首页> 外文期刊>Scandinavian journal of immunology. >Development of anti-dsDNA autoantibodies prior to clinical diagnosis of systemic lupus erythematosus.
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Development of anti-dsDNA autoantibodies prior to clinical diagnosis of systemic lupus erythematosus.

机译:在临床诊断系统性红斑狼疮之前开发抗dsDNA自身抗体。

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Anti-double stranded (dsDNA) antibodies are of considerable diagnostic value and are thought to be involved in the pathogenesis of systemic lupus erythematosus (SLE). Fluctuations in anti-dsDNA antibody levels are also used as markers for disease activity and exacerbations. In this study we sought to evaluate the anti-dsDNA antibody level in serum samples collected before the onset of SLE diagnosis. A total of 130 SLE patients were identified with stored serum samples available prior to diagnosis within the US Department of Defense serum repository. All 633 sera available from these patients were screened for anti-dsDNA antibodies using an enzyme linked immunosorbant assay (ELISA). Within this cohort 55% of cases had detectable anti-dsDNA antibodies prior to SLE diagnosis. The onset of anti-dsDNA antibodies ranged from 9.3 years before to within the same month as diagnosis (with a mean onset 2.7 years before diagnosis). In order to assess for fluctuations in anti-dsDNA levels relative to diagnosis, cases were selected with at least two positive samples, one within 6 months and a second greater than 6 months prior to diagnosis (n = 26). Seven of these cases also had samples available shortly after diagnosis (< or = 6 months) for comparison. Fifty-eight percent of the 26 cases developed a significant rise in anti-dsDNA antibody levels within 6 months of diagnosis. A significant decline in anti-dsDNA levels ensued after diagnosis (and following treatment with corticosteroids) in all seven cases with samples available. Patients with a significant rise in anti-dsDNA antibodies at diagnosis were more likely to have renal disease than those who did not (66.7% compared to 27.3%, chi2 =3.94, P<0.05). These data suggest that anti-dsDNA antibodies are present in SLE patient sera much earlier than previously suspected. In addition, the data are consistent with increases in anti-dsDNA levels contributing to the onset of clinical illness in some patients with SLE.
机译:抗双链(dsDNA)抗体具有重要的诊断价值,并被认为与系统性红斑狼疮(SLE)的发病机理有关。抗dsDNA抗体水平的波动也用作疾病活动和恶化的标志。在这项研究中,我们试图评估SLE诊断开始之前收集的血清样本中的抗dsDNA抗体水平。在美国国防部血清库中进行诊断之前,共鉴定出130名SLE患者的血清样本可用。使用酶联免疫吸附测定(ELISA),从这些患者获得的所有633个血清中筛选抗dsDNA抗体。在该队列中,有55%的病例在SLE诊断之前具有可检测的抗dsDNA抗体。抗dsDNA抗体的发作时间从诊断之前的9.3年到诊断的同一个月内(诊断之前的平均发作时间为2.7年)。为了评估抗dsDNA水平相对于诊断的波动,选择了至少两个阳性样本的病例,一个样本在诊断前6个月内,第二个样本在诊断前大于6个月(n = 26)。这些病例中有7例在诊断后不久(<或= 6个月)也有样本可供比较。在诊断的6个月内,这26例患者中有58%的抗dsDNA抗体水平显着升高。在有可用样品的所有七例病例中,诊断后(以及用糖皮质激素治疗后)随后的抗dsDNA水平均显着下降。确诊时具有抗dsDNA抗体显着升高的患者比没有接受抗dsDNA抗体的患者更容易患肾脏疾病(66.7%比27.3%,chi2 = 3.94,P <0.05)。这些数据表明,SLE患者血清中存在的抗dsDNA抗体比以前怀疑的要早得多。此外,该数据与某些SLE患者的抗dsDNA水平升高有助于临床疾病发作有关。

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