胶原诱导人血单核细胞释放白细胞介素1。纤连蛋白与α5β1整合素结合的增强作用。
Collagen-induced release of interleukin 1 from human blood mononuclear cells. Potentiation by fibronectin binding to the alpha 5 beta 1 integrin.
作者信息
Pacifici R, Basilico C, Roman J, Zutter M M, Santoro S A, McCracken R
机构信息
Division of Endocrinology and Bone Metabolism, Jewish Hospital of St. Louis, Washington University Medical Center, MO 63110, USA.
出版信息
J Clin Invest. 1992 Jan;89(1):61-7. doi: 10.1172/JCI115586.
PBMC express cell surface receptors for extracellular matrix components known as integrins. We have recently shown that ligand binding to one PBMC integrin, the collagen receptor alpha 2 beta 1, stimulates the secretion of interleukin 1 (IL-1). We have now investigated the role of fibronectin (Fn), an adherence protein that has binding sites for both PBMC and collagen, in the generation of the IL-1 response to collagen. In contrast to collagen, Fn did not stimulate IL-1 release but Fn-depleted serum decreased the release of IL-1 induced by collagen. A polyclonal antiserum directed against Fn also decreased the collagen-induced IL-1 secretion. The IL-1 response to collagen from cells incubated in Fn-depleted serum was restored by the addition of either purified Fn or the 120-kD cell-binding fragment of Fn, which contains the cell-binding site but not the collagen-binding domain. Smaller Arg-Gly-Asp (RGD) peptides failed to enhance the PBMC response to collagen but inhibited in a concentration-dependent fashion the potentiating effect Fn. As expected, a MAb against the alpha 2 beta 1 collagen receptor decreased collagen-induced IL-1 release. However collagen-induced IL-1 release was also inhibited by a MAb against the alpha 5 beta 1 Fn receptor. The effect of the two MAbs was not additive, suggesting that the occupancy of both receptors by ligands is required in order for collagen to induce an maximal response from PBMC. The mechanism by which Fn exerts its effect remains unknown. However, flow-cytometric analysis revealed that Fn does not alter expression of the alpha2beta1 receptor on PBMC. These data demonstrate a potentiating effect of Fn on the collagen-induced secretion of IL-1 from human PBMC and suggest that this effect is mediated via the integrin alpha5beta1. These findings indicate a complex interactive role for specific integrin receptors in the regulation of the mononuclear cell immune response.
外周血单核细胞(PBMC)表达细胞表面受体,这些受体针对细胞外基质成分,即整合素。我们最近发现,配体与一种PBMC整合素(胶原受体α2β1)结合会刺激白细胞介素1(IL-1)的分泌。我们现在研究了纤连蛋白(Fn)在对胶原的IL-1反应产生过程中的作用,Fn是一种黏附蛋白,对PBMC和胶原都有结合位点。与胶原不同,Fn不会刺激IL-1释放,但去除Fn的血清会降低胶原诱导的IL-1释放。一种针对Fn的多克隆抗血清也会降低胶原诱导的IL-1分泌。在去除Fn的血清中培养的细胞对胶原的IL-1反应,通过添加纯化的Fn或Fn的120-kD细胞结合片段得以恢复,该片段包含细胞结合位点但不包含胶原结合结构域。较小的精氨酸-甘氨酸-天冬氨酸(RGD)肽未能增强PBMC对胶原的反应,但以浓度依赖的方式抑制了Fn的增强作用。正如预期的那样,一种针对α2β1胶原受体的单克隆抗体(MAb)会降低胶原诱导的IL-1释放。然而,针对α5β1 Fn受体的MAb也会抑制胶原诱导的IL-1释放。这两种MAb的作用并非相加的,这表明配体占据这两种受体是胶原诱导PBMC产生最大反应所必需的。Fn发挥其作用的机制仍然未知。然而,流式细胞术分析显示,Fn不会改变PBMC上α2β1受体的表达。这些数据证明了Fn对人PBMC胶原诱导的IL-1分泌有增强作用,并表明这种作用是通过整合素α5β1介导的。这些发现表明特定整合素受体在调节单核细胞免疫反应中具有复杂的相互作用作用。
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