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具有促存活作用的肽Y-P30增强多效营养蛋白与多功能蛋白聚糖-2和-3的结合,并支持其神经突生长活性。

The survival-promoting peptide Y-P30 enhances binding of pleiotrophin to syndecan-2 and -3 and supports its neuritogenic activity.

作者信息

Landgraf Peter, Wahle Petra, Pape Hans-Christian, Gundelfinger Eckart D, Kreutz Michael R

机构信息

Project Group Neuroplasticity, Leibniz Institute for Neurobiology, Brenneckestrasse 6, Magdeburg 39118, Germany.

出版信息

J Biol Chem. 2008 Sep 5;283(36):25036-45. doi: 10.1074/jbc.M800963200. Epub 2008 Jul 3.

Abstract

Y-P30 is a polypeptide produced by peripheral blood mononuclear cells of the maternal immune system during pregnancy. The peptide passes the blood-placenta barrier and accumulates in neurons of the developing infant brain, where it enhances survival of thalamic neurons and displays neuritogenic activities. In this study, we identify pleiotrophin (PTN) and syndecan-2 and -3 as direct binding partners of Y-P30. PTN is known to promote neurite outgrowth of thalamic neurons due to its association with the proteoglycan syndecan-3. Via spontaneous oligomerization Y-P30 can capture large macromolecular complexes containing PTN and potentially syndecans. Accordingly, the neuritogenic activity of Y-P30 in thalamic primary cultures requires the presence of PTN in the media and binding to syndecans. Thus, we propose that the neurite outgrowth promoting actions of Y-P30 during brain development are essentially based on its association with the PTN/syndecan signaling complex. This identifies a new mechanism of communication between the nervous and the immune system that might directly affect the wiring of the brain during development.

摘要

Y-P30是孕期母体免疫系统外周血单核细胞产生的一种多肽。该肽穿过血胎盘屏障并积聚在发育中婴儿大脑的神经元中,在那里它可提高丘脑神经元的存活率并表现出神经突生成活性。在本研究中,我们鉴定出多效生长因子(PTN)以及多功能蛋白聚糖-2和-3是Y-P30的直接结合伴侣。已知PTN因其与蛋白聚糖多功能蛋白聚糖-3的关联而促进丘脑神经元的神经突生长。通过自发寡聚化,Y-P30可捕获包含PTN以及可能还有多功能蛋白聚糖的大型大分子复合物。因此,Y-P30在丘脑原代培养物中的神经突生成活性需要培养基中存在PTN并与多功能蛋白聚糖结合。因此,我们提出Y-P30在大脑发育过程中促进神经突生长的作用主要基于其与PTN/多功能蛋白聚糖信号复合物的关联。这确定了神经和免疫系统之间一种新的通信机制,该机制可能在发育过程中直接影响大脑的神经连接。

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