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首页> 外文期刊>Immunobiology: Zeitschrift fur Immunitatsforschung >Compstatin analog Cp40 inhibits complement dysregulation in vitro in C3 glomerulopathy
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Compstatin analog Cp40 inhibits complement dysregulation in vitro in C3 glomerulopathy

机译:坎普他汀类似物Cp40在体外抑制C3肾小球病变中的补体失调

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摘要

C3 glomerulopathy (C3G) defines a group of untreatable ultra-rare renal diseases caused by uncontrolled activation of the alternative complement pathway. Nearly half of patients progress to end stage renal failure within 10 years. Cp40, a second-generation compstatin analog in clinical development, is a 14 amino-acid cyclic peptide that selectively inhibits complement activation in humans and non-human primates by binding to C3 and C3b. We hypothesized that by targeting C3 Cp40 would provide an effective treatment for C3G. By investigating its effects in vitro using multiple assays of complement activity, we show that Cp40 prevents complement-mediated lysis of sheep erythrocytes in sera from C3G patients, prevents complement dysregulation in the presence of patient-derived autoantibodies to the C3 and C5 convertases, and prevents complement dysregulation associated with disease-causing genetic mutations. In aggregate, these data suggest that Cp40 may offer a novel and promising therapeutic option to C3G patients as a disease-specific, targeted therapy. As such, Cp40 could represent a major advance in the treatment of this disease. (C) 2015 Elsevier GmbH. All rights reserved.
机译:C3肾小球病(C3G)定义了一组由替代补体途径的失控激活引起的不可治愈的超罕见肾脏疾病。在10年内,将近一半的患者发展为晚期肾衰竭。 Cp40是临床开发中的第二代坎普他汀类似物,是一种14个氨基酸的环状肽,可通过结合C3和C3b选择性抑制人和非人灵长类动物的补体激活。我们假设通过靶向C3 Cp40将为C3G提供有效的治疗。通过使用补体活性的多种测定方法在体外研究其作用,我们显示Cp40可以防止补体介导的C3G患者血清中绵羊红细胞的溶解,防止在患者衍生的C3和C5转化酶自身抗体存在下补体失调。预防与致病基因突变相关的补体失调。总体而言,这些数据表明Cp40可以作为一种针对疾病的靶向治疗为C3G患者提供一种新颖而有希望的治疗选择。因此,Cp40可能代表该疾病治疗的重大进展。 (C)2015 Elsevier GmbH。版权所有。

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