Ogle J D, Noel J G, Balasurbramaniam A, Sramkoski R M, Ogle C K, Alexander J W
Department of Molecular Genetics, University of Cincinnati Medical Center, Ohio 45267.
Inflammation. 1990 Apr;14(2):185-94. doi: 10.1007/BF00917457.
Both recombinant IL-1 alpha and -beta caused an upregulation of C3b receptors (CR1) on human neutrophils and caused a receptor-mediated enhancement of phagocytosis of C3b.IgG-coated microspheres by these leukocytes. The alpha and beta forms of the recombinant cytokine were of comparable potency regarding CR1 upregulation, although both generally had less than 25% of the potency of FMLP in this respect. Recombinant IL-1 beta was slightly more potent than the alpha form of the cytokine regarding phagocytosis of opsonized microspheres and, again, both forms were less potent than FMLP in causing an enhancement of phagocytosis by neutrophils. The synthetic noninflammatory immunostimulatory nonapeptide corresponding to residues 163-171 of IL-1 beta was completely inert with respect to upregulation of CR1 on neutrophils and the enhancement of phagocytosis by these cells. Thus this domain in the intact IL-1 beta molecule apparently is not involved in CR1 upregulation and the ensuing enhancement in phagocytosis by neutrophils, although it is apparently important in the immunostimulatory activity regarding the proliferation of lymphocytes.
重组白细胞介素-1α和 -β均能使人类中性粒细胞上的C3b受体(CR1)上调,并通过这些白细胞引起受体介导的对C3b.IgG包被微球吞噬作用的增强。重组细胞因子的α和β形式在CR1上调方面具有相当的效力,尽管在这方面两者通常都只有甲酰甲硫氨酸-亮氨酸-苯丙氨酸(FMLP)效力的不到25%。就调理素化微球的吞噬作用而言,重组白细胞介素-1β比细胞因子的α形式略强,而且同样,两种形式在引起中性粒细胞吞噬作用增强方面都比FMLP效力低。对应于白细胞介素-1β 163 - 171位残基的合成非炎性免疫刺激九肽在中性粒细胞CR1上调以及这些细胞吞噬作用增强方面完全无活性。因此,完整白细胞介素-1β分子中的该结构域显然不参与CR1上调以及随后中性粒细胞吞噬作用的增强,尽管它在关于淋巴细胞增殖的免疫刺激活性方面显然很重要。
