首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >B7-DC cross-linking restores antigen uptake and augments antigen-presenting cell function by matured dendritic cells
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B7-DC cross-linking restores antigen uptake and augments antigen-presenting cell function by matured dendritic cells

机译:B7-DC交联通过成熟的树突状细胞恢复抗原摄取并增强抗原呈递细胞的功能

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Dendritic cells (DCs) are classified in two states: immature DCs (iDCs), which perform sentinel functions, sampling for antigen and danger signals, and mature DCs (mDCs), which exhibit enhanced antigen-presenting functions but are no longer capable of acquiring antigen. We now describe DCs with a different activation phenotype: cells having the strong antigen-presenting functions of mDCs and the antigen-acquiring functions of iDCs. We have described an antibody that binds the costimulatory molecule B7-DC and activates DCs. The resulting phenotype is distinct from iDCs or mDCs matured by using Toll-like receptor (TLR) agonists. Ability to take up antigen increases, while expression of B71/2 costimulatory and MHC molecules remains unchanged. DCs matured with TLR agonists and then superactivated through B7-DC exhibit a previously unrecognized phenotype. These DCs recover the ability to take up antigen, which is normally lost after treatment with TLR-3 and TLR-9 agonists, yet retain the high expression of costimulatory and MHC molecules and strong antigen-presenting functions of mDCs. Immunization using TLR agonists and B7-DC XAb (cross-linking antibody) together as adjuvant resulted in substantially increased cytolytic T cell responses, particularly when minimal peptide antigens were used. By stimulating DCs with two distinct activation signals, a previously unrecognized phenotype exhibiting augmented antigen-presenting functions was obtained.
机译:树突状细胞(DC)分为两种状态:执行前哨功能的未成熟DC(iDC),对抗原和危险信号进行采样以及表现出增强的抗原呈递功能但不再能够获得抗原的成熟DC(mDC)抗原。现在我们描述具有不同激活表型的DC:具有mDC的强抗原呈递功能和iDC的抗原获得功能的细胞。我们已经描述了结合共刺激分子B7-DC并激活DC的抗体。产生的表型不同于使用Toll样受体(TLR)激动剂成熟的iDC或mDC。吸收抗原的能力增加,而B71 / 2共刺激分子和MHC分子的表达保持不变。 DCs用TLR激动剂成熟,然后通过B7-DC超活化,表现出以前无法识别的表型。这些DC恢复了吸收抗原的能力,而抗原通常在用TLR-3和TLR-9激动剂治疗后会丢失,但仍保留了共刺激分子和MHC分子的高表达以及mDC强大的抗原呈递功能。使用TLR激动剂和B7-DC XAb(交联抗体)一起作为佐剂进行免疫可显着提高细胞溶解性T细胞反应,尤其是在使用最少的肽抗原时。通过用两个不同的激活信号刺激DC,获得了先前无法识别的表现出增强的抗原呈递功能的表型。

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