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Gastrointestinal microbiota contributes to the development of murine transfusion-related acute lung injury

机译:胃肠道微生物群促进与鼠输血有关的急性肺损伤的发展

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摘要

Transfusion-related acute lung injury (TRALI) is a syndrome of respiratory distress upon blood transfusion and is the leading cause of transfusion-related fatalities. Whether the gut microbiota plays any role in the development of TRALI is currently unknown. We observed that untreated barrier-free (BF) mice suffered from severe antibody-mediated acute lung injury, whereas the more sterile housed specific pathogen-free (SPF) mice and gut flora-depleted BF mice were both protected from lung injury. The prevention of TRALI in the SPF mice and gut flora–depleted BF mice was associated with decreased plasma macrophage inflammatory protein-2 levels as well as decreased pulmonary neutrophil accumulation. DNA sequencing of amplicons of the 16S ribosomal RNA gene revealed a varying gastrointestinal bacterial composition between BF and SPF mice. BF fecal matter transferred into SPF mice significantly restored TRALI susceptibility in SPF mice. These data reveal a link between the gut flora composition and the development of antibody-mediated TRALI in mice. Assessment of gut microbial composition may help in TRALI risk assessment before transfusion.
机译:与输血有关的急性肺损伤(TRALI)是输血时呼吸窘迫的综合症,并且是与输血有关的死亡的主要原因。目前尚不清楚肠道菌群是否在TRALI的发展中发挥任何作用。我们观察到未经治疗的无障碍(BF)小鼠遭受了严重的抗体介导的急性肺损伤,而无菌性更强的无特定病原体(SPF)的小鼠和肠道菌群耗尽的BF小鼠均受到了肺损伤的保护。在SPF小鼠和肠道菌群减少的BF小鼠中预防TRALI与血浆巨噬细胞炎性蛋白2水平降低以及肺中性粒细胞积聚降低有关。对16S核糖体RNA基因的扩增子进行的DNA测序揭示了BF和SPF小鼠之间胃肠道细菌组成的变化。高炉粪便转移到SPF小鼠体内可显着恢复SPF小鼠对TRALI的敏感性。这些数据揭示了肠道菌群组成与小鼠抗体介导的TRALI发育之间的联系。肠道微生物组成的评估可能有助于输血前TRALI风险评估。

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