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胞壁酰二肽(MDP)分别与白细胞介素2和白细胞介素4协同作用,以刺激B细胞的分化和增殖。

Muramyl dipeptide (MDP) synergizes with interleukin 2 and interleukin 4 to stimulate, respectively, the differentiation and proliferation of B cells.

作者信息

Souvannavong V, Brown S, Adam A

机构信息

CNRS UA 1116, Institut de Biochimie, Université Paris-Sud, Orsay, France.

出版信息

Cell Immunol. 1990 Mar;126(1):106-16. doi: 10.1016/0008-8749(90)90304-a.

Abstract

The synthetic immunomodulator muramyldipeptide (MDP) can stimulate B cells. MDP, when used alone, was apparently unable to induce the differentiation or proliferation of resting B cells. In contrast, MDP appeared to synergize with a single recombinant interleukin (IL) to stimulate either their differentiation or proliferation. We used single interleukins to avoid synergistic and antagonistic effects inherent in the use of several factors. IL-2 was found to be sufficient to restore the specific immune response of resting B cells to sheep erythrocytes; MDP greatly increased the number of plaque-forming cells of such IL-2-stimulated B cells. In contrast, IL-4 and interferon-gamma (IFN-gamma), either alone or in the presence of MDP, had no effect in this differentiation assay. MDP was also able to stimulate polyclonally activated B cells. IL-4 increased the proliferation of anti-IgM-stimulated B cells, leading to enlargement and driving more cells into the cell cycle; these effects were further enhanced by MDP, more cells being induced to proliferate, to enlarge, and to progress into the cycle with a higher frequency of cells in the G1B, S, and G2/M compartments. Intracellular free calcium levels were not increased by IL-4 and/or MDP, and the two compounds did not modify the anti-IgM-induced calcium mobilization. Therefore, MDP appears to amplify cytokine effects in B cell activation, by a mechanism which does not appear to involve free calcium mobilization.

摘要

合成免疫调节剂胞壁酰二肽(MDP)可刺激B细胞。单独使用时,MDP显然无法诱导静息B细胞的分化或增殖。相比之下,MDP似乎能与单一重组白细胞介素(IL)协同作用,刺激其分化或增殖。我们使用单一白细胞介素以避免使用多种因子时固有的协同和拮抗作用。发现IL-2足以恢复静息B细胞对绵羊红细胞的特异性免疫反应;MDP大大增加了此类IL-2刺激的B细胞中形成空斑细胞的数量。相比之下,IL-4和干扰素-γ(IFN-γ),无论是单独使用还是在MDP存在的情况下,在这种分化试验中均无作用。MDP还能够刺激多克隆激活的B细胞。IL-4增加了抗IgM刺激的B细胞的增殖,导致细胞增大并促使更多细胞进入细胞周期;MDP进一步增强了这些效应,诱导更多细胞增殖、增大,并以更高频率的细胞进入G1B、S和G2/M期。IL-4和/或MDP未增加细胞内游离钙水平,且这两种化合物未改变抗IgM诱导的钙动员。因此,MDP似乎通过一种似乎不涉及游离钙动员的机制,在B细胞激活中放大细胞因子效应。

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