Jacob M, Napirei M, Ricken A, Dixkens C, Mannherz H G
Abteilung für Anatomie und Embryologie, Ruhr-Universität Bochum, Germany.
Lupus. 2002;11(8):514-27. doi: 10.1191/0961203302lu242oa.
Deoxyribonuclease 1 (Dnase1)-deficient mice develop symptoms of Systemic lupus erythematosus (SLE). Here we analysed the renal histopathology of these animals in comparison to F1 hybrids of New Zealand black and white mice (NZB/W F1), an established model of SLE. Animals were divided into three groups according to the presence of anti-nuclear antibodies (ANA) and renal lesions. Groups 1a-1c were healthy, whereas group 2 and 3 were classified as lupus-prone and affected. Subendothelial and/or mesangial immune complex deposits, mesangial and endocapillary proliferation, haematoxylin bodies and platelet aggregation were detected in both mouse strains but were more severe in the NZB/W F1 mice. The lupus nephritis was classified as a proliferating (WHO type III or IV), which appeared to be preceded by a mesangial form (WHO type II). Subclassification of the ANA revealed a high prevalence of anti-nucleosome antibodies in Dnase1-deficient mice, whereas NZB/W F1 mice developed autoantibodies against a broad range of chromatin constituents. Mapping of the murine Dnase1 gene locus to chromosome 16A1-3 did not coincide with one of the reported susceptibility loci in the NZB/W F1 model, although a reduced Dnasel serum and urine activity has been described previously in these mice.
脱氧核糖核酸酶1(Dnase1)缺陷小鼠会出现系统性红斑狼疮(SLE)症状。在此,我们将这些动物的肾脏组织病理学与新西兰黑鼠和白鼠的F1代杂交种(NZB/W F1)进行了比较,NZB/W F1是一种已确立的SLE模型。根据抗核抗体(ANA)的存在情况和肾脏病变将动物分为三组。第1a - 1c组健康,而第2组和第3组被归类为易患狼疮和患病组。在两种小鼠品系中均检测到内皮下和/或系膜免疫复合物沉积、系膜和毛细血管内增生、苏木精小体和血小板聚集,但在NZB/W F1小鼠中更为严重。狼疮性肾炎被分类为增殖性(世界卫生组织III型或IV型),似乎之前有系膜型(世界卫生组织II型)。ANA的亚分类显示,Dnase1缺陷小鼠中抗核小体抗体的患病率很高,而NZB/W F1小鼠产生了针对多种染色质成分的自身抗体。将小鼠Dnase1基因座定位到染色体16A1 - 3与NZB/W F1模型中报道的一个易感基因座不一致,尽管之前在这些小鼠中已描述Dnasel血清和尿液活性降低。
