Knutson D W, Chia D, Barnett E V, Levy L
Immunology. 1985 Mar;54(3):439-48.
We studied the capacity of the mononuclear phagocytic system (MPS) of NZB/W and NZB mice to clear trace and saturating doses of soluble heat-aggregates of IgG (A-IgG) from the blood. Mature female NZB/W mice (aged 5-7 months) with early glomerulonephritis showed no differences in MPS clearance of A-IgG compared with younger NZB/W mice without glomerulonephritis. In contrast, mature NZB mice had a more rapid clearance of A-IgG and greater MPS localization of A-IgG than their younger counterparts. Further studies showed that older NZB/W mice (greater than 10 months) had a slightly more rapid clearance of A-IgG than 2-5-month-old mice (t 1/2 = 3.34 +/- 0.27 SEM vs 3.76 +/- 0.34 SEM, P less than 0.01), whereas NZB mice mice older than 10 months of age had a markedly more rapid clearance than 2-5-month-old NZB mice (t 1/2 = 2.84 +/- 0.15 SEM vs 3.76 +/- 0.32, P less than 0.005). The more rapid clearance seen in NZB mice was partly explained by greater splenic localization of A-IgG and appeared to be restricted to Fc- and/or C3b-receptor mediated clearance, in that clearance of aggregated albumin was not changed. We conclude that NZB/W mice have no impairment in MPS clearance capacity at the onset of their glomerulonephritis, and slightly increased clearance capacity late in the course of their disease. Thus, the presence of circulating immune complexes and the development of glomerulonephritis in NZB/W mice is unlikely to be due to a diminished MPS clearance capacity. NZB mice have an increase in MPS capacity to clear A-IgG as a function of age.
我们研究了NZB/W和NZB小鼠的单核吞噬细胞系统(MPS)从血液中清除痕量和饱和剂量可溶性热聚集IgG(A-IgG)的能力。患有早期肾小球肾炎的成熟雌性NZB/W小鼠(5-7个月龄)与未患肾小球肾炎的年轻NZB/W小鼠相比,在A-IgG的MPS清除方面没有差异。相比之下,成熟的NZB小鼠比其年轻的同类小鼠对A-IgG的清除更快,且A-IgG在MPS中的定位更多。进一步研究表明,年龄较大的NZB/W小鼠(大于10个月)对A-IgG的清除比2-5个月龄的小鼠略快(t 1/2 = 3.34 ± 0.27 SEM对3.76 ± 0.34 SEM,P < 0.01),而10个月龄以上的NZB小鼠比2-5个月龄的NZB小鼠清除明显更快(t 1/2 = 2.84 ± 0.15 SEM对3.76 ± 0.32,P < 0.005)。NZB小鼠中观察到的更快清除部分是由于A-IgG在脾脏中的定位更多,并且似乎仅限于Fc和/或C3b受体介导的清除,因为聚集白蛋白的清除没有变化。我们得出结论,NZB/W小鼠在肾小球肾炎发作时MPS清除能力没有受损,并且在疾病后期清除能力略有增加。因此,NZB/W小鼠中循环免疫复合物的存在和肾小球肾炎的发展不太可能是由于MPS清除能力降低。NZB小鼠的MPS清除A-IgG的能力随年龄增长而增加。