Wang Wei, Faubel Sarah, Ljubanovic Danica, Mitra Amit, Falk Sandor A, Kim Jun, Tao Yunxia, Soloviev Andrei, Reznikov Leonid L, Dinarello Charles A, Schrier Robert W, Edelstein Charles L
Department of Medicine, Division of Renal Diseases, University of Colorado Health Sciences Center, Denver, Colorado 80262, USA.
Am J Physiol Renal Physiol. 2005 May;288(5):F997-1004. doi: 10.1152/ajprenal.00130.2004. Epub 2005 Jan 11.
Caspase-1-deficient (-/-) mice are protected against sepsis-induced hypotension and mortality. We investigated the role of caspase-1 and its associated cytokines in a nonhypotensive model of endotoxemic acute renal failure (ARF). Mice were injected intraperitoneally with 2.5 mg of LPS that induces endotoxemic ARF. On immunoblot analysis of whole kidney, there was an increase in caspase-1 protein in LPS-treated mice compared with vehicle-treated controls. In LPS-treated mice, the glomerular filtration rate (GFR) was significantly higher in caspase-1 -/- vs. wild-type mice at 16 and 36 h after LPS. To determine the mechanism of this protection, the caspase-1-activated cytokines IL-1beta and IL-18 were investigated. IL-1beta and IL-18 protein were significantly increased in the kidneys of LPS- vs. vehicle-treated mice. To determine the role of these cytokines, mice were treated with recombinant IL-1 receptor antagonist (IL-1Ra) or IL-18-neutralizing antiserum. In LPS-treated mice, GFR was not different in IL-1Ra-treated or IL-18-neutralizing antiserum-treated or combination therapy (IL-1Ra plus IL-18-neutralizing antiserum-treated) compared with control mice. In addition, tubular cell apoptosis, neutrophil infiltration, myeloperoxidase activity, caspase-3 activity, and calpain activity were not different between wild-type and caspase-1 -/- mice with endotoxemic ARF. In LPS- vs. vehicle-treated wild-type mice, renal IL-1alpha was significantly increased. In both LPS- and vehicle-treated caspase-1 -/- mice, renal IL-1alpha was very low. In summary, caspase-1 -/- mice are functionally protected against endotoxemic ARF. Neutralization of IL-1beta and IL-18 is not functionally protective. The role of the intracellular proinflammatory cytokine IL-1alpha in endotoxemic ARF merits further study.
半胱天冬酶 -1缺陷(-/-)小鼠可免受败血症诱导的低血压和死亡影响。我们在内毒素血症性急性肾衰竭(ARF)的非低血压模型中研究了半胱天冬酶 -1及其相关细胞因子的作用。给小鼠腹腔注射2.5 mg可诱导内毒素血症性ARF的脂多糖(LPS)。对整个肾脏进行免疫印迹分析时,与用赋形剂处理的对照相比,LPS处理的小鼠中半胱天冬酶 -1蛋白增加。在LPS处理的小鼠中,LPS注射后16小时和36小时,半胱天冬酶 -1基因敲除小鼠的肾小球滤过率(GFR)显著高于野生型小鼠。为了确定这种保护作用的机制,研究了半胱天冬酶 -1激活的细胞因子白细胞介素 -1β(IL -1β)和白细胞介素 -18(IL -18)。与用赋形剂处理的小鼠相比,LPS处理的小鼠肾脏中IL -1β和IL -18蛋白显著增加。为了确定这些细胞因子的作用,用重组IL -1受体拮抗剂(IL -1Ra)或IL -18中和抗血清处理小鼠。在LPS处理的小鼠中,与对照小鼠相比,IL -1Ra处理组、IL -18中和抗血清处理组或联合治疗组(IL -1Ra加IL -18中和抗血清处理组)的GFR没有差异。此外,在内毒素血症性ARF的野生型和半胱天冬酶 -1基因敲除小鼠之间,肾小管细胞凋亡、中性粒细胞浸润、髓过氧化物酶活性、半胱天冬酶 -3活性和钙蛋白酶活性没有差异。与用赋形剂处理的野生型小鼠相比,LPS处理的野生型小鼠肾脏中IL -1α显著增加。在LPS处理和赋形剂处理的半胱天冬酶 -1基因敲除小鼠中,肾脏IL -1α都非常低。总之,半胱天冬酶 -1基因敲除小鼠在内毒素血症性ARF方面具有功能保护作用。中和IL -1β和IL -18在功能上没有保护作用。细胞内促炎细胞因子IL -1α在内毒素血症性ARF中的作用值得进一步研究。
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