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神经瘤中巨噬细胞的分布及轴突关系

Distribution and axonal relations of macrophages in a neuroma.

作者信息

Frisén J, Risling M, Fried K

机构信息

Department of Neuroscience and Anatomy, Karolinska Institutet, Stockholm, Sweden.

出版信息

Neuroscience. 1993 Aug;55(4):1003-13. doi: 10.1016/0306-4522(93)90314-6.

Abstract

After axotomy in the peripheral nervous system, most axons regrow and re-establish contact with their targets. Depending on the type of lesion, a varying number of nerve fibers fail to regenerate and terminate far from the target, forming a neuroma. Sensory axons trapped in a neuroma show abnormal sensitivity to various stimuli, and often fire spontaneously. In this study we have examined the distribution and axonal relations of macrophages in rat sciatic neuromas three days to one year after cutting and ligating the nerve. ED1-immunoreactive macrophages migrated into the neuroma in large numbers within the two first weeks after the injury. Most cells were at that time located 0.5-1 mm proximal to the ligature. From three weeks on, a majority of the ED1-immunoreactive cells contained numerous large vacuoles filled with myelin fragments. At sites of focal demyelination, macrophages often had direct contact with axonal membranes. At later survival stages (three months to one year) ED1-immunoreactive cells were seen not only in the area just proximal to the ligature, but also several millimeters proximal to this. Macrophages persisted in considerable numbers in the neuroma for at least one year. These data suggest that neuroma macrophages may participate in the genesis of electrophysiological abnormalities thought to underly chronic pain after neuroma formation, possibly by creating demyelinated axonal regions susceptible to external stimuli from e.g. neighboring nerve fibers, by releasing substances which influence regeneration and remodelling of axonal growth cones, or by direct actions on the denuded axonal membranes.

摘要

在周围神经系统轴突切断后,大多数轴突会再生并重新与它们的靶标建立联系。根据损伤类型的不同,数量不等的神经纤维无法再生,并在远离靶标的位置终止,形成神经瘤。被困在神经瘤中的感觉轴突对各种刺激表现出异常的敏感性,并且常常自发放电。在本研究中,我们检查了大鼠坐骨神经瘤在切断和结扎神经后三天至一年期间巨噬细胞的分布及轴突关系。ED1免疫反应性巨噬细胞在损伤后的头两周内大量迁移至神经瘤中。此时大多数细胞位于结扎部位近端0.5 - 1毫米处。从三周开始,大多数ED1免疫反应性细胞含有大量充满髓鞘碎片的大液泡。在局灶性脱髓鞘部位,巨噬细胞常常与轴突膜直接接触。在后期存活阶段(三个月至一年),不仅在结扎部位近端的区域可见ED1免疫反应性细胞,在该部位近端几毫米处也可见到。巨噬细胞在神经瘤中大量持续存在至少一年。这些数据表明,神经瘤巨噬细胞可能参与了被认为是神经瘤形成后慢性疼痛基础的电生理异常的发生过程,可能是通过形成易受例如相邻神经纤维外部刺激影响的脱髓鞘轴突区域、释放影响轴突生长锥再生和重塑的物质,或直接作用于裸露的轴突膜来实现的。

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