A Randomzied Phase II Trial of CMV Prevention in Acute Lung Injury

急性肺损伤中 CMV 预防的随机 II 期试验

• 批准号: 8321520
• 负责人: MICHAEL J BOECKH
• 金额: $ 211.89万
• 依托单位: FRED HUTCHINSON CANCER RESEARCH CENTER
• 依托单位国家: 美国
• 财政年份: 2010
• 资助国家: 美国
• 起止时间: 2010-06-01 至 2016-12-31
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8321520
• 关键词: Acute Lung Injury; Adult; Affect; Blood; Clinical Protocols; Collagen; Cytomegalovirus; Cytomegalovirus Infections; Deposition; Double-Blind Method; Failure; Fibrosis; Functional disorder; Ganciclovir; Health Expenditures; Herpesviridae; Human; Immune; Immunocompetent; Immunosuppression; In Vitro; Infection; Inflammation; Inflammatory; Inflammatory Response; Injury; Interleukin-6; Length of Stay; Lung; Mechanical ventilation; Mediating; Mediator of activation protein; Morbidity - disease rate; Murid herpesvirus 1; Mus; Outcome; Pathogenesis; Pathway interactions; Patients; Phase; Phase II Clinical Trials; Placebo Control; Pneumonia; Prevention; Prophylactic treatment; Sepsis; Serum; Valganciclovir; Virus; Virus Diseases; abstracting; body system; cytokine; improved; in vivo; lung injury; mortality; mouse model; outcome forecast; standard of care

DESCRIPTION (provided by applicant): Acute lung injury (ALI) is a major cause of morbidity, mortality and health care expenditure. Cytomegalovirus (CMV) is a human herpesvirus known to infect 50-70% of US adults. Mouse models have shown that subclinical CMV infection can produce significant biologic effects in the lung, such as inflammation and fibrosis. Each of these biologic effects of subclinical CMV infection have either previously been demonstrated (inflammation, fibrosis) or could theoretically be important (immunosuppression) in sepsis associated ALI and its complications. Recently, CMV has been demonstrated to commonly reactivate in the blood and lung of immunocompetent adults with sepsis, and to be independently associated with prolonged mechanical ventilation and increased ICU and hospital length of stay. Furthermore, CMV infection has been demonstrated both in vitro and in vivo to elicit multiple pro-inflammatory and pro-fibrosis mediators that have previously been hypothesized to be important in the pathogenesis of ALI and its complications, including multi-organ system failure. Thus, we hypothesize that CMV reactivation in CMV seropositive patients with acute lung injury both amplifies and perpetuates pulmonary and systemic inflammation, resulting in persistent lung dysfunction and multi-organ system failure. We propose to use anti-CMV prophylaxis in immunocompetent subjects with ALI to interrupt the cascade of virus-induced magnification of inflammatory cytokine-mediated lung damage. We also propose mechanistic studies in a mouse model to examine the mechanistic pathway of CMV infection and lung injury. The Clinical Protocol is to conduct a phase II double-blind placebo-controlled multicenter phase II trial of ganciclovir/valganciclovir prophylaxis in patients with sepsis -associated ALI. The primary endpoint of the study is IL-6 levels in serum at day 14. The Ancillary Project will determine the mechanisms by which latent MCMV (MCMV) amplifies lung inflammatory responses injury and the mechanisms by which MCMV reactivation promotes collagen deposition during lung injury. Specifically, we will examine in the mouse model whether the initial inflammatory response to acute lung injury is affected by murine CMV (MCMV) infection and whether isolated ALI results in MCMV reactivation; whether MCMV reactivation increases collagen accumulation during ALI by increased collagen deposition or by decreased degradation; and whether ganciclovir alters the course of acute lung injury in mice with MCMV infection. RELEVANCE: This study will examine whether prophylaxis against a common viral infection, called cytomegalovirus infection, reduces inflammation in the lung and thereby improves outcome in immune competent patients with acute lung injury following sepsis or pneumonia. If successful, this therapy has the potential to change the standard of care for patients with acute lung injury and to improve overall prognosis. (End of Abstract)

描述（由申请人提供）：急性肺损伤（ALI）是发病率、死亡率和医疗费用的主要原因。巨细胞病毒（CMV）是一种人类疱疹病毒，已知感染50-70%的美国成年人。小鼠模型表明，亚临床CMV感染可在肺中产生显著的生物学效应，如炎症和纤维化。亚临床CMV感染的这些生物学效应中的每一个先前已经被证明（炎症、纤维化）或理论上在脓毒症相关的ALI及其并发症中可能是重要的（免疫抑制）。最近，CMV已被证明通常在免疫功能正常的脓毒症成人的血液和肺中重新激活，并与延长机械通气和增加ICU和住院时间独立相关。此外，巨细胞病毒感染已被证明在体外和体内引起多种促炎和促纤维化介质，以前被假设为是重要的发病机制的ALI及其并发症，包括多器官系统衰竭。因此，我们假设CMV血清阳性急性肺损伤患者的CMV再激活既放大又延续了肺部和全身炎症，导致持续性肺功能障碍和多器官系统衰竭。我们建议对免疫功能正常的ALI受试者使用抗CMV预防，以中断病毒诱导的炎症细胞因子介导的肺损伤放大的级联反应。我们还建议在小鼠模型中进行机制研究，以检查CMV感染和肺损伤的机制途径。临床方案是在脓毒症相关ALI患者中进行更昔洛韦/缬更昔洛韦预防的II期双盲安慰剂对照多中心II期试验。研究的主要终点是第14天血清中的IL-6水平。辅助项目将确定潜在MCMV（MCMV）放大肺部炎症反应损伤的机制，以及MCMV再活化促进肺损伤期间胶原沉积的机制。具体来说，我们将研究在小鼠模型中，是否初始炎症反应急性肺损伤的影响，小鼠巨细胞病毒（MCMV）感染，是否孤立的ALI导致MCMV再激活;是否MCMV再激活增加胶原蛋白的积累，在ALI增加胶原蛋白沉积或减少降解;是否更昔洛韦改变过程中的急性肺损伤与MCMV感染的小鼠。相关性：这项研究将检查预防一种常见的病毒感染，称为巨细胞病毒感染，是否减少肺部炎症，从而改善脓毒症或肺炎后急性肺损伤的免疫功能正常患者的预后。如果成功，这种疗法有可能改变急性肺损伤患者的护理标准，并改善整体预后。(End摘要）