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Early upregulation of acute respiratory distress syndrome-associated cytokines promotes lethal disease in an aged-mouse model of severe acute respiratory syndrome coronavirus infection

机译:在严重急性呼吸综合征冠状病毒感染的老年小鼠模型中,急性呼吸窘迫综合征相关细胞因子的早期上调促进致死性疾病

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textabstractSeveral respiratory viruses, including influenza virus and severe acute respiratory syndrome coronavirus (SARS-CoV), produce more severe disease in the elderly, yet the molecular mechanisms governing age-related susceptibility remain poorly studied. Advanced age was significantly associated with increased SARS-related deaths, primarily due to the onset of early- and late-stage acute respiratory distress syndrome (ARDS) and pulmonary fibrosis. Infection of aged, but not young, mice with recombinant viruses bearing spike glycoproteins derived from early human or palm civet isolates resulted in death accompanied by pathological changes associated with ARDS. In aged mice, a greater number of differentially expressed genes were observed than in young mice, whose responses were significantly delayed. Differences between lethal and nonlethal virus phenotypes in aged mice could be attributed to differences in host response kinetics rather than virus kinetics. SARS-CoV infection induced a range of interferon, cytokine, and pulmonary wound-healing genes, as well as several genes associated with the onset of ARDS. Mice that died also showed unique transcriptional profiles of immune response, apoptosis, cell cycle control, and stress. Cytokines associated with ARDS were signifi-cantly upregulated in animals experiencing lung pathology and lethal disease, while the same animals experienced downregulation of the ACE2 receptor. These data suggest that the magnitude and kinetics of a disproportionately strong host innate immune response contributed to severe respiratory stress and lethality. Although the molecular mechanisms governing ARDS pathophysiology remain unknown in aged animals, these studies reveal a strategy for dissecting the genetic pathways by which SARS-CoV infection induces changes in the host response, leading to death. Copyright
机译:包括流感病毒和严重急性呼吸系统综合症冠状病毒(SARS-CoV)在内的几种呼吸道病毒在老年人中产生的疾病更为严重,但控制与年龄相关的易感性的分子机制仍然缺乏研究。高龄与SARS相关的死亡增加显着相关,这主要是由于早期和晚期急性呼吸窘迫综合征(ARDS)和肺纤维化的发作。用重组病毒感染年长但不年轻的小鼠,这些病毒带有源自早期人类或棕榈果子狸分离物的刺突糖蛋白,导致死亡,并伴有与ARDS相关的病理变化。在年老的小鼠中,观察到的差异表达基因数量比年幼的小鼠要多,后者的反应明显延迟。老年小鼠的致命和非致命病毒表型之间的差异可能归因于宿主反应动力学的差异,而不是病毒的动力学差异。 SARS-CoV感染诱导了一系列干扰素,细胞因子和肺伤口愈合基因,以及与ARDS发作相关的几个基因。死亡的小鼠还表现出独特的转录应答,包括免疫应答,细胞凋亡,细胞周期控制和应激。与ARDS相关的细胞因子在经历肺部病理和致死性疾病的动物中显着上调,而同一动物的ACE2受体则下调。这些数据表明,过强的宿主先天免疫反应的强度和动力学有助于严重的呼吸压力和致死性。尽管在成年动物中控制ARDS病理生理的分子机制仍然未知,但这些研究揭示了剖析SARS-CoV感染诱导宿主反应变化并导致死亡的遗传途径的策略。版权

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