Early Intravascular Events Are Associated with Development of Acute Respiratory Distress Syndrome. A Substudy of the LIPS-A Clinical Trial

机译：早期血管内事件与急性呼吸窘迫综合征的发展有关。 LIPS-A临床试验的子研究

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>Rationale: Acute respiratory distress syndrome (ARDS) is a devastating illness with limited therapeutic options. A better understanding of early biochemical and immunological events in ARDS could inform the development of new preventive and treatment strategies.>Objectives: To determine select peripheral blood lipid mediator and leukocyte responses in patients at risk for ARDS.>Methods: Patients at risk for ARDS were randomized as part of a multicenter, double-blind clinical trial of aspirin versus placebo (the LIPS-A [Lung Injury Prevention Study with Aspirin] trial; ). Plasma thromboxane B2 (TXB2), aspirin-triggered lipoxin A4 (15-epi-LXA4, ATL), and peripheral blood leukocyte number and activation were determined on enrollment and after treatment with either aspirin or placebo.>Measurements and Main Results: Thirty-three of 367 subjects (9.0%) developed ARDS after randomization. Baseline ATL levels, total monocyte counts, intermediate monocyte counts, and monocyte–platelet aggregates were associated with the development of ARDS. Peripheral blood neutrophil count and monocyte–platelet aggregates significantly decreased over time. Of note, nine subjects developed ARDS after randomization yet before study drug initiation, including seven subjects assigned to aspirin treatment. Subjects without ARDS at the time of first dose demonstrated a lower incidence of ARDS with aspirin treatment. Compared with placebo, aspirin significantly decreased TXB2 and increased the ATL/TXB2 ratio.>Conclusions: Biomarkers of intravascular monocyte activation in at-risk patients were associated with development of ARDS. The potential clinical benefit of early aspirin for prevention of ARDS remains uncertain. Together, results of the biochemical and immunological analyses provide a window into the early pathogenesis of human ARDS and represent potential vascular biomarkers of ARDS risk.Clinical trial registered with ().>Keywords: ARDS; monocyte–platelet aggregates; aspirin; lipoxin; thromboxane

机译：>理论上：急性呼吸窘迫综合征（ARDS）是一种毁灭性疾病，治疗选择有限。更好地了解ARDS中的早期生化和免疫学事件可能有助于开发新的预防和治疗策略。>目的：确定处于ARDS风险的患者中选择的外周血脂介质和白细胞反应。 >方法：将有ARDS风险的患者随机分为阿司匹林和安慰剂的多中心，双盲临床试验（LIPS-A [阿司匹林预防肺损伤研究]试验）。在入组时以及在使用阿司匹林或安慰剂治疗后，测定血浆血栓烷B2（TXB2），阿司匹林触发的脂蛋白A4（15-epi-LXA4，ATL）以及外周血白细胞的数目和激活。>测量和主要结果：随机分配后，有367名受试者中的33名（9.0％）出现了ARDS。基线ATL水平，总单核细胞计数，中间单核细胞计数和单核细胞-血小板聚集与ARDS的发展有关。随着时间的推移，外周血中性粒细胞计数和单核细胞-血小板聚集显着减少。值得注意的是，有9名受试者在随机分组后但在研究药物开始之前出现了ARDS，其中包括7名接受阿司匹林治疗的受试者。首次给药时无ARDS的受试者经阿司匹林治疗后ARDS发生率较低。与安慰剂相比，阿司匹林显着降低TXB2并增加ATL / TXB2比。>结论：高危患者血管内单核细胞活化的生物标志物与ARDS的发生有关。早期阿司匹林预防ARDS的潜在临床益处仍不确定。总之，生化和免疫学分析的结果为了解人类ARDS的早期发病机理提供了一个窗口，并代表了ARDS风险的潜在血管生物标志物。临床试验已在（）中注册。>关键字：单核细胞-血小板聚集体；阿司匹林;脂蛋白血栓烷

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期刊名称 American Journal of Respiratory and Critical Care Medicine
作者
Raja-Elie E. Abdulnour; Tina Gunderson; Ioanna Barkas; Jack Y. Timmons; Cindy Barnig; Michelle Gong; Daryl J. Kor; Ognjen Gajic; Daniel Talmor; Rickey E. Carter; Bruce D. Levy;
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年(卷),期 -1(197),12
年度 -1
页码 1575–1585
总页数 11
原文格式 PDF
正文语种
中图分类呼吸生理学;护理学;
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专利

1. US Critical Illness and Injury Trials Group: Lung Injury Prevention with Aspirin Study Group (USCIITG: LIPS-A). Effect of aspirin on development of ARDS in at-risk patients presenting to the emergency department: the LIPS-A randomized clinical trial (vol 315, pg 2406, 2016) [J] . Kor D. J., Carter R. E., Park P. K. JAMA: the Journal of the American Medical Association . 2016,第10期

机译：美国关键疾病和损伤试验组：阿司匹林研究组肺损伤预防（USCIITG：嘴唇-A）。阿司匹林对急诊部门患者ARDS发展的影响：嘴唇 - 一个随机临床试验（Vol 315，PG 2406,2016）
2. US Critical Illness and Injury Trials Group: Lung Injury Prevention with Aspirin Study Group (USCIITG: LIPS-A). Effect of aspirin on development of ARDS in at-risk patients presenting to the emergency department: the LIPS-A randomized clinical trial (vol 315, pg 2406, 2016) [J] . Kor D. J., Carter R. E., Park P. K. JAMA: the Journal of the American Medical Association . 2016,第10期

机译：美国重大疾病和伤害试验小组：阿司匹林预防肺损伤研究小组（USCIITG：LIPS-A）。阿司匹林对急诊科高危患者ARDS发生的影响：LIPS-A随机临床试验（第315卷，第2406页，2016年）
3. Inhaled nitric oxide in acute lung injury and acute respiratory distress syndrome. Inability to translate physiologic benefit to clinical outcome benefit in adult clinical trials (editorial; comment) [J] . Dellinger RP Intensive care medicine . 1999,第9期

机译：吸入急性肺损伤的一氧化氮和急性呼吸窘迫综合征。无法将生理学益处转化为成年临床试验中的临床结果效益（编辑;评论）
4. Secretory phospholipase A2 and pulmonary surfactant interaction: a vicious circle during the development of acute respiratory distress syndrome. [C] . Acta pharmacologica sinica . 2002

机译：分泌型磷脂酶A2与肺表面活性物质的相互作用：急性呼吸窘迫综合征发展过程中的恶性循环。
5. Development and testing of a modified clinical definition of the acute respiratory distress syndrome. [D] . Ferguson, Niall Douglas. 2002

机译：开发和测试急性呼吸窘迫综合征的改良临床定义。
6. Lung Injury Prevention with Aspirin (LIPS-A): a protocol for a multicentre randomised clinical trial in medical patients at high risk of acute lung injury [O] . Daryl Jon Kor, Daniel S Talmor, Valerie M Banner-Goodspeed, 2012

机译：阿司匹林预防肺损伤（LIPS-A）：一项针对具有急性肺损伤高风险的医学患者的多中心随机临床试验方案
7. Faculty Opinions recommendation of Randomized clinical trial of a combination of an inhaled corticosteroid and beta agonist in patients at risk of developing the acute respiratory distress syndrome. [O] . Kathryn Anne Hibbert 2019

机译：教师意见建议随机临床试验的吸入皮质类固醇和β激动剂组合有患有急性呼吸窘迫综合征的风险。

Early Intravascular Events Are Associated with Development of Acute Respiratory Distress Syndrome. A Substudy of the LIPS-A Clinical Trial

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