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浆细胞样树突状细胞产生细胞因子,并在对Toll样受体7激动剂咪喹莫特和瑞喹莫特的反应中成熟。

Plasmacytoid dendritic cells produce cytokines and mature in response to the TLR7 agonists, imiquimod and resiquimod.

作者信息

Gibson Sheila J, Lindh Jana M, Riter Tony R, Gleason Raymond M, Rogers Lisa M, Fuller Ashley E, Oesterich JoAnn L, Gorden Keith B, Qiu Xiaohong, McKane Scott W, Noelle Randy J, Miller Richard L, Kedl Ross M, Fitzgerald-Bocarsly Patricia, Tomai Mark A, Vasilakos John P

机构信息

Department of Pharmacology, 3M Pharmaceuticals, 3M Center, 270-2S-06, St. Paul, MN 55144-1000, USA.

出版信息

Cell Immunol. 2002 Jul-Aug;218(1-2):74-86. doi: 10.1016/s0008-8749(02)00517-8.

Abstract

The immune response modifiers, imiquimod and resiquimod, are TLR7 agonists that induce type I interferon in numerous species, including humans. Recently, it was shown that plasmacytoid dendritic cells (pDC) are the primary interferon-producing cells in the blood in response to viral infections. Here, we characterize the activation of human pDC with the TLR7 agonists imiquimod and resiquimod. Results indicate that imiquimod and resiquimod induce IFN-alpha and IFN-omega from purified pDC, and pDC are the principle IFN-producing cells in the blood. Resiquimod-stimulated pDC also produce a number of other cytokines including TNF-alpha and IP-10. Resiquimod enhances co-stimulatory marker expression, CCR7 expression, and pDC viability. Resiquimod was compared throughout the study to the pDC survival factors, IL-3 and IFN-alpha; resiquimod more effectively matures pDC than either IL-3 or IFN-alpha alone. These results demonstrate that imidazoquinoline molecules directly induce pDC maturation as determined by cytokine induction, CCR7 and co-stimulatory marker expression and prolonging viability.

摘要

免疫反应调节剂咪喹莫特和瑞喹莫特是Toll样受体7(TLR7)激动剂,可在包括人类在内的众多物种中诱导I型干扰素产生。最近有研究表明,浆细胞样树突状细胞(pDC)是血液中对病毒感染产生应答的主要干扰素产生细胞。在此,我们对咪喹莫特和瑞喹莫特这两种TLR7激动剂激活人pDC的情况进行了表征。结果表明,咪喹莫特和瑞喹莫特可从纯化的pDC诱导产生IFN-α和IFN-ω,且pDC是血液中主要的干扰素产生细胞。瑞喹莫特刺激的pDC还会产生包括TNF-α和IP-10在内的多种其他细胞因子。瑞喹莫特可增强共刺激标志物表达、CCR7表达以及pDC的活力。在整个研究过程中,将瑞喹莫特与pDC存活因子IL-3和IFN-α进行了比较;瑞喹莫特比单独使用IL-3或IFN-α更有效地使pDC成熟。这些结果表明,咪唑喹啉分子可通过细胞因子诱导、CCR7和共刺激标志物表达以及延长活力来直接诱导pDC成熟。

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