Laboratory of Immunogenetics, National Institute of Allergy and Infectious Diseases, National Institutes of Health, Rockville, MD 20852, USA.
Blood. 2011 Dec 8;118(24):6332-41. doi: 10.1182/blood-2011-05-353102. Epub 2011 Sep 8.
Fc receptor-like 4 (FcRL4) is expressed on the surface of a subset of memory B cells (MBCs) located at sites of invading pathogens in mucosal lymphoid tissues in healthy individuals. Recently, FcRL4(+) MBCs were shown to be greatly increased in number in the peripheral blood of HIV-infected viremic individuals, in whom they are associated with B-cell exhaustion, and in individuals chronically reinfected with malaria. In the present study, we provide evidence that the expression of FcRL4 in human B-cell lines disrupts immune synapse formation and blocks antigen-induced BCR signaling at the point of Syk phosphorylation, blocking downstream activation of PLC-γ2 and Vav and the induction of calcium responses and CD69 expression. FcRL4 functions by ligation-independent mechanisms that require the 3 tyrosine residues in its cytoplasmic domain and involves its phosphorylation and association with the tyrosine phosphatases SHP-1 and SHP-2. Remarkably, FcRL4 is concentrated in endosomes after treatment with the TLR9 agonist CpG and enhances signaling through TLR9, as measured by increased expression of CD23. These findings suggest that FcRL4 may act as a molecular switch in B cells to dampen adaptive immune signaling and enhance innate signaling in response to chronic antigenic stimulation.
Fc 受体样蛋白 4(FcRL4)表达在健康个体黏膜淋巴组织中入侵病原体部位的记忆 B 细胞(MBC)亚群表面。最近,研究表明,HIV 感染病毒血症个体的外周血中 FcRL4(+)MBC 数量大量增加,与 B 细胞耗竭有关,并且与慢性疟疾再感染个体有关。在本研究中,我们提供的证据表明,FcRL4 在人 B 细胞系中的表达会破坏免疫突触的形成,并在 Syk 磷酸化处阻断抗原诱导的 BCR 信号转导,阻断下游 PLC-γ2 和 Vav 的激活以及钙反应和 CD69 表达的诱导。FcRL4 通过非依赖性配体结合机制发挥作用,该机制需要其细胞质结构域中的 3 个酪氨酸残基,并涉及磷酸化和与酪氨酸磷酸酶 SHP-1 和 SHP-2 的关联。值得注意的是,FcRL4 在 TLR9 激动剂 CpG 处理后集中在内涵体中,并增强 TLR9 的信号转导,如通过增加 CD23 的表达来衡量。这些发现表明,FcRL4 可作为 B 细胞中的分子开关,抑制适应性免疫信号转导,并增强对慢性抗原刺激的固有信号转导。
