑损伤和药物成瘾等疾病中扮演重要角色,有必要深入理解ATF4在学习记忆障碍相关疾病中发挥的作用,为相关疾病的治疗提供新靶点。     

突触的可塑性与学习,记忆机制

位于哺乳动物海马、小脑皮层的不同类型的可塑性突触,分别具有突触传递的长时程强化(LTP)或抑制(LTD)现象,它们可能是某些经典条件反射形成的基础。以LTD型突触为记忆装置的小脑局部神经网络,具有典型的适应控制能力。突触可塑性的另一类表现是突触前纤维长芽,有证据表明,伴随大脑—红核系统条件反射的建立,在红核神经元胞体附近有新的突触形成,这可能是长期记忆的基础。     

多巴胺调节海马神经元可塑性的研究进展

多巴胺是脑内重要的信息传递物质,不仅可以作为递质释放到前额叶、伏隔核等脑区,直接进行信息传递,也可以作为调质调节其它突触递质的传递,并影响神经元可塑性。海马参与构成边缘系统,受多巴胺能神经支配,执行着有关学习记忆以及空间定位的功能。海马神经元的可塑性是学习记忆的细胞分子基础。研究表明,多巴胺对海马神经元的突触可塑性和兴奋性可塑性都具有重要的调节作用。本文扼要综述多巴胺对海马神经元突触可塑性和兴奋性可塑性的调节机制的研究进展,以期为DA系统参与海马区学习记忆功能的研究提供新思路,更深入地了解学习记忆的神经机制。     

神经细胞粘附分子与记忆

记忆的形成阶段包含着神经元突触的可塑性变化过程.近年来的研究表明,神经细胞粘附分子可同时增进突触的可塑性和维持突触结构的稳定性.许多研究证实神经细胞粘附分子对与学习和记忆相关的过程起着一定的调节作用.     

与长时程增强相关的基因表达的研究进展

长地程增强（long-term potentiation,LTP)现象在细胞水平和分子水平反映突触的可塑性,它被认为是记忆过程中神经元活动的客观电生理指标。对其机制的研究表明,伴随着LTP的产生,有基因表达和蛋白质成分的改变。揭开LTP形成过程中所伴随的基因表达的改变,也许是探讨LTP形成机制的关键。     

非常规肌球蛋白与突触可塑性

突触可塑性是学习记忆的基础,其分子机制是理解记忆形成和维持的关键,也为神经退行性疾病的预防与治疗提供了新靶点。肌球蛋白超家族广泛存在于人体各种组织细胞中,主要分为常规肌球蛋白和非常规肌球蛋白。越来越多的研究发现,非常规肌球蛋白参与了许多重要的生命活动,尤其是在神经系统对突触可塑性的调节中,起到了十分重要的作用。     

表观遗传修饰在学习记忆中的研究进展

学习记忆是大脑的重要功能.记忆的形成涉及基因转录、新蛋白质合成和突触可塑性改变等一系列分子和细胞乃至神经环路的变化.近些年研究者逐渐发现各种表观遗传修饰,包括DNA甲基化、组蛋白修饰及RNA修饰在各种学习记忆类型、记忆阶段和突触可塑性中发挥了不同程度的作用.本文阐述了参与学习记忆的不同表观遗传调控因子,为进一步理解学习...     

突触长时程增强形成与学习记忆的相关研究

突触长时程增强(LTP)的形成与学习记忆有相似特征,将其作为记忆的一种模式加以研究,并深入探索LTP机制产生与静止突触的关系,长时程突触修饰与突触后神经细胞内Ca^2 的作用机制,学习行为后海马内出现的突触效能变化与行为学习之间的关系,以及BDNF对海马突触的LTP调节与长时记忆所涉及关于LTP的相关基因表达。     

Cholinergic Neurotransmission and Synaptic Plasticity Concerning Memory Processing

The brain is able to change the synaptic strength in response to stimuli that leave a memory trace. Long-term potentiation (LTP) and long-term depression (LTD) are forms of activity-dependent synaptic plasticity proposed to underlie memory. The induction of LTP appears mediated by glutamate acting on AMPA and then on NMDA receptors. Cholinergic muscarinic agonists facilitate learning and memory. Acetylcholine depolarizes pyramidal neurons, reduces inhibition, upregulates NMDA channels and activates the phosphoinositide cascade. Postsynaptic Ca²⁺ rises and stimulates Ca-dependent PK, promoting synaptic changes. Electroencephalographic desynchronization and hippocampal theta rhythm are related to learning and memory, are inducible by Cholinergic agonists and elicited by hippocampal Cholinergic terminals. Their loss results in memory deficits. Hence, Cholinergic pathways may act synergically with glutamatergic transmission, regulating and leading to synaptic plasticity. The stimulation that induces plasticity in vivo has not been established. The patterns for LTP/LTD induction in vitro may be due to the loss of ascending Cholinergic inputs. As a rat explores pyramidal cells fire bursts that could be relevant to plasticity.     

神经胶质细胞与突触可塑性研究新进展

突触的可塑性是研究学习与记忆的基础,很长时间以来人们对突触的可塑性研究主要集中在神经元和突触上;而胶质细胞的作用较少受到注意。最近的研究发现胶质细胞也参与突触的构成并影响突触的活动。研究表明中枢神经系统中的胶质细胞包括星形胶质细胞、小胶质细胞和少突胶质细胞可分别通过谷氨酸、丝氨酸、甘氨酸、ATP等信号调节突触的可塑性,从而为突触的可塑性研究提供了新的思路和方向,并有助于阐明突触的发生以及学习与记忆的机制。     

A Review of Aspects of Synaptic Plasticity in Hippocampus via mT Extremely Low-Frequency Magnetic Fields

The subthreshold magnetic modulation technique stimulates cells with mT extremely low-frequency magnetic fields (ELF-MFs), which are insufficient to induce neuronal action potentials. Although they cannot directly induce resting neurons to discharge, mT magnetic stimulation can regulate the excitability of the nervous system, which regulates learning and memory by some unknown mechanisms. Herein, we describe the regulation of mT ELF-MFs with different parameters on synaptic plasticity in hippocampal neurons. Additionally, we summarize the latest research on the possible mechanism of the effect of ELF-MFs on synaptic plasticity. Some studies have shown that ELF-MFs are able to inhibit long-term potentiation (LTP) by increasing concentration of intracellular Ca²⁺ concentration ([Ca²⁺]_i), as well as concentration of reactive oxygen species. The research in this paper has significance for the comprehensive understanding of relevant neurological mechanisms of learning and memory by mT ELF-MFs stimulation. However, more high-quality research is necessary to determine the regulatory mechanism of mT ELF-MFs on synaptic plasticity in order to optimize this technique as a treatment for neurological diseases. © 2023 Bioelectromagnetics Society.     

A critical role for the glial-derived neuromodulator D-serine in the age-related deficits of cellular mechanisms of learning and memory

Age-associated deficits in learning and memory are closely correlated with impairments of synaptic plasticity. Analysis of N-methyl-D-aspartate receptor (NMDAr)-dependent long-term potentiation (LTP) in CA1 hippocampal slices indicates that the glial-derived neuromodulator D-serine is required for the induction of synaptic plasticity. During aging, the content of D-serine and the expression of its synthesizing enzyme serine racemase are significantly decreased in the hippocampus. Impaired LTP and NMDAr-mediated synaptic potentials in old rats are rescued by exogenous D-serine. These results highlight the critical role of glial cells and presumably astrocytes, through the availability of D-serine, in the deficits of synaptic mechanisms of learning and memory that occur in the course of aging.     

Characterizing spine issues: If offers novel therapeutics to Angelman syndrome

Angelman syndrome (AS) is a rare neurodevelopmental disorder characterized by severe mental retardation, microcephaly, speech impairment, frequent epilepsy, EEG abnormalities, ataxic movements, tongue protrusion, bursts of laughter, sleep abruptions, and hyperactivity. AS results from loss of function of the imprinted UBE3A (ubiquitin‐protein ligase E3A) gene on chromosome 15q11–q13, including a mutation on the maternal allele of Ube3a, a large deletion of the maternally inherited chromosomal region 15q11–13, paternal uniparental disomy of chromosome 15q11–13, or an imprinting defect. The Ube3a maternal deleted mouse model recaptured the major phenotypes of AS patients include seizure, learning and memory impairments, sleep disturbance, and motor problems. Owing to the activity‐dependent structural and functional plasticity, dendritic spines are believed as the basic subcellular compartment for learning and memory and the sites where LTP and LTD are induced. Defects of spine formation and dynamics are common among several neurodevelopmental disorders and neuropsychiatric disorders including AS and reflect the underlying synaptopathology, which drives clinically relevant behavioral deficits. This review will summarize the impaired spine density, morphology, and synaptic plasticity in AS and propose that future explorations on spine dynamics and synaptic plasticity may help develop novel interventions and therapy for neurodevelopmental disorders like AS.     

The making of a memory mechanism

Long-Term Potentiation (LTP) is akind of synaptic plasticity that manycontemporary neuroscientists believe is acomponent in mechanisms of memory. This essaydescribes the discovery of LTP and thedevelopment of the LTP research program. Thestory begins in the 1950's with the discoveryof synaptic plasticity in the hippocampus (amedial temporal lobe structure now associatedwith memory), and it ends in 1973 with thepublication of three papers sketching thefuture course of the LTP research program. Themaking of LTP was a protracted affair.Hippocampal synaptic plasticity was initiallyencountered as an experimental tool, thenreported as a curiosity, and finally includedin the ontic store of the neurosciences. Earlyresearchers were not investigating thehippocampus in search of a memory mechanism;rather, they saw the hippocampus as a usefulexperimental model or as a structure implicatedin the etiology of epilepsy. The link betweenhippocampal synaptic plasticity and learning ormemory was a separate conceptual achievement.That link was formulated in at least threedifferent ways at different times: reductively(claiming that plasticity is identical tolearning), analogically (claiming thatplasticity is an example or model of learning),and mechanistically (claiming that plasticityis a component in learning or memorymechanisms). The hypothesized link withlearning or memory, coupled with developmentsin experimental techniques and preparations,shaped how researchers understood LTP itself.By 1973, the mechanistic formulation of thelink between LTP and memory provided anabstract framework around which findings frommultiple perspectives could be integrated intoa multifield research program.     

Increase in proportion of hippocampal spine synapses expressing neural cell adhesion molecule NCAM180 following long-term potentiation

Neural recognition molecules such as the neural cell adhesion molecule (NCAM) have been implicated in synaptic plasticity, including long-term potentiation (LTP), sensitization, and learning and memory. The major isoform of NCAM carrying the longest cytoplasmic domain of all NCAM isoforms (NCAM180) is predominantly localized in postsynaptic membranes and postsynaptic densities of hippocampal neurons, with only a proportion of synapses carrying detectable levels of NCAM180. To investigate whether this differential expression of NCAM180 may correlate with distinct states of synaptic activity, LTP was induced by high-frequency stimulation of the perforant path and the percentage of NCAM180 immunopositive spine synapses determined in the outer third of the dentate molecular layer of the dentate gyrus by immunoelectron microscopy. Twenty-four hours following induction of LTP by high-frequency stimulation, the percentage of spine synapses expressing NCAM180 increases from 37% (passive control) to 70%. This increase was inhibited by the noncompetitive N-methyl-D -aspartate receptor antagonist MK801. Following repeated LTP induction at 10 consecutive days with one tetanization each day, 60% of all spine synapses were NCAM180 immunoreactive. Compared to passive control animals, the percentage of NCAM180 expressing synapses in low-frequency stimulated animals decreased from 37% to 28%. Spine synapses in the inner part of the dentate molecular layer not contacted by the afferents of the perforant path did not change the percentage of NCAM180-expressing synapses. The results obtained by the postembedding immunogold staining technique confirmed the difference in NCAM180 expression of spine synapses between passive control and potentiated animals. These observations suggest a role for NCAM180 in synaptic remodeling accompanying LTP. © 1998 John Wiley & Sons, Inc. J Neurobiol 37: 359–372, 1998