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How the stimulus defines the dynamics of vesicle pool recruitment, fusion mode, and vesicle recycling in neuroendocrine cells

期刊

JOURNAL OF NEUROCHEMISTRY
卷 137, 期 6, 页码 867-879

出版社

WILEY-BLACKWELL
DOI: 10.1111/jnc.13565

关键词

calcium; endocytosis; exocytosis; immediately releasable pool; kiss-and-run; secretion

资金

  1. Agencia Nacional de Promocion Cientifica y Tecnologica (Argentina) [PICT 0029-2010, PICT 0351-2012]
  2. CONICYT, Chile [ACT-1121]
  3. ICM-Chile [P09-022-F]
  4. Millennium Scientific Initiative

向作者/读者索取更多资源

The pattern of stimulation defines important characteristics of the secretory process in neurons and neuroendocrine cells, including the pool of secretory vesicles being recruited, the type and amount of transmitters released, the mode of membrane retrieval, and the mechanisms associated with vesicle replenishment. This review analyzes the mechanisms that regulate these processes in chromaffin cells, as well as in other neuroendocrine and neuronal models. A common factor in these mechanisms is the spatial and temporal distribution of the Ca2+ signal generated during cell stimulation. For instance, neurosecretory cells and neurons have pools of vesicles with different locations with respect to Ca2+ channels, and those pools are therefore differentially recruited following different patterns of stimulation. In this regard, a brief stimulus will induce the exocytosis of a small pool of vesicles that is highly coupled to voltage-dependent Ca2+ channels, whereas longer or more intense stimulation will provoke a global Ca2+ increase, promoting exocytosis irrespective of vesicle location. The pattern of stimulation, and therefore the characteristics of the Ca2+ signal generated by the stimulus also influence the mode of exocytosis and the type of endocytosis. Indeed, low-frequency stimulation favors kiss-and-run exocytosis and clathrin-independent fast endocytosis, whereas higher frequencies promote full fusion and clathrin-dependent endocytosis. This latter type of endocytosis is accelerated at high-frequency stimulation. Synaptotagmins, calcineurin, dynamin, complexin, and actin remodeling, appear to be involved in the mechanisms that determine the response of these processes to Ca2+.

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