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尿酸:跨越临床前和人体数据的脑保护转化之旅。

Uric Acid: A Translational Journey in Cerebroprotection That Spanned Preclinical and Human Data.

机构信息

From the Department of Neurology (E.L., A.C.), and Departments of Neurosurgery & Epidemiology (E.L.), University of Iowa, Iowa City; Institute of Biomedical Research of Barcelona (IIBB) (A.M.P.), Spanish National Research Council (CSIC); August Pi i Sunyer Biomedical Research Institute (IDIBAPS) (A.M.P., A.C.), Barcelona, Spain; Department of Internal Medicine (A.K.C.), University of Iowa, Iowa City; and Hospital Clinic (A.C.), University of Barcelona, Spain.

出版信息

Neurology. 2023 Dec 4;101(23):1068-1074. doi: 10.1212/WNL.0000000000207825.

Abstract

Uric acid (UA) is a strong endogenous antioxidant that neutralizes the toxicity of peroxynitrite and other reactive species on the neurovascular unit generated during and after acute brain ischemia. The realization that a rapid reduction of UA levels during an acute ischemic stroke was associated with a worse stroke outcome paved the way to investigate the value of exogenous UA supplementation to counteract the progression of redox-mediated ischemic brain damage. The long translational journey for UA supplementation recently reached a critical milestone when the results of the multicenter NIH stroke preclinical assessment network (SPAN) were reported. In a novel preclinical paradigm, 6 treatment candidates including UA supplementation were selected and tested in 6 independent laboratories following predefined criteria and strict methodological rigor. UA supplementation was the only intervention in SPAN that exceeded the prespecified efficacy boundary with male and female animals, young mice, young rats, aging mice, obese mice, and spontaneously hypertensive rats. This unprecedented achievement will allow UA to undergo clinical testing in a pivotal clinical trial through a NIH StrokeNet thrombectomy endovascular platform created to assess new treatment strategies in patients treated with mechanical thrombectomy. UA is a particularly appealing adjuvant intervention for mechanical thrombectomy because it targets the microcirculatory hypoperfusion and oxidative stress that limits the efficacy of this therapy. This descriptive review aims to summarize the translational development of UA supplementation, highlighting those aspects that likely contributed to its success. It includes having a well-defined target and mechanism of action, and an approach that simultaneously integrated rigorous preclinical assessment, with epidemiologic and preliminary human intervention studies. Validation of the clinical value of UA supplementation in a pivotal trial would confirm the translational value of the SPAN paradigm in preclinical research.

摘要

尿酸(UA)是一种强大的内源性抗氧化剂,可中和神经血管单元中产生的过氧亚硝酸盐和其他活性物质的毒性,这些物质在急性脑缺血期间和之后产生。人们意识到,急性缺血性中风期间 UA 水平的快速降低与更严重的中风结果相关,这为研究外源性 UA 补充以抵消氧化还原介导的缺血性脑损伤的进展提供了价值。UA 补充的长期转化之旅最近达到了一个关键的里程碑,当时 NIH 中风临床前评估网络(SPAN)的多中心结果报告。在一个新的临床前范例中,根据预先确定的标准和严格的方法学严谨性,在 6 个独立的实验室中选择并测试了包括 UA 补充在内的 6 种治疗候选物。在 SPAN 中,UA 补充是唯一一种干预措施,它使雄性和雌性动物、年轻小鼠、年轻大鼠、衰老小鼠、肥胖小鼠和自发性高血压大鼠都超过了预先指定的疗效边界。这一前所未有的成就将使 UA 能够通过 NIH StrokeNet 取栓血管内平台进行临床试验,该平台旨在评估接受机械取栓治疗的患者的新治疗策略。UA 是机械取栓的一种特别有吸引力的辅助干预措施,因为它针对限制这种治疗效果的微循环灌注不足和氧化应激。本描述性综述旨在总结 UA 补充的转化发展,强调那些可能促成其成功的方面。它包括具有明确的目标和作用机制,以及一种同时整合严格的临床前评估、流行病学和初步人类干预研究的方法。在一项关键性试验中验证 UA 补充的临床价值将确认 SPAN 范式在临床前研究中的转化价值。

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