Yokoyama H, Kreft B, Kelley V R
Laboratory of Immunogenetics and Transplantation, Brigham and Women's Hospital, Boston, Massachusetts, USA.
Kidney Int. 1995 Jan;47(1):122-30. doi: 10.1038/ki.1995.14.
Tumor necrosis factor (TNF)-alpha contributes to expansion of lymphocytes in neonatal mice and can accelerate renal injury. T cells induced by the lpr gene promote renal injury. However, the lpr gene alone is insufficient to cause renal damage, since MRL-lpr, but not C3H-lpr mice develop lupus nephritis. In this study, we examined the temporal expression of TNF-alpha in the kidney and circulation of mice (MRL and C3H) with the lpr gene and their congenic counterparts (++). We measured a bioactive TNF-alpha using L929 cells and tissue expression with an avidin-biotin immunoperoxidase method. A biphasic increase in circulating TNF-alpha in MRL-lpr mice was detected. There was an initial peak in neonatal mice (703 +- 208 pg/ml) which normalized by two months of age (87 +- 13 pg/ml) and reascended proportional to the severity of renal injury (non-proteinuric 570 +/- 87, proteinuric; 1255 +/- 135 pg/ml). In addition, there was only a single peak in neonatal C3H-lpr mice (1270 +/- 318 pg/ml) with a nadir by six weeks of age (434 +/- 52 pg/ml). In contrast, serum TNF-alpha was low in MRL-(++) and C3H-(++) mice (80 +/- 3 and 95 +/- 30 pg/ml), respectively. TNF-alpha expression in kidneys paralleled the serum pattern in MRL-lpr mice. Enhanced TNF-alpha expression was restricted to tubular epithelial cells (TEC) in neonatal MRL-lpr and C3H-lpr mice, and not detected in congenics. In adult mice, intrarenal TNF-alpha expression was more ubiquitous and was detected in glomeruli, vascular smooth muscle and perivascular infiltrating cells as well as TEC.(ABSTRACT TRUNCATED AT 250 WORDS)
肿瘤坏死因子(TNF)-α有助于新生小鼠淋巴细胞的扩增,并可加速肾损伤。lpr基因诱导的T细胞会促进肾损伤。然而,仅lpr基因不足以导致肾损伤,因为MRL-lpr小鼠会发生狼疮性肾炎,而C3H-lpr小鼠则不会。在本研究中,我们检测了带有lpr基因的小鼠(MRL和C3H)及其同基因对照(++)的肾脏和循环系统中TNF-α的时序表达。我们使用L929细胞测量生物活性TNF-α,并采用抗生物素蛋白-生物素免疫过氧化物酶法检测组织表达。检测到MRL-lpr小鼠循环TNF-α呈双相增加。新生小鼠出现初始峰值(703±208 pg/ml),到2月龄时恢复正常(87±13 pg/ml),随后随着肾损伤严重程度再次升高(无蛋白尿570±87,有蛋白尿1255±135 pg/ml)。此外,新生C3H-lpr小鼠仅出现一个峰值(1270±318 pg/ml),6周龄时降至最低点(434±52 pg/ml)。相比之下,MRL-(++)和C3H-(++)小鼠血清TNF-α较低(分别为80±3和95±30 pg/ml)。MRL-lpr小鼠肾脏中TNF-α的表达与血清模式相似。新生MRL-lpr和C3H-lpr小鼠中TNF-α表达增强仅限于肾小管上皮细胞(TEC),同基因对照中未检测到。在成年小鼠中,肾内TNF-α表达更为普遍,在肾小球、血管平滑肌、血管周围浸润细胞以及TEC中均有检测到。(摘要截短于250字)
