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由递质物质的胞吐作用和扩散释放介导的突触外神经传递。

Extrasynaptic Neurotransmission Mediated by Exocytosis and Diffusive Release of Transmitter Substances.

作者信息

Del-Bel Elaine, De-Miguel Francisco F

机构信息

Department of Morphology Physiology and Basic Pathology, Dental School of Ribeirão Preto, USP-Center for Interdisciplinary Research on Applied Neurosciences (NAPNA), University of São Paulo (USP), São Paulo, Brazil.

Instituto de Fisiología Celular-Neurociencias, Centro de Ciencias de la Complejidad, Universidad Nacional Autónoma de México, Mexico City, Mexico.

出版信息

Front Synaptic Neurosci. 2018 Jun 8;10:13. doi: 10.3389/fnsyn.2018.00013. eCollection 2018.

Abstract

This review article deals with the mechanisms of extrasynaptic release of transmitter substances, namely the release from the soma, axon and dendrites in the absence of postsynaptic counterparts. Extrasynaptic release occurs by exocytosis or diffusion. Spillover from the synaptic cleft also contributes to extrasynaptic neurotransmission. Here, we first describe two well-known examples of exocytosis from the neuronal soma, which may release copious amounts of transmitter for up to hundreds of seconds after electrical stimulation. The mechanisms for somatic exocytosis of the low molecular weight transmitter serotonin, and the peptides oxytocin and vasopressin have been studied in detail. Serotonin release from leech neurons and oxytocin and vasopressin from rodent neurons have a common multi-step mechanism, which is completely different from that for exocytosis from presynaptic endings. Most transmitters and peptides released extrasynaptically seem to follow this same mechanism. Extrasynaptic exocytosis may occur onto glial cells, which act as intermediaries for long-term and long-distance transmission. The second part of this review article focuses on the release upon synthesis of the representative diffusible molecules nitric oxide (NO) and endocannabinoids. Diffusible molecules are synthesized "on demand" from postsynaptic terminals in response to electrical activity and intracellular calcium elevations. Their effects include the retrograde modulation of presynaptic electrical activity and transmitter release. Extrasynaptic neurotransmission is well exemplified in the retina. Light-evoked extrasynaptic communication sets the gain for visual responses and integrates the activity of neurons, glia and blood vessels. Understanding how extrasynaptic communication changes the function of hard-wired circuits has become fundamental to understand the function of the nervous system.

摘要

这篇综述文章探讨了神经递质的突触外释放机制,即在没有突触后对应物的情况下,从胞体、轴突和树突释放递质的机制。突触外释放通过胞吐作用或扩散发生。突触间隙的递质溢出也有助于突触外神经传递。在这里,我们首先描述两个从神经元胞体进行胞吐作用的著名例子,电刺激后,胞体可能会在长达数百秒的时间内释放大量递质。低分子量递质5-羟色胺以及肽类催产素和加压素的胞体胞吐机制已得到详细研究。水蛭神经元释放5-羟色胺以及啮齿动物神经元释放催产素和加压素具有共同的多步骤机制,这与突触前末梢的胞吐机制完全不同。大多数突触外释放的递质和肽似乎都遵循相同的机制。突触外胞吐作用可能发生在胶质细胞上,胶质细胞充当长期和长距离传递的中介。这篇综述文章的第二部分重点关注代表性的可扩散分子一氧化氮(NO)和内源性大麻素合成时的释放。可扩散分子是突触后终末根据电活动和细胞内钙升高“按需”合成的。它们的作用包括对突触前电活动和递质释放的逆行调节。视网膜中很好地体现了突触外神经传递。光诱发的突触外通讯设定了视觉反应的增益,并整合了神经元、胶质细胞和血管的活动。了解突触外通讯如何改变硬连线电路的功能已成为理解神经系统功能的基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/c79d/6003215/981e0c4ee55c/fnsyn-10-00013-g0001.jpg

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