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首页> 外文期刊>Fluids and Barriers of the CNS >Tunneling nanotubes evoke pericyte/endothelial communication during normal and tumoral angiogenesis
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Tunneling nanotubes evoke pericyte/endothelial communication during normal and tumoral angiogenesis

机译:隧道纳米管在正常和肿瘤血管生成过程中引起周细胞/内皮通讯

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Nanotubular structures, denoted tunneling nanotubes (TNTs) have been described in recent times as involved in cell-to-cell communication between distant cells. Nevertheless, TNT-like, long filopodial processes had already been described in the last century as connecting facing, growing microvessels during the process of cerebral cortex vascularization and collateralization. Here we have investigated the possible presence and the cellular origin of TNTs during normal brain vascularization and also in highly vascularized brain tumors. We searched for TNTs by high-resolution immunofluorescence confocal microscopy, applied to the analysis of 20-μm, thick sections from lightly fixed, unembedded samples of both developing cerebral cortex and human glioblastoma (GB), immunolabeled for endothelial, pericyte, and astrocyte markers, and vessel basal lamina molecules. The results revealed the existence of pericyte-derived TNTs, labeled by proteoglycan NG2/CSPG4 and CD146. In agreement with the described heterogeneity of these nanostructures, ultra-long (?300?μm) and very thin (?0.8 μm) TNTs were observed to bridge the gap between the wall of distant vessels, or were detected as short (?300?μm) bridging cables connecting a vessel sprout with its facing vessel or two apposed vessel sprouts. The pericyte origin of TNTs ex vivo in fetal cortex and GB was confirmed by in vitro analysis of brain pericytes, which were able to form and remained connected by typical TNT structures. None of the multiple roles described for TNTs can be excluded from a possible involvement during the processes of both normal and pathological vessel growth. A possible function, suggested by the pioneering studies made during cerebral cortex vascularization, is in cell searching and cell-to-cell recognition during the processes of vessel collateralization and vascular network formation. According to our results, it is definitely the pericyte-derived TNTs that seem to actively explore the surrounding microenvironment, searching for (site-to-site recognition), and connecting with (pericyte-to-pericyte and/or pericyte-to-endothelial cell communication), the targeted vessels. This idea implies that TNTs may have a primary role in the very early phases of both physiological and tumor angiogenesis in the brain.
机译:近来已经描述了纳米管结构,表示为隧穿纳米管(TNT),其涉及远距离细胞之间的细胞间通信。然而,在上个世纪,已经描述了TNT样的长丝状过程,将大脑皮层血管化和抵押过程中正在生长的微血管连接起来。在这里,我们研究了正常脑血管化过程中以及高度血管化脑肿瘤中TNT的可能存在和细胞起源。我们通过高分辨率的免疫荧光共聚焦显微镜搜索了TNTs,用于分析发育中的大脑皮层和人胶质母细胞瘤(GB)的轻度固定,未包埋的样品中的20μm厚切片,并对其进行了内皮,周细胞和星形胶质细胞标记物的免疫标记和血管基底膜分子。结果表明存在周细胞衍生的TNT,其被蛋白聚糖NG2 / CSPG4和CD146标记。与所描述的这些纳米结构的异质性相一致,观察到超长(>?300?μm)和非常薄(<?0.8μm)的TNT弥合了远处血管壁之间的间隙,或被检测为短(< 300微米(μm)的桥接电缆,将一个容器发芽与其面对的容器或两个并置的容器发芽连接起来。通过体外分析脑周细胞证实了TNTs在胎儿皮质和GB中的周细胞起源,后者能够形成并通过典型的TNT结构保持连接。在正常和病理性血管生长过程中,都不能排除TNT所描述的多种作用。在大脑皮层血管化过程中进行的开创性研究表明,可能的功能是在血管抵押和血管网络形成过程中的细胞搜索和细胞间识别。根据我们的结果,肯定是周细胞来源的TNT似乎在积极探索周围的微环境,寻找(位点识别)并与(周细胞到周细胞和/或周细胞到内皮)连接。细胞通讯),目标血管。这个想法暗示,TNT可能在大脑的生理和肿瘤血管生成的早期阶段都起主要作用。

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