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Hydroxychloroquine inhibits proteolytic processing of endogenous TLR7 protein in human primary plasmacytoid dendritic cells

机译:羟氯喹抑制蛋白水解处理人类主要的内源性TLR7蛋白质血浆树突细胞

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摘要

Toll-like receptor 7 (TLR7) triggers antiviral immune responses through its capacity to recognize ssRNA. Proteolytic cleavage of TLR7 protein is required for its functional maturation in the endosomal compartment. Structural studies demonstrated that the N- and C-terminal domains of TLR7 are connected and involved in ligand binding after cleavage. Hydroxychloroquine (HCQ), an antimalarial drug, has been studied for its antiviral effects. HCQ increases pH in acidic organelles and has been reported to potently inhibit endosomal TLR activation. Whether HCQ can prevent endogenous TLR7 cleavage in primary immune cells, such as plasmacytoid DCs (pDCs), had never been examined. Here, using a validated anti-TLR7 antibody suitable for biochemical detection of native TLR7 protein, we show that HCQ treatment of fresh PBMCs, CAL-1 leukemic, and primary human pDCs inhibits TLR7 cleavage and results in accumulation of full-length protein. As a consequence, we observe an inhibition of pDC activation in response to TLR7 stimulation with synthetic ligands and viruses including inactivated SARS-CoV2, which we show herein activates pDCs through TLR7-signaling. Together, our finding suggests that the major pathway by which HCQ inhibits ssRNA sensing by pDCs may rely on its capacity to inhibit endosomal acidification and the functional maturation of TLR7 protein.
机译:toll样受体7 (TLR7)触发抗病毒免疫反应能力认识ssRNA。蛋白质是其所需功能成熟在endosomal隔间。证明了N -和c端域TLR7连接和参与配位卵裂后绑定。一个抗疟药物,研究其抗病毒效果。细胞器,据报道有说服力地抑制endosomal TLR激活。防止主要内生TLR7乳沟免疫细胞,如血浆DCs(髓样)从来没有检查。anti-TLR7抗体适用于生化本机TLR7蛋白质的检测,我们证明HCQ治疗新鲜PBMCs CAL-1白血病,主要人类pDCs抑制TLR7乳沟和导致全身蛋白质的积累。因此,我们观察一个抑制pDC在TLR7刺激激活合成配体和病毒等灭活SARS-CoV2,我们展示通过TLR7-signaling激活的髓。我们的发现表明,主要的途径HCQ抑制ssRNA传感的髓样可以依赖吗在其抑制endosomal的能力酸化和的功能成熟TLR7蛋白质。

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