Single-cell topographical profiling of the immune synapse reveals a biomechanical signature of cytotoxicity

细胞毒性 免疫系统 生物 免疫突触 细胞毒性T细胞 突触 细胞骨架 神经科学 细胞 细胞生物学 免疫学 T细胞 遗传学 体外 T细胞受体
作者
Miguel de Jesús,Alexander Settle,Daan Vorselen,Thomas K. Gaetjens,Michael Galiano,Yevgeniy Romin,E Hui Clarissa Lee,Yung Yu Wong,Tian-Ming Fu,Endi K. Santosa,Benjamin Y. Winer,Fella Tamzalit,Mitchell S. Wang,Anthony Santella,Zhirong Bao,Joseph C. Sun,Pavak K. Shah,Julie A. Theriot,Steven M. Abel,Morgan Huse
出处
期刊:Science immunology [American Association for the Advancement of Science (AAAS)]
卷期号:9 (96) 被引量:1
标识
DOI:10.1126/sciimmunol.adj2898
摘要

Immune cells have intensely physical lifestyles characterized by structural plasticity and force exertion. To investigate whether specific immune functions require stereotyped mechanical outputs, we used super-resolution traction force microscopy to compare the immune synapses formed by cytotoxic T cells with contacts formed by other T cell subsets and by macrophages. T cell synapses were globally compressive, which was fundamentally different from the pulling and pinching associated with macrophage phagocytosis. Spectral decomposition of force exertion patterns from each cell type linked cytotoxicity to compressive strength, local protrusiveness, and the induction of complex, asymmetric topography. These features were validated as cytotoxic drivers by genetic disruption of cytoskeletal regulators, live imaging of synaptic secretion, and in silico analysis of interfacial distortion. Synapse architecture and force exertion were sensitive to target stiffness and size, suggesting that the mechanical potentiation of killing is biophysically adaptive. We conclude that cellular cytotoxicity and, by implication, other effector responses are supported by specialized patterns of efferent force.
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