Topham P S, Csizmadia V, Soler D, Hines D, Gerard C J, Salant D J, Hancock W W
LeukoSite Inc., Cambridge, Massachusetts 02142, USA.
J Clin Invest. 1999 Dec;104(11):1549-57. doi: 10.1172/JCI7707.
During the development of nephrotoxic nephritis (NTN) in the mouse, we find that a variety of chemokines and chemokine receptors are induced: CCR1 (RANTES, MIP-1alpha), CCR2 (MCP-1), CCR5 (RANTES, MIP-1alpha, MIP-1beta), CXCR2 (MIP-2), and CXCR3 (IP-10). Their timing of expression indicated that CXCR2 and CCR1 are probably important in the neutrophil-dependent heterologous phase of the disease, whereas CCR1, CCR2, CCR5, and CXCR3 accompany the subsequent mononuclear cell infiltration characteristic of autologous disease. We therefore assessed the role of CCR1 in NTN using CCR1(-/-) mice. We found that neutrophil accumulation in CCR1(-/-) mice was comparable to that in wild-type animals but that renal recruitment of CD4(+) and CD8(+) T cells and macrophages increased significantly. Moreover, CCR1(-/-) mice developed more severe glomerulonephritis than did controls, with greater proteinuria and blood urea nitrogen, as well as a higher frequency of crescent formation. In addition, CCR1(-/-) mice showed enhanced Th1 immune responses, including titers of antigen-specific IgG2a antibody, delayed-type hypersensitivity responses, and production of IFN-gamma and TNF-alpha. Lastly, using recombinant proteins and transfected cells that overexpressed CCR1, we demonstrated that MIP-1alpha, but not RANTES, bound CCR1 and induced cell chemotaxis. Thus, rather than simply promoting leukocyte recruitment during NTN, CCR1 expression profoundly alters the effector phase of glomerulonephritis. Therapeutic targeting of chemokine receptors may, on occasion, exacerbate underlying disease.
在小鼠肾毒性肾炎(NTN)的发展过程中,我们发现多种趋化因子和趋化因子受体被诱导表达:CCR1(RANTES、MIP-1α)、CCR2(MCP-1)、CCR5(RANTES、MIP-1α、MIP-1β)、CXCR2(MIP-2)和CXCR3(IP-10)。它们的表达时间表明,CXCR2和CCR1可能在该疾病依赖中性粒细胞的异源期起重要作用,而CCR1、CCR2、CCR5和CXCR3则伴随着随后自体疾病特征性的单核细胞浸润。因此,我们使用CCR1基因敲除(CCR1(-/-))小鼠评估了CCR1在NTN中的作用。我们发现,CCR1(-/-)小鼠中的中性粒细胞积累与野生型动物相当,但CD4(+)和CD8(+) T细胞以及巨噬细胞的肾脏募集显著增加。此外,CCR1(-/-)小鼠发生的肾小球肾炎比对照组更严重,伴有更多的蛋白尿和血尿素氮,以及更高的新月体形成频率。此外,CCR1(-/-)小鼠表现出增强的Th1免疫反应,包括抗原特异性IgG2a抗体滴度、迟发型超敏反应以及IFN-γ和TNF-α的产生。最后,使用过表达CCR1的重组蛋白和转染细胞,我们证明MIP-1α而非RANTES与CCR1结合并诱导细胞趋化。因此,CCR1的表达并非简单地促进NTN期间的白细胞募集,而是深刻改变了肾小球肾炎的效应期。趋化因子受体的治疗性靶向有时可能会加重潜在疾病。