不依赖受体的直接膜结合导致树突状细胞中的细胞表面脂质分选和Syk激酶激活。
Receptor-independent, direct membrane binding leads to cell-surface lipid sorting and Syk kinase activation in dendritic cells.
作者信息
Ng Gilbert, Sharma Karan, Ward Sandra M, Desrosiers Melanie D, Stephens Leslie A, Schoel W Michael, Li Tonglei, Lowell Clifford A, Ling Chang-Chun, Amrein Matthias W, Shi Yan
机构信息
Department of Microbiology and Infectious Diseases, Immunology Research Group, University of Calgary, Calgary, Alberta T2N 4N1, Canada.
出版信息
Immunity. 2008 Nov 14;29(5):807-18. doi: 10.1016/j.immuni.2008.09.013.
Abstract
Binding of particulate antigens by antigen-presenting cells is a critical step in immune activation. Previously, we demonstrated that uric acid crystals are potent adjuvants, initiating a robust adaptive immune response. However, the mechanisms of activation are unknown. By using atomic force microscopy as a tool for real-time single-cell activation analysis, we report that uric acid crystals could directly engage cellular membranes, particularly the cholesterol components, with a force substantially stronger than protein-based cellular contacts. Binding of particulate substances activated Syk kinase-dependent signaling in dendritic cells. These observations suggest a mechanism whereby immune cell activation can be triggered by solid structures via membrane lipid alteration without the requirement for specific cell-surface receptors, and a testable hypothesis for crystal-associated arthropathies, inflammation, and adjuvanticity.
摘要
抗原呈递细胞与颗粒性抗原的结合是免疫激活中的关键步骤。此前,我们证明尿酸晶体是强效佐剂,可引发强烈的适应性免疫反应。然而,激活机制尚不清楚。通过使用原子力显微镜作为实时单细胞激活分析工具,我们报告尿酸晶体可直接与细胞膜结合,特别是胆固醇成分,其作用力明显强于基于蛋白质的细胞接触。颗粒物质的结合激活了树突状细胞中Syk激酶依赖性信号传导。这些观察结果提示了一种机制,即免疫细胞激活可由固体结构通过膜脂质改变触发,而无需特定的细胞表面受体,这也为晶体相关的关节病、炎症和佐剂作用提供了一个可检验的假说。
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