The extracellular matrix in the kidney: a source of novel non-invasive biomarkers of kidney fibrosis?

Federica Genovese, Alba A Manresa, Diana Julie Leeming, Morten Asser Karsdal, Peter Boor
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引用次数: 278

Abstract

Interstitial fibrosis is the common endpoint of end-stage chronic kidney disease (CKD) leading to kidney failure. The clinical course of many renal diseases, and thereby of CKD, is highly variable. One of the major challenges in deciding which treatment approach is best suited for a patient but also in the development of new treatments is the lack of markers able to identify and stratify patients with stable versus progressive disease. At the moment renal biopsy is the only means of diagnosing renal interstitial fibrosis. Novel biomarkers should improve diagnosis of a disease, estimate its prognosis and assess the response to treatment, all in a non-invasive manner. Existing markers of CKD do not fully and specifically address these requirements and in particular do not specifically reflect renal fibrosis. The aim of this review is to give an insight of the involvement of the extracellular matrix (ECM) proteins in kidney diseases and as a source of potential novel biomarkers of renal fibrosis. In particular the use of the protein fingerprint technology, that identifies neo-epitopes of ECM proteins generated by proteolytic cleavage by proteases or other post-translational modifications, might identify such novel biomarkers of renal fibrosis.

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肾脏中的细胞外基质:一种新的无创肾纤维化生物标志物的来源?
间质纤维化是导致肾衰竭的终末期慢性肾脏疾病(CKD)的常见终点。许多肾脏疾病的临床病程,因此CKD,是高度可变的。在决定哪种治疗方法最适合患者以及在开发新治疗方法时,主要挑战之一是缺乏能够识别和区分稳定与进展性疾病患者的标志物。目前,肾活检是诊断肾间质纤维化的唯一手段。新的生物标志物应该可以改善疾病的诊断,估计其预后并评估对治疗的反应,所有这些都是以非侵入性的方式进行的。现有的CKD标志物不能完全和特异性地满足这些要求,特别是不能特异性地反映肾纤维化。本综述的目的是深入了解细胞外基质(ECM)蛋白在肾脏疾病中的作用,以及作为潜在的肾纤维化新生物标志物的来源。特别是蛋白质指纹技术的使用,可以识别由蛋白酶或其他翻译后修饰的蛋白水解裂解产生的ECM蛋白的新表位,可能会识别出肾纤维化的这种新型生物标志物。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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