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Morphofunctional Effects of C5 Convertase Blockade in Immune Complex-Mediated Membranoproliferative Glomerulonephritis: Report of Two Cases with Evidence of Terminal Complement Activation

机译:C5转化酶阻滞在免疫复合介导的膜上肺炎肾细胞肾盂肾炎的形态官能效应:终端补体激活证据报告

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A membranoproliferative pattern of glomerular injury is frequently observed in patients with complement-mediated disorders, such as C3 glomerulopathies (C3G) and primary immune complex-mediated membranoproliferative glo-merulonephritis (IC-MPGN). The outcomes of C3G and IC-MPGN are poor, independently of immunosuppressive therapy. However, two 48-week treatment periods with the anti-C5 monoclonal antibody eculizumab, divided by a 12-week washout period, achieved remission of proteinuria and stabilization/improvement of the glomerular filtration rate (GFR), measured through iohexol plasma clearance, in 3 of 10 patients with biopsy-proven MPGN, nephrotic syndrome and terminal complement complex sC5b-9 plasma levels > 1,000 mg/mL, at inclusion. Baseline and end-of-study kidney biopsies were available for 2 patients with IC-MPGN, and their baseline characteristics were similar. However, in 1 patient proteinuria and GFR did not improve during the study, whereas in the other proteinuria decreased from 4.84 to 2.12 g/24-h and GFR increased from 91.5 to 142.7 mL/ min/1.73 m~2. Glomerular inflammation improved and median (interquartile range) glomerular staining for C5b-9 decreased in both cases: from 23.6 to 18.2% (p = 0.021) in the patient who achieved remission and from 15.8 to 10.7% (p = 0.019) in the patient with persistent proteinuria. Chronic glomerular lesions progressed and C3 glomerular staining and electron-dense deposits did not change appreciably in either case. However, in the patient who achieved remission, ultrastructural evaluation revealed features of glomerular microangiopathy at inclusion, which fully recovered post-treatment. Podocyte foot process effacement was observed in both patients at inclusion, but recovered only in the patient with microangiopathy.Thus, in 2 patients with IC-MPGN, chronic glomerular changes progressed despite eculizum-ab-induced amelioration of glomerular inflammation and inhibition of sC5b-9 deposition, and independently of treatment effects on proteinuria and podocytes. The finding that the regression of microangiopathic changes was associated with improved clinical outcomes suggests that C5 blockade might have a therapeutic role in patients with IC-MPGN displaying microangiopathic endothelial injury.
机译:在补蛋白介导的疾病(如C3肾小球术(C3G)和原发性免疫复合介导的膜上血管炎(IC-MPGN)中,经常观察到膜上损伤的膜血管损伤模式。 C3G和IC-MPGN的结果差,独立于免疫抑制治疗。然而,通过碘醇等离子体清除,抗C5单克隆抗体生态,除以抗C5单克隆抗体生态物,除以抗C5单克隆抗体生态物,除以12周的洗涤期,达到蛋白尿缓解/改善肾小球过滤速率(GFR), 3例10名活组织检查验证的MPGN患者,肾病综合征和末端补体,复合SC5B-9血浆水平> 1,000mg / ml,夹杂物。基线和研究结束肾脏活检可用于2例IC-MPGN患者,它们的基线特性相似。然而,在1例患者蛋白尿和GFR在研究中没有改善,而在其他蛋白尿中从4.84降低到2.12g / 24-h,GFR从91.5增加到142.7ml / min / 1.73m〜2。肾小球炎症改善和中位数(四分位数范围)C5B-9的肾小球染色在两种情况下降低:在患者中患者中的23.6%至18.2%(p = 0.021),患者患者(P = 0.019)持续蛋白尿。慢性肾小球病变进展,并且C3肾小球染色和电子密集的沉积物在任何一种情况下都不会显着变化。然而,在实现缓解的患者中,超微结构评估揭示了包含在包合物中的肾小球微神经病症的特征,其完全回收后处理。在含有的患者中观察到podocyte足处理效应,但仅在患者中恢复微血管病变。在2例IC-MPGN患者中,尽管慢性肾小球变化,尽管生态 - AB诱导的肾小球炎症和抑制SC5B的抑制作用9沉积,独立于蛋白尿和诱饵的治疗效果。结果表明,微肺病变变化的回归与改善的临床结果有关表明C5封闭患者可能对患者患有微盲管内皮损伤的IC-MPGN患者具有治疗作用。

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