Ma Bing, Zhu Zhou, Homer Robert J, Gerard Craig, Strieter Robert, Elias Jack A
Section of Pulmonary and Critical Care Medicine, Department of Internal Medicine, Yale University School of Medicine, New Haven, CT 06520, USA.
J Immunol. 2004 Feb 1;172(3):1872-81. doi: 10.4049/jimmunol.172.3.1872.
IL-13 is a potent stimulator of inflammation and tissue remodeling that plays a key role in the pathogenesis of a wide variety of human disorders. To further understand these responses, studies were undertaken to define the role(s) of the chemokine C10/CCL6 in the pathogenesis of IL-13-induced alterations in the murine lung. IL-13 was a very potent stimulator of C10/CCL6 mRNA and protein, and IL-13-induced inflammation, alveolar remodeling, and compliance alterations were markedly ameliorated after C10/CCL6 neutralization. Treatment with anti-C10/CCL6 decreased the levels of mRNA encoding matrix metalloproteinase-2 (MMP-2), MMP-9, and tissue inhibitor of metalloproteinase-4 (TIMP-4) in lungs from wild-type mice. C10/CCL6 neutralization also decreased the ability of IL-13 to stimulate the production of monocyte chemoattractant protein-1, macrophage inflammatory protein-1alpha, MMP-2, MMP-9, and cathepsins-K, -L, and -S and the ability of IL-13 to inhibit alpha1-antitrypsin. In accord with these findings, a targeted null mutation of CCR1, a putative C10/CCL6 receptor, also decreased IL-13-induced inflammation and alveolar remodeling and caused alterations in chemokines, proteases, and antiproteases comparable to those seen after C10/CCL6 neutralization. These C10/CCL6 and CCR1 manipulations did not alter the production of transgenic IL-13. These studies demonstrate that IL-13 is a potent stimulator of C10/CCL6 and highlight the importance of C10/CCL6 and signaling via CCR1 in the pathogenesis of the IL-13-induced pulmonary phenotype. They also describe a C10/CCL6 target gene cascade in which C10/CCL6 induction is required for optimal IL-13 stimulation of selected chemokines (monocyte chemoattractant protein-1 and MIP-1alpha) and proteases (MMP-2, MMP-9, and cathepsins-K, -L, and -S) and the inhibition of alpha1-antitrypsin.
白细胞介素-13是炎症和组织重塑的强效刺激因子,在多种人类疾病的发病机制中起关键作用。为了进一步了解这些反应,开展了相关研究以确定趋化因子C10/CCL6在白细胞介素-13诱导的小鼠肺部改变发病机制中的作用。白细胞介素-13是C10/CCL6信使核糖核酸和蛋白质的强效刺激因子,在C10/CCL6中和后,白细胞介素-13诱导的炎症、肺泡重塑及顺应性改变均得到显著改善。用抗C10/CCL6治疗可降低野生型小鼠肺中编码基质金属蛋白酶-2(MMP-2)、基质金属蛋白酶-9和金属蛋白酶组织抑制剂-4(TIMP-4)的信使核糖核酸水平。C10/CCL6中和还降低了白细胞介素-13刺激单核细胞趋化蛋白-1、巨噬细胞炎性蛋白-1α、MMP-2、MMP-9以及组织蛋白酶-K、-L和-S产生的能力,以及白细胞介素-13抑制α1-抗胰蛋白酶的能力。与这些发现一致,假定的C10/CCL6受体CCR1的靶向无效突变也减少了白细胞介素-13诱导的炎症和肺泡重塑,并导致趋化因子、蛋白酶和抗蛋白酶的改变,与C10/CCL6中和后所见的改变相似。这些对C10/CCL6和CCR1的操作并未改变转基因白细胞介素-13的产生。这些研究表明白细胞介素-13是C10/CCL6的强效刺激因子,并突出了C10/CCL6以及通过CCR1信号传导在白细胞介素-13诱导的肺部表型发病机制中的重要性。它们还描述了一个C10/CCL6靶基因级联反应,其中C10/CCL6的诱导是白细胞介素-13对选定趋化因子(单核细胞趋化蛋白-1和MIP-1α)和蛋白酶(MMP-2、MMP-9以及组织蛋白酶-K、-L和-S)进行最佳刺激以及抑制α1-抗胰蛋白酶所必需的。
