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在前列腺素E2存在的情况下,从外周血前体细胞中获得的树突状细胞可促进Th2反应。

Dendritic cells, obtained from peripheral blood precursors in the presence of PGE2, promote Th2 responses.

作者信息

Kaliński P, Hilkens C M, Snijders A, Snijdewint F G, Kapsenberg M L

机构信息

Department of Cell Biology and Histology, University of Amsterdam, The Netherlands.

出版信息

Adv Exp Med Biol. 1997;417:363-7. doi: 10.1007/978-1-4757-9966-8_59.

Abstract

In order to investigate the impact of an inflammatory mediator PGE2 on the functions of maturing DC we used an in vitro model of DC generation from peripheral blood monocytes. Addition of PGE2 (10(-9) M-10(-6) M) to the cultures performed in the presence of GM-CSF and IL-4 did not alter the morphology nor high levels of expression of class II MHC and co-stimulatory molecules on arising DC, although at concentrations above 10(-8) M, the acquisition of CD1a was selectively prevented. Control DC and the DC maturing in the presence of PGE2 (PGE2-DC) induced a similar proliferation of naive Th cells. Control DC produced high amounts of IL-12, and only trace amounts of IL-10, whereas PGE2-DC produced no IL-12 and high levels of IL-10, when stimulated after the removal of PGE2. The deficient IL-12 production by PGE2-DC was observed after stimulation both in the absence and in the presence of IFN gamma, and was not compensated during further 48 h culture in the absence of PGE2. Compared to control DC, PGE2-DC induced development of Th cells secreting elevated amounts of IL-4 and IL-5, from naive precursors. These data indicate that elevated tissue levels of PGE2 may promote type 2 Th responses by impairing the ability of locally maturing DC to produce IL-12. Since Th2 responses mediate protection in Th1-related autoimmune disorders, the use of PGE2-DC in immunotherapy of such disorders may be considered.

摘要

为了研究炎性介质前列腺素E2(PGE2)对成熟树突状细胞(DC)功能的影响,我们使用了一种从外周血单核细胞生成DC的体外模型。在存在粒细胞-巨噬细胞集落刺激因子(GM-CSF)和白细胞介素-4(IL-4)的情况下进行培养时,添加PGE2(10^(-9) M - 10^(-6) M)不会改变所产生DC的形态,也不会改变其II类主要组织相容性复合体(MHC)和共刺激分子的高表达水平,尽管在浓度高于10^(-8) M时,CD1a的获得会被选择性地阻止。对照DC和在PGE2存在下成熟的DC(PGE2-DC)诱导幼稚Th细胞发生相似的增殖。对照DC产生大量的IL-12,仅产生微量的IL-10,而去除PGE2后受到刺激时,PGE2-DC不产生IL-12且产生高水平的IL-10。在不存在和存在干扰素γ(IFNγ)的情况下刺激后,均观察到PGE2-DC产生IL-12不足,并且在不存在PGE2的情况下进一步培养48小时也未得到补偿。与对照DC相比,PGE2-DC从幼稚前体诱导分泌升高量的IL-4和IL-5的Th细胞发育。这些数据表明,组织中升高的PGE2水平可能通过损害局部成熟DC产生IL-12的能力来促进2型Th反应。由于Th2反应在与Th1相关的自身免疫性疾病中介导保护作用,因此可以考虑将PGE2-DC用于此类疾病的免疫治疗。

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