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诱导型一氧化氮合酶二聚化抑制剂可预防烧伤合并烟雾吸入性损伤绵羊的心血管和肾脏疾病。

Inducible nitric oxide synthase dimerization inhibitor prevents cardiovascular and renal morbidity in sheep with combined burn and smoke inhalation injury.

作者信息

Enkhbaatar Perenlei, Murakami Kazunori, Shimoda Katsumi, Mizutani Akio, Traber Lillian, Phillips Gary, Parkinson John, Salsbury John R, Biondo Nettie, Schmalstieg Frank, Burke Ann, Cox Robert, Hawkins Hal, Herndon David, Traber Daniel

机构信息

Department of Anesthesiology, University of Texas Medical Branch, 610 Texas Ave., Galveston, TX 77555, USA.

出版信息

Am J Physiol Heart Circ Physiol. 2003 Dec;285(6):H2430-6. doi: 10.1152/ajpheart.00055.2003. Epub 2003 Aug 14.

Abstract

Inducible nitric oxide synthase (iNOS) is implicated in the pathogenesis of acute respiratory distress syndrome (ARDS). ARDS treatment is frequently complicated by significant extrapulmonary comorbidity. This study was designed to clarify the role of iNOS in mediating extrapulmonary comorbidity in sheep after combined burn and smoke inhalation injuries using a potent and highly selective iNOS dimerization inhibitor, BBS-2. Twenty-two female sheep were operatively prepared. After 5 days of recovery, tracheostomy was performed under ketamine-halothane anesthesia. Sheep were given a 40% total body surface third-degree burns and insufflated with cotton smoke (48 breaths, <40 degrees C). Sheep were divided into four groups: noninjured and nontreated (sham group; n = 6), noninjured but treated with BBS-2 (sham/BBS-2 group; n = 4), injured but nontreated (control group, n = 6), and injured but treated with 100 microg.kg-1.h-1 BBS-2 (BBS-2 group; n = 6). Evaluation was in a laboratory intensive care unit setting for 48 h. The sham group had stable cardiopulmonary and systemic hemodynamics. Control animals showed multiple signs of morbidity. Decreased left ventricular stroke work index and stroke volume index with elevated left atrial pressure indicated myocardial depression. Systemic vascular leak was evidenced by robust hemoconcentration, decreased plasma oncotic pressure, and increased transvascular fluid flux into the lymphatic system. Finally, severely impaired renal function (urinary output) was associated with adverse net fluid balance. Treatment with BBS-2 prevented all these morbidities without adversely effecting cardiovascular hemodynamics such as cardiac index and mean arterial pressure. The results identify a major role for iNOS in mediating extrapulmonary comorbidity in a clinically relevant and severe trauma model and support the use of highly selective iNOS inhibitors as novel treatments in critical care medicine.

摘要

诱导型一氧化氮合酶(iNOS)与急性呼吸窘迫综合征(ARDS)的发病机制有关。ARDS治疗常因严重的肺外合并症而复杂化。本研究旨在使用一种强效且高度选择性的iNOS二聚化抑制剂BBS-2,阐明iNOS在合并烧伤和烟雾吸入损伤的绵羊中介导肺外合并症的作用。22只雌性绵羊接受手术准备。恢复5天后,在氯胺酮-氟烷麻醉下进行气管切开术。给绵羊造成40%体表面积的三度烧伤,并吸入棉烟(48次呼吸,<40摄氏度)。绵羊分为四组:未受伤且未治疗(假手术组;n = 6)、未受伤但用BBS-2治疗(假手术/BBS-2组;n = 4)、受伤但未治疗(对照组,n = 6)以及受伤但用100μg·kg-1·h-1 BBS-2治疗(BBS-2组;n = 6)。在实验室重症监护病房环境中评估48小时。假手术组心肺和全身血流动力学稳定。对照动物出现多种发病迹象。左心室每搏功指数和每搏量指数降低,左心房压力升高表明心肌抑制。全身血管渗漏表现为明显的血液浓缩、血浆胶体渗透压降低以及进入淋巴系统的跨血管液体通量增加。最后,严重受损的肾功能(尿量)与不利的净液体平衡相关。用BBS-2治疗可预防所有这些发病情况,且对诸如心脏指数和平均动脉压等心血管血流动力学没有不利影响。结果表明,在一个临床相关的严重创伤模型中,iNOS在介导肺外合并症方面起主要作用,并支持使用高度选择性的iNOS抑制剂作为重症医学中的新型治疗方法。

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