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The three cytokines IL-1β IL-18 and IL-1α share related but distinct secretory routes

机译:三种细胞因子IL-1βIL-18和IL-1α共享相关但截然不同的分泌途径

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摘要

Interleukin (IL)-1 family cytokines potently regulate inflammation, with the majority of the IL-1 family proteins being secreted from immune cells via unconventional pathways. In many cases, secretion of IL-1 cytokines appears to be closely coupled to cell death, yet the secretory mechanisms involved remain poorly understood. Here, we studied the secretion of the three best-characterized members of the IL-1 superfamily, IL-1α, IL-1β, and IL-18, in a range of conditions and cell types, including murine bone marrow–derived and peritoneal macrophages, human monocyte–derived macrophages, HeLa cells, and mouse embryonic fibroblasts. We discovered that IL-1β and IL-18 share a common secretory pathway that depends upon membrane permeability and can operate in the absence of complete cell lysis and cell death. We also found that the pathway regulating the trafficking of IL-1α is distinct from the pathway regulating IL-1β and IL-18. Although the release of IL-1α could also be dissociated from cell death, it was independent of the effects of the membrane-stabilizing agent punicalagin, which inhibited both IL-1β and IL-18 release. These results reveal that in addition to their role as danger signals released from dead cells, IL-1 family cytokines can be secreted in the absence of cell death. We propose that models used in the study of IL-1 release should be considered context-dependently.
机译:白介素(IL)-1家族细胞因子有效调节炎症,大部分IL-1家族蛋白通过非常规途径从免疫细胞分泌。在许多情况下,IL-1细胞因子的分泌似乎与细胞死亡密切相关,但所涉及的分泌机制仍知之甚少。在这里,我们研究了在一系列条件和细胞类型(包括鼠源于骨髓和腹膜的各种条件和细胞类型)中IL-1超家族三个最典型成员的分泌巨噬细胞,人类单核细胞衍生的巨噬细胞,HeLa细胞和小鼠胚胎成纤维细胞。我们发现IL-1β和IL-18共有一个共同的分泌途径,该途径取决于膜的通透性,并且可以在没有完整的细胞裂解和细胞死亡的情况下运行。我们还发现调节IL-1α运输的途径不同于调节IL-1β和IL-18的途径。尽管IL-1α的释放也可以从细胞死亡中解离出来,但它与膜稳定剂punicalagin的作用无关,punicalagin抑制IL-1β和IL-18的释放。这些结果表明,除了作为死亡细胞释放危险信号的作用外,IL-1家族细胞因子还可以在没有细胞死亡的情况下被分泌出来。我们建议研究IL-1释放所用的模型应视情况而定。

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