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周围神经系统与中枢神经系统在对荧光素钠通透性方面的差异。

Differences between the peripheral and the central nervous system in permeability to sodium fluorescein.

作者信息

Malmgren L T, Olsson Y

出版信息

J Comp Neurol. 1980 May 1;191(1):103-7. doi: 10.1002/cne.901910106.

Abstract

Sodium fluorescein (SF) was used as a very small tracer (mol wt 376; 5 A diameter) to examine diffusion barriers in peripheral nerves and to compare them to those in other regions of the nervous system. The technique involved immobilization of the tracer by rapid freezing, followed by freeze-drying and vacuum embedding in paraffin. The localization of the SF was then determined in tissue secretions using fluorescence microscopy. Even at the highest doses of intravenously (IV) injected tracer, no extravasation could be detected in the cerebral cortex. On the other hand, SF penetrated very rapidly into peripheral ganglia and into the epineurium and perineurium of large peripheral nerves. The penetration of SF into the endoneurium of large nerves was, however, much more restricted with tracer detectable within the endoneurium only at high doses and long survival times. Even in such cases, the level of SF fluorescence was much lower within nerve fascicles than in the epineurium and the perineurium, and a sharp gradient in fluorescence intensity persisted at the inner border of the perineurium. The extent of extravasation into the endoneurium varied markedly betwen different fascicles of the same nerve and between different nerves in the same animal. Experiments involving injection of high doses of SF adjacent to the nerve indicated relatively little movement of SF across the perineurium, which indicates that the observed accumulation of tracer within the endoneurium was the result of direct extravasation of SF from the endoneural blood vessels. Small nerve branches (< 100 mu diameter) showed an earlier and more extensive penetration of SF into the endoneurium than large nerves like the sciatic, hypoglossal, or ventral tail nerve. This may be due to a diffusion of SF along the extracellular space of the endoneurium from nerve terminals where the perineurial barrier is open-ended. In experiments involving IV injection of a solution containing both green fluorescent SF and red fluorescent Evans Blue (Evans Blue-serum albumin conplex, EBA = mol wt. 69,000), the distribution of SF could be directly compared at various sites and sacrifice times to that of EBA, a much larger tracer. SF appeared more rapidly and extensively than EBA in the various compartments in ganglia and peripheral nerve. The distribution of EBA was the same as is typically seen when this tracer is injected alone, indicating that there was no change in vascular permeability associated with IV injection of SF. Since SF is of very small size, freely diffusible, nontoxic, and detectable at very low concentrations, it should be a useful complement to existing tracers. When tissues are processed according to the indicated procedure, one can obtain a very sensitive and reliable localization of this tracer which should be of value for studies in the nervous system concerning various pathological conditions associated with permeability alterations.

摘要

荧光素钠(SF)被用作一种非常小的示踪剂(分子量376;直径5埃),以研究周围神经中的扩散屏障,并将其与神经系统其他区域的扩散屏障进行比较。该技术包括通过快速冷冻固定示踪剂,然后进行冷冻干燥并真空包埋在石蜡中。然后使用荧光显微镜在组织分泌物中确定SF的定位。即使静脉注射(IV)示踪剂的剂量最高,在大脑皮层中也未检测到外渗。另一方面,SF非常迅速地渗透到外周神经节以及大型周围神经的神经外膜和神经束膜中。然而,SF渗透到大型神经的神经内膜的情况受到更多限制,只有在高剂量和长存活时间时才能在神经内膜内检测到示踪剂。即使在这种情况下,神经束内的SF荧光水平也比神经外膜和神经束膜中的低得多,并且在神经束膜的内边界处荧光强度持续存在明显的梯度。同一神经的不同神经束之间以及同一动物的不同神经之间,渗入神经内膜的外渗程度差异明显。涉及在神经附近注射高剂量SF的实验表明,SF穿过神经束膜的移动相对较少,这表明在神经内膜内观察到的示踪剂积累是SF从神经内膜血管直接外渗的结果。小神经分支(直径<100微米)比坐骨神经、舌下神经或尾腹神经等大型神经更早且更广泛地渗透到神经内膜中。这可能是由于SF沿着神经内膜的细胞外空间从神经束膜屏障开放的神经末梢扩散。在涉及静脉注射含有绿色荧光SF和红色荧光伊文思蓝(伊文思蓝 - 血清白蛋白复合物,EBA = 分子量69,000)的溶液的实验中,可以将SF在不同部位和处死时间的分布与EBA(一种大得多的示踪剂)的分布直接进行比较。在神经节和周围神经的各个隔室中,SF比EBA出现得更快且更广泛。EBA的分布与单独注射这种示踪剂时通常看到的相同,这表明静脉注射SF不会改变血管通透性。由于SF尺寸非常小、可自由扩散、无毒且在非常低的浓度下即可检测到,它应该是现有示踪剂的有用补充。当按照所示程序处理组织时,可以获得这种示踪剂非常敏感和可靠的定位,这对于研究神经系统中与通透性改变相关的各种病理状况应该是有价值的。

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