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由MDP、LPS、PMA和MIF/MAF诱导的巨噬细胞迁移抑制:巨噬细胞迁移增强因子(MEF)、L-岩藻糖、L-岩藻糖基牛血清白蛋白、D-甘露糖和D-甘露糖基牛血清白蛋白可使其逆转。

Macrophage migration inhibition induced by MDP, LPS, PMA, and MIF/MAF: reversal by macrophage migration enhancement factor (MEF), L-fucose, L-fucosyl BSA, D-mannose, and D-mannosyl BSA.

作者信息

Gordon M R, Chida K, Takata I, Myrvik Q N

出版信息

J Leukoc Biol. 1987 Sep;42(3):197-203. doi: 10.1002/jlb.42.3.197.

Abstract

Our data establish that migration inhibition factor (MIF) and migration enhancement factor (MEF) mutually neutralize the effect of each other in a concentration-dependent manner. The monosaccharides L-fucose and D-mannose were also shown to reverse MIF and additionally to stimulate alveolar macrophage (AM) migration in the absence of MIF. The specific activity of these sugars was increased 200-fold when conjugated to bovine serum albumin (BSA). Macrophage activation is usually observed concurrently with migration inhibition when macrophages are incubated with MIF preparations. Migration inhibition occurred also when AM were incubated in the presence of known metabolic activators (MDP, PMA, and LPS). It was found that L-fucose, D-mannose, L-fucosyl BSA, and D-mannosyl BSA could reverse migration inhibition caused by MIF as well as by these metabolic activators. These observations suggest that reversal of MIF by L-fucose is unexplained solely on the basis that L-fucose is functioning as a competitive inhibitor; instead, they suggest that MEF and the above sugars and their conjugates stimulate AM through a receptor system different from the MIF receptor. These observations support the concept that MEF is an important macrophage modulator in CMI responses.

摘要

我们的数据表明,迁移抑制因子(MIF)和迁移增强因子(MEF)以浓度依赖的方式相互抵消彼此的作用。单糖L-岩藻糖和D-甘露糖也被证明可逆转MIF的作用,并且在没有MIF的情况下还能刺激肺泡巨噬细胞(AM)迁移。当与牛血清白蛋白(BSA)偶联时,这些糖的比活性增加了200倍。当巨噬细胞与MIF制剂一起孵育时,通常会同时观察到巨噬细胞活化和迁移抑制。当在已知的代谢激活剂(MDP、PMA和LPS)存在的情况下孵育AM时,也会发生迁移抑制。研究发现,L-岩藻糖、D-甘露糖、L-岩藻糖基BSA和D-甘露糖基BSA可以逆转由MIF以及这些代谢激活剂引起的迁移抑制。这些观察结果表明,L-岩藻糖对MIF的逆转不能仅仅基于L-岩藻糖作为竞争性抑制剂的作用来解释;相反,它们表明MEF以及上述糖类及其偶联物通过不同于MIF受体的受体系统刺激AM。这些观察结果支持了MEF是细胞介导免疫反应中重要的巨噬细胞调节剂这一概念。

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