Norton Thoracic Institute, St. Joseph's Hospital and Medical Center, Phoenix, AZ, USA.
Yale School of Medicine, CT, USA.
Cell Immunol. 2020 Sep;355:104172. doi: 10.1016/j.cellimm.2020.104172. Epub 2020 Jul 15.
Human lung transplant recipients undergoing rejection induce circulatory exosomes with lung self-antigens (SAgs), K-alpha 1 Tubulin and Collagen V, and immunization of C57BL/6 mice with exosomes induced obliterative airway disease (HEI-OAD). We analyzed whether exosomes with SAgs induced immunity in microRNA-155 knockout mice (miR-155KO), as microRNA-155 is an immune regulator. C57BL/6 and miR-155KO were immunized with exosomes from stable or chronic rejection (bronchiolitis obliterans syndrome (BOS) and on day 30, induction of exosomes, antibodies (Abs) to SAgs and cellular immunity were determined. C57BL/6 immunized with exosomes from BOS developed OAD. These immunized animals also developed Abs to SAgs and increased frequency of SAg-specific IFNγ and IL17- producing cells. In contrast, Abs to SAgs did not develop in miR-155KO and there was reduction in frequency of cells producing IL10. Upregulation of suppressor of cytokine signaling for lung inflammation was also noted resulting in abrogation of induction of exosomes with SAgs OAD.
人类肺移植受者发生排斥反应时会产生带有肺自身抗原(SAgs)的循环外泌体,如 K-alpha 1 微管蛋白和胶原 V,用外泌体免疫 C57BL/6 小鼠可诱导闭塞性细支气管炎样病变(HEI-OAD)。我们分析了带有 SAg 的外泌体是否会在 microRNA-155 敲除小鼠(miR-155KO)中诱导免疫,因为 microRNA-155 是一种免疫调节剂。用稳定或慢性排斥(细支气管阻塞综合征(BOS)的外泌体免疫 C57BL/6 和 miR-155KO,并在第 30 天测定外泌体、针对 SAg 的抗体(Abs)和细胞免疫的诱导情况。用 BOS 外泌体免疫的 C57BL/6 发展为 OAD。这些免疫动物还产生了针对 SAg 的 Abs,并增加了 SAg 特异性 IFNγ和 IL17 产生细胞的频率。相比之下,miR-155KO 中没有产生针对 SAg 的 Abs,产生 IL10 的细胞频率降低。还注意到与肺部炎症相关的细胞因子信号转导抑制剂的上调,导致诱导带有 SAg 的外泌体 OAD 失败。
