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在早产儿中,脑室内出血会导致脑血管痉挛及相关神经功能障碍:血红素诱导炎性小体介导的白细胞介素-1生成及一氧化氮耗竭。

In Premature Newborns Intraventricular Hemorrhage Causes Cerebral Vasospasm and Associated Neurodisability Heme-Induced Inflammasome-Mediated Interleukin-1 Production and Nitric Oxide Depletion.

作者信息

Eisenhut Michael, Choudhury Samyami

机构信息

Pediatric Department, Luton and Dunstable University Hospital NHS Foundation Trust, Luton, Bedfordshire, United Kingdom.

出版信息

Front Neurol. 2017 Aug 18;8:423. doi: 10.3389/fneur.2017.00423. eCollection 2017.

Abstract

BACKGROUND

Intraventricular hemorrhage (IVH) occurs in 60-70% of neonates weighing 500-750 g and 10-20% of those weighing 1,000-1,500 g. All forms of IVH have been associated with neurocognitive deficits. Both subarachnoid and IVHs have been associated with delayed vasospasm leading to neurological deficits. Pathways linking hemoglobin release from blood clots to vasospasm include heme-induced activation of inflammasomes releasing interleukin-1 (IL-1) that can cause calcium dependent and independent vasospasm. Free hemoglobin is a potent scavenger of nitric oxide (NO). Depletion of NO, a potent endogenous vasodilator, has been associated with features of vasospasm.

HYPOTHESIS

In premature newborns, IVH causes cerebral vasospasm and associated neurodisability heme-induced increased inflammasome-mediated IL-1 production and NO depletion.

CONFIRMATION OF HYPOTHESIS AND IMPLICATIONS

This hypothesis could be confirmed in the IVH animal model with visualization of any associated vasospasm by angiography and in newborns with IVH by transcranial Doppler ultrasonography and correlation with cerebrospinal fluid IL-1 and NO metabolite levels. Confirmation of the role of heme in activation of inflammasomes causing IL-1 production and NO binding could be achieved by measuring the effect of heme scavenging interventions on IL-1 levels and levels of NO metabolites. In addition to removal of the accumulated blood of an IVH by drainage, irrigation, and fibrinolytic therapy intrathecal application of vasodilators and heme scavenging agents like haptoglobin and haemopexin and systemic treatment with inhibitors of inflammasomes like telmisartan could be used to prevent and treat cerebral vasospasm, and thus reduce the risk of associated brain injury in premature neonates.

摘要

背景

体重500 - 750克的新生儿中,60 - 70%会发生脑室内出血(IVH),体重1000 - 1500克的新生儿中,10 - 20%会发生IVH。所有形式的IVH都与神经认知缺陷有关。蛛网膜下腔出血和IVH均与导致神经功能缺损的延迟性血管痉挛有关。将血凝块中血红蛋白释放与血管痉挛联系起来的途径包括血红素诱导炎性小体激活,释放白细胞介素-1(IL-1),其可导致钙依赖性和非依赖性血管痉挛。游离血红蛋白是一氧化氮(NO)的强效清除剂。NO作为一种强效内源性血管舒张剂,其消耗与血管痉挛的特征有关。

假说

在早产新生儿中,IVH通过血红素诱导炎性小体介导的IL-1生成增加和NO消耗导致脑血管痉挛及相关神经功能障碍。

假说的证实及意义

该假说可在IVH动物模型中通过血管造影观察任何相关的血管痉挛来证实,在患有IVH的新生儿中通过经颅多普勒超声检查并与脑脊液IL-1和NO代谢物水平进行相关性分析来证实。通过测量血红素清除干预对IL-1水平和NO代谢物水平的影响,可证实血红素在激活炎性小体导致IL-1生成和NO结合中的作用。除了通过引流、冲洗和纤溶疗法清除IVH积聚的血液外,鞘内应用血管舒张剂和血红素清除剂(如触珠蛋白和血红素结合蛋白)以及用替米沙坦等炎性小体抑制剂进行全身治疗,可用于预防和治疗脑血管痉挛,从而降低早产新生儿相关脑损伤的风险。

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