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中性粒细胞和树突状细胞产生的 BAFF 受到不同的调节,在抗西尼罗河病毒的抗体反应和保护性免疫中发挥不同的作用。

BAFF Produced by Neutrophils and Dendritic Cells Is Regulated Differently and Has Distinct Roles in Antibody Responses and Protective Immunity against West Nile Virus.

机构信息

Department of Immunology, University of Washington, Seattle, WA 98109; and

Department of Immunology, University of Washington, Seattle, WA 98109; and.

出版信息

J Immunol. 2020 Mar 15;204(6):1508-1520. doi: 10.4049/jimmunol.1901120. Epub 2020 Feb 7.

Abstract

B cell activating factor (BAFF) is essential for B cells to develop and respond to Ags. Dysregulation of BAFF contributes to the development of some autoimmune diseases and malignancies. Little is known about when, where, and how BAFF is produced in vivo and about which BAFF-producing cells contribute to B cell responses. To better understand BAFF functions, we created BAFF reporter (BAFF-RFP) mice and floxed ( ) mice. Splenic and bone marrow neutrophils (Nphs) from BAFF-RFP mice expressed the highest constitutive levels of BAFF; other myeloid subsets, including conventional dendritic cells (cDCs) and monocyte (MO) subsets, expressed lower levels. Treatment of BAFF-RFP mice with polyinosinic:polycytidylic acid increased BAFF expression in splenic Ly6C inflammatory MOs, CD11b activated NK subset, and in bone marrow myeloid precursors. Postinfection with West Nile virus (WNV), BAFF increased in CD8 cDCs and Nphs, and BAFF CD11b NK cells expanded in draining lymph nodes. The cell- and tissue-specific increases in BAFF expression were dependent on type I IFN signaling. MAVS also was required or contributed to BAFF expression in dendritic cell and MO subsets, respectively. Mice with deletion of in either cDCs or Nphs had reduced Ab responses after NP-Ficoll immunization; thus, BAFF produced by both cDCs and Nphs contributes to T cell-independent Ab responses. Conversely, mice with a cDC deficiency had increased mortality after WNV infection and decreased WNV-specific IgG and neutralizing Ab responses. BAFF produced by Nphs and cDCs is regulated differently and has key roles in Ab responses and protective immunity.

摘要

B 细胞激活因子 (BAFF) 对于 B 细胞的发育和对抗原的应答至关重要。BAFF 的失调导致一些自身免疫性疾病和恶性肿瘤的发生。目前对于体内 BAFF 何时、何地以及如何产生,以及哪些产生 BAFF 的细胞有助于 B 细胞应答知之甚少。为了更好地理解 BAFF 的功能,我们构建了 BAFF 报告(BAFF-RFP)小鼠和 floxed()小鼠。BAFF-RFP 小鼠的脾脏和骨髓中性粒细胞(Nphs)表达最高水平的 BAFF;其他髓系亚群,包括传统树突状细胞(cDCs)和单核细胞(MO)亚群,表达较低水平的 BAFF。用多聚肌苷酸:多聚胞苷酸处理 BAFF-RFP 小鼠可增加脾脏 Ly6C 炎症性 MO、CD11b 激活的 NK 亚群和骨髓髓样前体细胞中的 BAFF 表达。感染西尼罗河病毒(WNV)后,CD8 cDCs 和 Nphs 中的 BAFF 增加,引流淋巴结中 CD11b NK 细胞扩增。BAFF 表达的细胞和组织特异性增加依赖于 I 型 IFN 信号。MAVS 也分别需要或有助于树突状细胞和 MO 亚群中 BAFF 的表达。cDC 或 Nphs 中缺失的小鼠在 NP-Ficoll 免疫后抗体反应减少;因此,cDC 和 Nphs 产生的 BAFF 有助于 T 细胞非依赖性抗体反应。相反,WNV 感染后 cDC 缺陷小鼠死亡率增加,WNV 特异性 IgG 和中和抗体反应降低。Nphs 和 cDC 产生的 BAFF 的调节方式不同,在抗体反应和保护性免疫中具有关键作用。

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