Department of Cell and Developmental Biology, Sackler Faculty of Medicine, Tel Aviv University, Tel Aviv, Israel.
Department of Basic and Translational Sciences, School of Dental Medicine, University of Pennsylvania, Philadelphia, PA, United States.
Front Immunol. 2022 Jun 28;13:892239. doi: 10.3389/fimmu.2022.892239. eCollection 2022.
MRGPRX2, the human member of the MAS-related G protein coupled receptors (Mrgprs), serves as the cellular target of human mast cells (MCs) for innate ligands, including neuropeptides and antimicrobial peptides. In addition, MRGPRX2 also functions as the receptor for multiple FDA-approved drugs. As such, MRGPRX2 is a mediator of MC responses in neurogenic inflammation, host defense and pseudoallergy. We analyzed the spatiotemporal patterns of MRGPRX2 following its binding of the neuropeptide substance P (SP). Herein, we show that MRGPRX2 internalizes both endocytosis and macropinocytosis, followed by its distribution between a perinuclear region and the secretory granules (SGs). Further, we show that MRGPRX2-containing macropinosomes undergo resolution by a mechanism that involves dynamin and LC3, giving rise to the incorporation of both LC3 and MRGPRX2 into the SGs. SP then promotes the acidification of the LC3-associated SGs, presumably by stimulating their fusion with lysosomes. Taken together, our results reveal a unique mode of MRGPRX2 trafficking that complements endocytosis and involves macropinocytosis, autophagic machinery-assisted macropinosome resolution and receptor delivery to the SGs.
MRGPRX2 是人类 MAS 相关 G 蛋白偶联受体 (Mrgprs) 家族的成员,是人类肥大细胞 (MCs) 天然配体的细胞靶标,包括神经肽和抗菌肽。此外,MRGPRX2 还作为多种 FDA 批准药物的受体发挥作用。因此,MRGPRX2 是神经源性炎症、宿主防御和假性过敏反应中 MC 反应的介质。我们分析了 MRGPRX2 与其结合后的神经肽物质 P (SP) 的时空模式。在此,我们表明 MRGPRX2 同时通过内吞作用和巨胞饮作用内化,然后在核周区域和分泌颗粒 (SGs) 之间分布。此外,我们表明含有 MRGPRX2 的巨胞饮体通过涉及 dynamin 和 LC3 的机制进行解析,导致 LC3 和 MRGPRX2 都被纳入 SGs。SP 随后促进 LC3 相关 SGs 的酸化,推测通过刺激它们与溶酶体融合来实现。总之,我们的结果揭示了一种独特的 MRGPRX2 运输模式,它补充了内吞作用,并涉及巨胞饮作用、自噬机制辅助的巨胞饮体解析以及受体递送至 SGs。
