白细胞介素-4 通过下调转录因子 BCL6 促进生发中心记忆 B 细胞的选择。
Interleukin-4 downregulates transcription factor BCL6 to promote memory B cell selection in germinal centers.
机构信息
Department of Immunology, University of Washington School of Medicine, Seattle, WA 98109, USA.
Center for Immunity and Immunotherapies, Seattle Children's Research Institute, Seattle, WA 98101, USA.
出版信息
Immunity. 2024 Apr 9;57(4):843-858.e5. doi: 10.1016/j.immuni.2024.02.018. Epub 2024 Mar 20.
Abstract
Germinal center (GC)-derived memory B cells (MBCs) are critical for humoral immunity as they differentiate into protective antibody-secreting cells during re-infection. GC formation and cellular interactions within the GC have been studied in detail, yet the exact signals that allow for the selection and exit of MBCs are not understood. Here, we showed that IL-4 cytokine signaling in GC B cells directly downregulated the transcription factor BCL6 via negative autoregulation to release cells from the GC program and to promote MBC formation. This selection event required additional survival cues and could therefore result in either GC exit or death. We demonstrate that both increasing IL-4 bioavailability or limiting IL-4 signaling disrupted MBC selection stringency. In this way, IL-4 control of BCL6 expression serves as a tunable switch within the GC to tightly regulate MBC selection and affinity maturation.
摘要
生发中心(GC)衍生的记忆 B 细胞(MBC)对于体液免疫至关重要,因为它们在再次感染时分化为保护性抗体分泌细胞。GC 的形成和 GC 内的细胞相互作用已经得到了详细研究,但允许选择和退出 MBC 的确切信号尚不清楚。在这里,我们表明 GC B 细胞中的 IL-4 细胞因子信号直接通过负反馈调节下调转录因子 BCL6,从而使细胞从 GC 程序中释放出来并促进 MBC 形成。这种选择事件需要额外的生存信号,因此可能导致 GC 退出或死亡。我们证明,增加 IL-4 生物利用度或限制 IL-4 信号均可破坏 MBC 选择的严格性。通过这种方式,IL-4 对 BCL6 表达的控制在 GC 内充当一个可调开关,以紧密调节 MBC 选择和亲和力成熟。
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