Alcohol and Burn Trauma: Multi-organ Inflammatory Responses

酒精和烧伤：多器官炎症反应

基本信息

批准号：
10192755
负责人：
ELIZABETH J. KOVACS
金额：
$ 43.06万
依托单位：
UNIVERSITY OF COLORADO DENVER
依托单位国家：
美国
项目类别：
财政年份：
2019
资助国家：
美国
起止时间：
2019-09-20 至 2024-06-30
项目状态：
已结题

来源：
https://reporter.nih.gov/project-details/10192755
关键词：
Address Adult Adult Respiratory Distress Syndrome Alcohol consumption Alcoholic Intoxication Alcohols Applications Grants Bacteria Biological Markers Blood Circulation Burn Trauma Burn injury Cutaneous Development Distal Distant Endotoxins Epithelial Cells Failure Functional disorder Grant Homeostasis Infection Inflammation Inflammatory Response Inhalation Injury Intestinal permeability Intestines Knowledge Laboratories Lead Lung Lung infections Measures Modeling Monitor Morbidity - disease rate Multiple Organ Failure Organ Outcome Patients Plasma Pneumonia Predisposition Process Pulmonary Inflammation Recovery Reporting Research Risk Secondary to System Testing Time Trauma alcohol effect alcohol exposure cell injury clinically relevant design drinking dysbiosis fecal microbiome gut microbiome improved functioning intestinal barrier intestinal epithelium lung injury microbial microbiome mortality mouse model novel therapeutics programs response response to injury skin burn stem systemic inflammatory response

项目摘要

Project Abstract/Summary This R35 MIRA grant application is designed to investigate mechanisms responsible for the exaggerated effects of alcohol intoxication on multi-organ system responses after burn injury. Of the million people per year who suffer burn injuries in the U.S., nearly half of the adult patients are intoxicated at the time of injury. Intoxicated burn patients have increased morbidity and mortality compared to those who had not been drinking. The lung is the most frequent organ to fail after a remote injury such as cutaneous burn, with 45% of burn patients showing some form of lung damage even in the absence of inhalation injury. Pneumonia and acute respiratory distress syndrome (ARDS) are among the major complications seen in intoxicated burn patients. Little is known about the mechanism by which alcohol intoxication upregulates the post-burn systemic inflammatory responses that lead to excessive pulmonary inflammation and increased susceptibility to lung infection. Recently, we reported that the post-burn pulmonary inflammatory response is exacerbated in intoxicated subjects because of a breach in the integrity of the intestinal epithelial barrier secondary to burn. This, along with dysbiosis of the fecal microbiome, could be critically involved in the systemic inflammation seen after burn injury. We and others have shown that burn trauma and alcohol intoxication independently cause these intestinal changes and that, after the “two hit” insult of alcohol and burn injury, these responses are amplified, which could result in a more dramatic shift in the microbiome and a greater release of bacterial products and endotoxins into the circulation, triggering systemic inflammation and damage to distant organs like the lung. To date, we know very little about how and when the intestine recovers from remote injury, such as a cutaneous scald burn, and even less about how factors including alcohol intoxication prior to injury alter that process. In this research program, we will use our clinically-relevant murine model of alcohol intoxication and burn injury along with burn patients, some of whom will have consumed alcohol prior to sustaining their injuries, to address the following questions: 1) What are the effects of alcohol intoxication and burn injury on the gut, specifically, the integrity of the intestinal epithelial barrier and the fecal microbiome, and how long do they last? 2) Can intestinal epithelial cell barrier dysfunction be accurately monitored by measuring plasma biomarkers of intestinal epithelial cell damage, microbial translocation and inflammation, rather than by more invasive tests? 3) Are there gut-directed therapies that can restore the intestinal barrier and microbial homeostasis, which, by virtue of reducing systemic inflammation, will improve the function of distal organs, such as the lung? Taken together, these studies will expand the knowledge of how alcohol exposure alters the gut in the context of remote injury such as burns and may lead to the development of novel therapies for the treatment of patients with burns and other forms of trauma.

项目摘要/总结此 R35 MIRA 拨款申请旨在调查造成夸大的机制酒精中毒对烧伤后多器官系统反应的影响。在美国遭受烧伤的成年患者中，近一半在受伤时处于醉酒状态。与没有中毒的烧伤患者相比，中毒烧伤患者的发病率和死亡率增加肺部是皮肤烧伤等远程损伤后最常见的衰竭器官，占 45%。即使没有吸入性损伤，烧伤患者也会出现某种形式的肺部损伤。急性呼吸窘迫综合征（ARDS）是中毒烧伤的主要并发症之一对于酒精中毒上调烧伤后全身系统的机制知之甚少。炎症反应导致肺部过度炎症并增加肺部易感性最近，我们报道烧伤后肺部炎症反应加剧。由于烧伤继发的肠上皮屏障完整性破裂而导致中毒的受试者。这与粪便微生物群的失调一起，可能与全身炎症密切相关我们和其他人已经证明烧伤和酒精中毒是独立的。导致这些肠道变化，并且在酒精和烧伤的“两次打击”侮辱之后，这些反应被放大，这可能导致微生物组发生更显着的变化和细菌的更多释放产物和内毒素进入循环，引发全身炎症和远端器官损伤就像肺部一样，迄今为止，我们对肠道如何以及何时从远程损伤中恢复知之甚少。例如皮肤烫伤，更不用说受伤前的酒精中毒等因素如何改变在这个过程中，我们将使用临床相关的酒精中毒小鼠模型。以及烧伤患者和烧伤患者，其中一些人在维持生命之前会饮酒伤害，解决以下问题： 1）酒精中毒和烧伤对人有什么影响？肠道，特别是肠上皮屏障和粪便微生物组的完整性，以及需要多长时间 2) 可以通过测量血浆来准确监测肠上皮细胞屏障功能障碍吗？肠上皮细胞损伤、微生物易位和炎症的生物标志物，而不是更多 3) 是否有可以恢复肠道屏障和微生物的肠道疗法？体内平衡，通过减少全身炎症，将改善远端器官的功能，总而言之，这些研究将扩大人们对酒精暴露如何改变的认识。肠道在烧伤等远程损伤的情况下可能会导致新疗法的开发治疗烧伤和其他形式的创伤患者。