血管舒缩对中枢神经系统淋巴-淋巴偶联和溶质运输的影响

James R Goodman, Jeffrey J. Iliff
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引用次数: 24

摘要

尽管最近描述了脑膜淋巴管从脑间质和脑脊液(CSF)中排出溶质,但控制颅淋巴流出的生理因素仍未得到充分研究。与最近的研究结果一致,与醒着的动物相比,注射70 kD和2000 kD荧光示踪剂的成年小鼠皮质在麻醉后颈部淋巴引流明显受损(示踪剂分布在2.1±4.5%和23.7±15.8%的颈深淋巴结);然而,自由呼吸麻醉小鼠明显高碳酸血症和酸性(paCO2 = 64±8 mmHg;pH = 7.22±0.05)。机械通气使麻醉动物的动脉血气正常化,并恢复麻醉小鼠间质溶质的淋巴外排。实验性高碳酸血症阻断了淋巴实质内示踪剂的颈部淋巴外排。当将示踪剂注射到蛛网膜下腔CSF室时,高碳酸血症几乎消除了进入脑组织的淋巴内流,而淋巴引流没有明显改变。这些发现表明,间质溶质的颈部淋巴引流在一定程度上受淋巴csf -间质液交换上游变化的调节。此外,他们认为在研究淋巴交换和脑膜淋巴引流时维持生理血气值可能对确定这些过程的生理调节至关重要。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Vasomotor influences on glymphatic-lymphatic coupling and solute trafficking in the central nervous system
Despite the recent description of meningeal lymphatic vessels draining solutes from the brain interstitium and cerebrospinal fluid (CSF), the physiological factors governing cranial lymphatic efflux remain largely unexplored. In agreement with recent findings, cervical lymphatic drainage of 70 kD and 2000 kD fluorescent tracers injected into the adult mouse cortex was significantly impaired in the anesthetized compared to waking animals (tracer distribution across 2.1 ± 4.5% and 23.7 ± 15.8% of deep cervical lymph nodes, respectively); however, free-breathing anesthetized mice were markedly hypercapnic and acidemic (paCO2 = 64 ± 8 mmHg; pH = 7.22 ± 0.05). Mechanical ventilation normalized arterial blood gases in anesthetized animals, and rescued lymphatic efflux of interstitial solutes in anesthetized mice. Experimental hypercapnia blocked cervical lymphatic efflux of intraparenchymal tracers. When tracers were injected into the subarachnoid CSF compartment, glymphatic influx into brain tissue was virtually abolished by hypercapnia, while lymphatic drainage was not appreciably altered. These findings demonstrate that cervical lymphatic drainage of interstitial solutes is, in part, regulated by upstream changes in glymphatic CSF-interstitial fluid exchange. Further, they suggest that maintaining physiological blood gas values in studies of glymphatic exchange and meningeal lymphatic drainage may be critical to defining the physiological regulation of these processes.
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