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小鼠系统性红斑狼疮血管病变的分析。I. 与血清学异常的关联。

Analysis of vascular lesions in murine SLE. I. Association with serologic abnormalities.

作者信息

Berden J H, Hang L, McConahey P J, Dixon F J

出版信息

J Immunol. 1983 Apr;130(4):1699-705.

PMID:6131920
Abstract

In murine SLE, two different vascular lesions can develop. A necrotizing polyarteritis (NPA), exclusively found in MRL/I mice, is characterized by a dense infiltration of PMN and fibrinoid necrosis of the arterial wall. The second, a degenerative vascular lesion, occurs in a low incidence in all SLE mice, except the (NZW X BXSB)F1 (WBF1) male, in which its incidence is 100%. This lesion shows subendothelial deposits of immunoglobulins with minimal or no inflammatory or proliferative reaction. This degenerative vascular disease (DVD) is predominantly localized in the coronary arteries and is highly correlated with myocardial infarction. Serologic analysis revealed that NPA in MRL/I mice was associated with relatively late development of high levels of autoantibodies and circulating immune complexes; DVD in WBF1 mice was associated with an early onset of autoantibody production of a low magnitude that gave rise to a persistent low level of circulating immune complexes. Characterization of circulating immune complexes in MRL/I mice showed these complexes were mainly of intermediate size (7S-19S) and contained predominantly anti-DNA antibodies. In WBF1 mice, complexes were barely detectable and contained mostly anti-gp70 antibodies. Elution of kidneys showed that the major antibody deposited in MRL/I mice has an anti-DNA specificity, whereas in WBF1 animals, the major antibody was anti-gp70. Furthermore, a 10 times greater amount of immunoglobulins could be eluted from WBF1 hearts with DVD than from MRL/I and BXSB hearts. Additionally, we found that the lack of an inflammatory reaction in DVD was not because of a preferential deposition of noncomplement-fixing IgG1 antibodies nor could it be related to a defective inflammatory response, because WBF1 mice had an undiminished reverse passive Arthus reaction throughout their lives. It is concluded that NPA develops secondary to high levels of autoantibodies with a concomitant rise in immune complexes, whereas DVD is associated with sustained low levels of circulating immune complexes.

摘要

在小鼠系统性红斑狼疮(SLE)中,可出现两种不同的血管病变。一种坏死性多动脉炎(NPA),仅在MRL/I小鼠中发现,其特征是中性粒细胞大量浸润和动脉壁的纤维蛋白样坏死。第二种是退行性血管病变,在所有SLE小鼠中发病率较低,但(NZW×BXSB)F1(WBF1)雄性小鼠除外,其发病率为100%。该病变表现为免疫球蛋白的内皮下沉积,炎症或增殖反应轻微或无。这种退行性血管疾病(DVD)主要局限于冠状动脉,与心肌梗死高度相关。血清学分析显示,MRL/I小鼠中的NPA与自身抗体和循环免疫复合物水平的相对较晚升高有关;WBF1小鼠中的DVD与低水平自身抗体产生的早期发作有关,后者导致循环免疫复合物持续处于低水平。对MRL/I小鼠循环免疫复合物的表征显示,这些复合物主要为中等大小(7S - 19S),主要包含抗DNA抗体。在WBF1小鼠中,复合物几乎检测不到,主要包含抗gp70抗体。肾脏洗脱显示,MRL/I小鼠中沉积的主要抗体具有抗DNA特异性,而在WBF1动物中,主要抗体是抗gp70。此外,与MRL/I和BXSB心脏相比,患有DVD的WBF1心脏可洗脱的免疫球蛋白量多10倍。此外,我们发现DVD中缺乏炎症反应不是因为非补体结合性IgG1抗体的优先沉积,也与炎症反应缺陷无关,因为WBF1小鼠在其一生中反向被动Arthus反应并未减弱。结论是,NPA继发于高水平的自身抗体以及免疫复合物的同时升高,而DVD与循环免疫复合物的持续低水平有关。

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