缺血性水肿早期脑液生理变化

IF 5.9 1区 医学 Q1 NEUROSCIENCES
Stephen B Hladky, Margery A Barrand
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引用次数: 0

摘要

当组织中积聚的溶质和水分超过正常量时,就会出现水肿。在脑实质组织中,血管源性水肿产生于血脑屏障通透性的变化,例如瘤周水肿。细胞毒性水肿源于细胞内溶质的过度积聚,如中风后的缺血性水肿。当受影响核心区域的血流量下降到足以剥夺脑细胞维持离子梯度所需的 ATP 时,就会引发这种类型的水肿。其结果是:神经元去极化;神经元吸收 Na+ 和 Cl-,失去 K+;神经元肿胀;星形胶质细胞吸收 Na+、K+ 和阴离子;星形胶质细胞肿胀;神经元和星形胶质细胞吸收液体导致 ISF 容量减少。由于新陈代谢产生渗透溶质以及 CSF 和血液中溶质的流入,实质溶质含量增加。大大增加的[K+]isf 会引发向周围半影扩散的去极化,增加代谢负荷,导致缺血核心增大。水主要从血液进入实质组织,其中一些通过 AQP4 进入星形胶质细胞内膜。在中期,例如三小时后,随着血脑屏障内皮细胞间紧密连接的部分打开以及 SUR1-TPRM4 通道的打开,NaCl 渗透性和肿胀率增加。然后,溶胀由唐南效应驱动。长此以往,血脑屏障会出现严重破坏。水肿消退的速度比水肿形成的速度慢。不含胶体的液体,如注入的模拟 CSF,可通过类似斯塔林的机制穿过血脑屏障被重吸收,而注入的含有胶体的血清则必须通过更缓慢的血管外途径排出。大面积水肿会使颅内压(ICP)升高,足以导致致命的脑疝。通过颅骨切除术或抽吸渗透压活跃的梗死区域,可以避免 ICP 的潜在致命性升高。然而,唯一能令人满意地保持功能的治疗方法是恢复血流,前提是能较快地实现。目前研究的一个重要目标是找到能延长再灌注成功时间的治疗方法。本文讨论了仍有待解决的问题。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Alterations in brain fluid physiology during the early stages of development of ischaemic oedema.

Oedema occurs when higher than normal amounts of solutes and water accumulate in tissues. In brain parenchymal tissue, vasogenic oedema arises from changes in blood-brain barrier permeability, e.g. in peritumoral oedema. Cytotoxic oedema arises from excess accumulation of solutes within cells, e.g. ischaemic oedema following stroke. This type of oedema is initiated when blood flow in the affected core region falls sufficiently to deprive brain cells of the ATP needed to maintain ion gradients. As a consequence, there is: depolarization of neurons; neural uptake of Na+ and Cl- and loss of K+; neuronal swelling; astrocytic uptake of Na+, K+ and anions; swelling of astrocytes; and reduction in ISF volume by fluid uptake into neurons and astrocytes. There is increased parenchymal solute content due to metabolic osmolyte production and solute influx from CSF and blood. The greatly increased [K+]isf triggers spreading depolarizations into the surrounding penumbra increasing metabolic load leading to increased size of the ischaemic core. Water enters the parenchyma primarily from blood, some passing into astrocyte endfeet via AQP4. In the medium term, e.g. after three hours, NaCl permeability and swelling rate increase with partial opening of tight junctions between blood-brain barrier endothelial cells and opening of SUR1-TPRM4 channels. Swelling is then driven by a Donnan-like effect. Longer term, there is gross failure of the blood-brain barrier. Oedema resolution is slower than its formation. Fluids without colloid, e.g. infused mock CSF, can be reabsorbed across the blood-brain barrier by a Starling-like mechanism whereas infused serum with its colloids must be removed by even slower extravascular means. Large scale oedema can increase intracranial pressure (ICP) sufficiently to cause fatal brain herniation. The potentially lethal increase in ICP can be avoided by craniectomy or by aspiration of the osmotically active infarcted region. However, the only satisfactory treatment resulting in retention of function is restoration of blood flow, providing this can be achieved relatively quickly. One important objective of current research is to find treatments that increase the time during which reperfusion is successful. Questions still to be resolved are discussed.

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来源期刊
Fluids and Barriers of the CNS
Fluids and Barriers of the CNS Neuroscience-Developmental Neuroscience
CiteScore
10.70
自引率
8.20%
发文量
94
审稿时长
14 weeks
期刊介绍: "Fluids and Barriers of the CNS" is a scholarly open access journal that specializes in the intricate world of the central nervous system's fluids and barriers, which are pivotal for the health and well-being of the human body. This journal is a peer-reviewed platform that welcomes research manuscripts exploring the full spectrum of CNS fluids and barriers, with a particular focus on their roles in both health and disease. At the heart of this journal's interest is the cerebrospinal fluid (CSF), a vital fluid that circulates within the brain and spinal cord, playing a multifaceted role in the normal functioning of the brain and in various neurological conditions. The journal delves into the composition, circulation, and absorption of CSF, as well as its relationship with the parenchymal interstitial fluid and the neurovascular unit at the blood-brain barrier (BBB).
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