Department of Surgery, and.
Division of Pulmonary, Allergy, Critical Care and Sleep, Department of Medicine, Emory University School of Medicine, Atlanta, Georgia, USA.
JCI Insight. 2019 May 2;4(9). doi: 10.1172/jci.insight.126030.
Recent seminal studies have revealed that laboratory mice differ from adult humans with regard to the frequency, number, and distribution of memory T cells. Because our data show that memory T cells are more susceptible to sepsis-induced death than naive T cells, in this study we developed a model in which mice possess a memory T cell compartment more similar to that of adult humans, to better study immune responses during sepsis in the more physiologically relevant context of high frequencies of memory T cells. Using this model, we found that CD44hi memory T cells significantly upregulated the coinhibitory molecule 2B4 during sepsis, and 2B4+ memory T cells coexpressed markers of both activation and exhaustion. Genetic deficiency in 2B4 resulted in decreased mortality during sepsis. Mechanistically, this decreased mortality was associated with reduced caspase-3/7+ apoptotic T cells in 2B4-/- relative to WT, septic hosts. These results were corroborated by analysis of PBMCs isolated from human patients with sepsis, which showed increased frequencies of caspase-3/7+ apoptotic cells among 2B4+ relative to 2B4- T cells. Thus, 2B4 plays a critical role in sepsis-induced apoptosis in both murine memory T cells and those isolated from human patients with sepsis.
最近的开创性研究表明,实验小鼠在记忆 T 细胞的频率、数量和分布方面与成年人类不同。由于我们的数据表明记忆 T 细胞比幼稚 T 细胞更容易受到脓毒症诱导的死亡,因此在这项研究中,我们开发了一种模型,其中小鼠具有更类似于成年人类的记忆 T 细胞区室,以便在更具生理相关性的高频率记忆 T 细胞背景下更好地研究脓毒症期间的免疫反应。使用这种模型,我们发现 CD44hi 记忆 T 细胞在脓毒症期间显著上调共抑制分子 2B4,并且 2B4+记忆 T 细胞共表达激活和衰竭的标志物。2B4 的遗传缺陷导致脓毒症期间死亡率降低。从机制上讲,与 WT 脓毒症宿主相比,2B4-/-中的 caspase-3/7+凋亡 T 细胞减少导致死亡率降低。从分离自脓毒症患者的 PBMCs 的分析中得到了这些结果的证实,该分析表明 2B4+细胞中 caspase-3/7+凋亡细胞的频率高于 2B4-细胞。因此,2B4 在脓毒症诱导的小鼠记忆 T 细胞和分离自脓毒症患者的记忆 T 细胞中的凋亡中都发挥了关键作用。
