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神经炎症作为蛛网膜下腔出血的干预靶点

Neuroinflammation as a Target for Intervention in Subarachnoid Hemorrhage.

作者信息

de Oliveira Manoel Airton Leonardo, Macdonald R Loch

机构信息

Adult Critical Care Unit, Hospital Paulistano - United Health Group, São Paulo, Brazil.

Keenan Research Center for Biomedical Science, Department of Surgery, Li Ka Shing Knowledge Institute, University of Toronto, Toronto, ON, Canada.

出版信息

Front Neurol. 2018 May 2;9:292. doi: 10.3389/fneur.2018.00292. eCollection 2018.

Abstract

Aneurysmal subarachnoid hemorrhage (SAH) is a sub-type of hemorrhagic stroke associated with the highest rates of mortality and long-term neurological disabilities. Despite the improvement in the management of SAH patients and the reduction in case fatality in the last decades, disability and mortality remain high in this population. Brain injury can occur immediately and in the first days after SAH. This early brain injury can be due to physical effects on the brain such as increased intracranial pressure, herniations, intracerebral, intraventricular hemorrhage, and hydrocephalus. After the first 3 days, angiographic cerebral vasospasm (ACV) is a common neurological complication that in severe cases can lead to delayed cerebral ischemia and cerebral infarction. Consequently, the prevention and treatment of ACV continue to be a major goal. However, most treatments for ACV are vasodilators since ACV is due to arterial vasoconstriction. Other targets also have included those directed at the underlying biochemical mechanisms of brain injury such as inflammation and either independently or as a consequence, cerebral microthrombosis, cortical spreading ischemia, blood-brain barrier breakdown, and cerebral ischemia. Unfortunately, no pharmacologic treatment directed at these processes has yet shown efficacy in SAH. Enteral nimodipine and the endovascular treatment of the culprit aneurysm, remain the only treatment options supported by evidence from randomized clinical trials to improve patients' outcome. Currently, there is no intervention directly developed and approved to target neuroinflammation after SAH. The goal of this review is to provide an overview on anti-inflammatory drugs tested after aneurysmal SAH.

摘要

动脉瘤性蛛网膜下腔出血(SAH)是出血性卒中的一种亚型,其死亡率和长期神经功能障碍发生率最高。尽管在过去几十年中SAH患者的管理有所改善,病死率有所降低,但该人群的残疾率和死亡率仍然很高。SAH后,脑损伤可立即发生,并在最初几天内出现。这种早期脑损伤可能是由于对大脑的物理影响,如颅内压升高、脑疝、脑内、脑室内出血和脑积水。在最初3天后,血管造影性脑血管痉挛(ACV)是一种常见的神经并发症,在严重情况下可导致迟发性脑缺血和脑梗死。因此,ACV的预防和治疗仍然是一个主要目标。然而,由于ACV是由动脉血管收缩引起的,大多数治疗ACV的药物都是血管扩张剂。其他靶点还包括针对脑损伤潜在生化机制的靶点,如炎症以及独立或作为其结果的脑微血栓形成、皮质扩散性缺血、血脑屏障破坏和脑缺血。不幸的是,针对这些过程的药物治疗在SAH中尚未显示出疗效。肠内给予尼莫地平和对责任动脉瘤进行血管内治疗,仍然是随机临床试验证据支持的、可改善患者预后的唯一治疗选择。目前,尚无直接针对SAH后神经炎症开发并获批的干预措施。本综述的目的是概述动脉瘤性SAH后测试的抗炎药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2ddf/5941982/aa89e9f54d5b/fneur-09-00292-g001.jpg

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