滤泡 B 细胞通过 T 细胞介导的分化为浆细胞并分泌致病性免疫球蛋白 G 促进动脉粥样硬化。
Follicular B Cells Promote Atherosclerosis via T Cell-Mediated Differentiation Into Plasma Cells and Secreting Pathogenic Immunoglobulin G.
机构信息
From the Vascular Biology and Atherosclerosis Lab, Baker Heart and Diabetes Institute, Melbourne, Victoria, Australia (C.T., Y.-H.L., P.K., Y.L., A.C., H.H., A.B., T.K.).
Walter and Eliza Hall Institute, Parkville, Victoria, Australia (A.K.).
出版信息
Arterioscler Thromb Vasc Biol. 2018 May;38(5):e71-e84. doi: 10.1161/ATVBAHA.117.310678. Epub 2018 Mar 29.
OBJECTIVE
B cells promote or protect development of atherosclerosis. In this study, we examined the role of MHCII (major histocompatibility II), CD40 (cluster of differentiation 40), and Blimp-1 (B-lymphocyte-induced maturation protein) expression by follicular B (FO B) cells in development of atherosclerosis together with the effects of IgG purified from atherosclerotic mice.
APPROACH AND RESULTS
Using mixed chimeric mice whose B cells are deficient in MHCII or CD40, we demonstrate that these molecules are critical for the proatherogenic actions of FO B cells. During development of atherosclerosis, these deficiencies affected T-B cell interactions, germinal center B cells, plasma cells, and IgG. As FO B cells differentiating into plasma cells require Blimp-1, we also assessed its role in the development of atherosclerosis. Blimp-1-deficient B cells greatly attenuated atherosclerosis and immunoglobulin-including IgG production, preventing IgG accumulation in atherosclerotic lesions; Blimp-1 deletion also attenuated lesion proinflammatory cytokines, apoptotic cell numbers, and necrotic core. To determine the importance of IgG for atherosclerosis, we purified IgG from atherosclerotic mice. Their transfer but not IgG from nonatherosclerotic mice into mice whose B cells are Blimp-1-deficient increased atherosclerosis; transfer was associated with IgG accumulating in atherosclerotic lesions, increased lesion inflammatory cytokines, apoptotic cell numbers, and necrotic core size.
CONCLUSIONS
The mechanism by which FO B cells promote atherosclerosis is highly dependent on their expression of MHCII, CD40, and Blimp-1. FO B cell differentiation into IgG-producing plasma cells also is critical for their proatherogenic actions. Targeting B-T cell interactions and pathogenic IgG may provide novel therapeutic strategies to prevent atherosclerosis and its adverse cardiovascular complications.
目的
B 细胞促进或保护动脉粥样硬化的发展。在这项研究中,我们研究了滤泡 B(FO B)细胞中 MHCII(主要组织相容性复合体 II)、CD40(分化群 40)和 Blimp-1(B 淋巴细胞诱导成熟蛋白)的表达在动脉粥样硬化发展中的作用,以及从动脉粥样硬化小鼠中纯化的 IgG 的作用。
方法和结果
使用 B 细胞缺乏 MHCII 或 CD40 的混合嵌合小鼠,我们证明这些分子对于 FO B 细胞的促动脉粥样硬化作用至关重要。在动脉粥样硬化发展过程中,这些缺陷影响了 T-B 细胞相互作用、生发中心 B 细胞、浆细胞和 IgG。由于 FO B 细胞分化为浆细胞需要 Blimp-1,我们还评估了其在动脉粥样硬化发展中的作用。Blimp-1 缺陷的 B 细胞极大地减轻了动脉粥样硬化和免疫球蛋白(包括 IgG)的产生,防止 IgG 在动脉粥样硬化病变中积累;Blimp-1 缺失还减轻了病变促炎细胞因子、凋亡细胞数量和坏死核心。为了确定 IgG 在动脉粥样硬化中的重要性,我们从动脉粥样硬化小鼠中纯化了 IgG。它们的转移,而不是非动脉粥样硬化小鼠 IgG 的转移,进入 Blimp-1 缺陷的小鼠,增加了动脉粥样硬化;转移与 IgG 在动脉粥样硬化病变中的积累、病变炎症细胞因子的增加、凋亡细胞数量和坏死核心大小有关。
结论
FO B 细胞促进动脉粥样硬化的机制高度依赖于其 MHCII、CD40 和 Blimp-1 的表达。FO B 细胞分化为产生 IgG 的浆细胞对于其促动脉粥样硬化作用也至关重要。针对 B-T 细胞相互作用和致病性 IgG 可能为预防动脉粥样硬化及其不良心血管并发症提供新的治疗策略。
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