白细胞介素 10/转化生长因子-β修饰的巨噬细胞诱导调节性 T 细胞并防止阿霉素肾病。
IL-10/TGF-beta-modified macrophages induce regulatory T cells and protect against adriamycin nephrosis.
机构信息
Centre for Transplantation and Renal Research, University of Sydney, Westmead Millennium Institute, and Centre for Kidney Research, Children's Hospital at Westmead, Level 2 Block D, Darcy Road, Westmead, New South Wales, Australia.
出版信息
J Am Soc Nephrol. 2010 Jun;21(6):933-42. doi: 10.1681/ASN.2009060592. Epub 2010 Mar 18.
IL-10/TGF-beta-modified macrophages, a subset of activated macrophages, produce anti-inflammatory cytokines, suggesting that they may protect against inflammation-mediated injury. Here, macrophages modified ex vivo by IL-10/TGF-beta (IL-10/TGF-beta Mu2) significantly attenuated renal inflammation, structural injury, and functional decline in murine adriamycin nephrosis (AN). These cells deactivated effector macrophages and inhibited CD4+ T cell proliferation. IL-10/TGF-beta Mu2 expressed high levels of the regulatory co-stimulatory molecule B7-H4, induced regulatory T cells from CD4+CD25- T cells in vitro, and increased the number of regulatory T cells in lymph nodes draining the kidneys in AN. The phenotype of IL-10/TGF-beta Mu2 did not switch to that of effector macrophages in the inflamed kidney, and these cells did not promote fibrosis. Taken together, these data demonstrate that IL-10/TGF-beta-modified macrophages effectively protect against renal injury in AN and may become part of a therapeutic strategy for chronic inflammatory disease.
IL-10/TGF-β 修饰的巨噬细胞是活化巨噬细胞的一个亚群,可产生抗炎细胞因子,提示其可能有助于防止炎症介导的损伤。在此,经 IL-10/TGF-β(IL-10/TGF-β Mu2)体外修饰的巨噬细胞可显著减轻小鼠阿霉素肾病(AN)中的肾脏炎症、结构损伤和功能下降。这些细胞使效应巨噬细胞失活并抑制 CD4+T 细胞增殖。IL-10/TGF-β Mu2 表达高水平的调节共刺激分子 B7-H4,可在体外诱导 CD4+CD25-T 细胞分化为调节性 T 细胞,并增加 AN 中肾脏引流淋巴结中调节性 T 细胞的数量。IL-10/TGF-β Mu2 的表型在炎症肾脏中不会转变为效应巨噬细胞表型,且这些细胞不会促进纤维化。综上所述,这些数据表明,IL-10/TGF-β 修饰的巨噬细胞可有效防止 AN 中的肾脏损伤,可能成为慢性炎症性疾病治疗策略的一部分。
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