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用于治疗人类缺血/再灌注损伤的一氧化氮供体药物:系统评价。

Nitric oxide donor agents for the treatment of ischemia/reperfusion injury in human subjects: a systematic review.

机构信息

Department of Emergency Medicine, Cooper University Hospital, Camden, NJ 08103, USA.

出版信息

Shock. 2013 Mar;39(3):229-39. doi: 10.1097/SHK.0b013e31827f565b.

DOI:10.1097/SHK.0b013e31827f565b
PMID:23358103
Abstract

In animal models, administration of nitric oxide (NO) donor agents has been shown to reduce ischemia/reperfusion (I/R) injury. Our aim was to systematically analyze the biomedical literature to determine the effects of NO-donor agent administration on I/R injury in human subjects. We hypothesized that NO-donor agents reduce I/R injury. We performed a search of Cochrane Library, PubMed, CINAHL, conference proceedings, and other sources with no restriction to language using a comprehensive strategy. Study inclusion criteria were as follows: (a) human subjects, (b) documented periods of ischemia and reperfusion, (c) treatment arm composed of NO-donor agent administration, and (d) use of a control arm. We excluded secondary reports, reviews, correspondence, and editorials. We performed a qualitative analysis to collate and summarize treatment effects according to the recommended methodology from the Cochrane Handbook. Twenty-six studies involving multiple etiologies of I/R injury (10 cardiopulmonary bypass, six organ transplant, seven myocardial infarction, three limb tourniquet) met all inclusion and no exclusion criteria. Six (23%) of 26 were considered high-quality studies as per the Cochrane criteria for assessing risk of bias. In 20 (77%) of 26 studies and four (67%) of six high-quality studies, patients treated with NO-donor agents experienced reduced I/R injury compared with controls. Zero clinical studies to date have tested NO-donor agent administration in patients with cerebral I/R injury (e.g., cardiac arrest, stroke). Despite a paucity of high-quality clinical investigations, the preponderance of evidence to date suggests that administration of NO-donor agents may be an effective treatment for I/R injury in human subjects.

摘要

在动物模型中,给予一氧化氮(NO)供体药物已被证明可减轻缺血/再灌注(I/R)损伤。我们的目的是系统地分析生物医学文献,以确定 NO 供体药物在人体 I/R 损伤中的作用。我们假设 NO 供体药物可减轻 I/R 损伤。我们使用全面的策略,在没有语言限制的情况下,对 Cochrane 图书馆、PubMed、CINAHL、会议记录和其他来源进行了搜索。研究纳入标准如下:(a)人体,(b)记录的缺血和再灌注期,(c)治疗组由 NO 供体药物给药组成,(d)使用对照组。我们排除了次要报告、综述、信件和社论。我们根据 Cochrane 手册推荐的方法进行了定性分析,以整理和总结治疗效果。26 项研究涉及多种 I/R 损伤的病因(10 例心肺旁路、6 例器官移植、7 例心肌梗死、3 例四肢止血带)均符合所有纳入标准且无排除标准。根据评估偏倚风险的 Cochrane 标准,26 项研究中有 6 项(23%)被认为是高质量研究。在 26 项研究中的 20 项(77%)和 6 项高质量研究中的 4 项(67%)中,与对照组相比,接受 NO 供体药物治疗的患者的 I/R 损伤减轻。迄今为止,尚无临床研究测试过在患有脑 I/R 损伤(如心脏骤停、中风)的患者中给予 NO 供体药物。尽管高质量的临床研究很少,但迄今为止的大量证据表明,给予 NO 供体药物可能是治疗人体 I/R 损伤的有效方法。

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