Cancer and Inflammation Program, Center for Cancer Research, NCI-Frederick, National Institutes of Health, Frederick, Maryland 21702, USA.
J Biol Chem. 2010 Jan 29;285(5):2976-85. doi: 10.1074/jbc.M109.038398. Epub 2009 Nov 30.
Triggering receptor expressed on myeloid cells-2 (TREM-2) is rapidly emerging as a key regulator of the innate immune response via its regulation of macrophage inflammatory responses. Here we demonstrate that proximal TREM-2 signaling parallels other DAP12-based receptor systems in its use of Syk and Src-family kinases. However, we find that the linker for activation of T cells (LAT) is severely reduced as monocytes differentiate into macrophages and that TREM-2 exclusively uses the linker for activation of B cells (LAB encoded by the gene Lat2(-/-)) to mediate downstream signaling. LAB is required for TREM-2-mediated activation of Erk1/2 and dampens proximal TREM-2 signals through a novel LAT-independent mechanism resulting in macrophages with proinflammatory properties. Thus, Lat2(-/-) macrophages have increased TREM-2-induced proximal phosphorylation, and lipopolysaccharide stimulation of these cells leads to increased interleukin-10 (IL-10) and decreased IL-12p40 production relative to wild type cells. Together these data identify LAB as a critical, LAT-independent regulator of TREM-2 signaling and macrophage development capable of controlling subsequent inflammatory responses.
髓系细胞触发受体 2(TREM-2)作为先天免疫反应的关键调节因子,通过调节巨噬细胞炎症反应而迅速成为研究热点。在这里,我们证明了近端 TREM-2 信号与其他基于 DAP12 的受体系统一样,使用 Syk 和 Src 家族激酶。然而,我们发现,随着单核细胞分化为巨噬细胞,T 细胞激活连接蛋白(LAT)严重减少,而 TREM-2 仅使用 B 细胞激活连接蛋白(LAB,由 Lat2(-/-)基因编码)来介导下游信号。LAB 是 TREM-2 介导的 Erk1/2 激活所必需的,通过一种新的不依赖 LAT 的机制来抑制近端 TREM-2 信号,导致具有促炎特性的巨噬细胞。因此,Lat2(-/-)巨噬细胞中 TREM-2 诱导的近端磷酸化增加,与野生型细胞相比,这些细胞中脂多糖的刺激导致白细胞介素 10(IL-10)增加和白细胞介素 12p40 减少。这些数据共同表明,LAB 是 TREM-2 信号和巨噬细胞发育的关键、不依赖 LAT 的调节剂,能够控制随后的炎症反应。
