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TFH-derived dopamine accelerates productive synapses in germinal centres

机译:TFH衍生的多巴胺可促进生发中心的生产性突触

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摘要

Protective high-affinity antibody responses depend on competitive selection of B cells carrying somatically mutated B-cell receptors by follicular helper T (TFH) cells in germinal centres. The rapid T-B-cell interactions that occur during this process are reminiscent of neural synaptic transmission pathways. Here we show that a proportion of human TFH cells contain dense-core granules marked by chromogranin B, which are normally found in neuronal presynaptic terminals storing catecholamines such as dopamine. TFH cells produce high amounts of dopamine and release it upon cognate interaction with B cells. Dopamine causes rapid translocation of intracellular ICOSL (inducible T-cell co-stimulator ligand, also known as ICOSLG) to the B-cell surface, which enhances accumulation of CD40L and chromogranin B granules at the human TFH cell synapse and increases the synapse area. Mathematical modelling suggests that faster dopamine-induced T-B-cell interactions increase total germinal centre output and accelerate it by days. Delivery of neurotransmitters across the T-B-cell synapse may be advantageous in the face of infection.
机译:保护性高亲和力抗体反应取决于生发中心的滤泡辅助性T(TFH)细胞对携带体细胞突变B细胞受体的B细胞的竞争选择。在此过程中发生的快速T-B细胞相互作用使人联想到神经突触传递途径。在这里,我们显示一部分人类TFH细胞含有以嗜铬粒蛋白B标记的致密颗粒,通常在储存儿茶酚胺(如多巴胺)的神经元突触前末端中发现。 TFH细胞产生大量的多巴胺,并在与B细胞发生同源相互作用后释放。多巴胺会导致细胞内ICOSL(诱导性T细胞共刺激配体,也称为ICOSLG)快速转移至B细胞表面,从而增强CD40L和嗜铬粒蛋白B颗粒在人TFH细胞突触处的蓄积并增加突触区域。数学模型表明,更快的多巴胺诱导的T-B细胞相互作用增加了生发中心的总输出量,并加快了几天的速度。面对感染,跨T-B细胞突触传递神经递质可能是有利的。

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