Podocyturia: Potential applications and current limitations.

Hernán Trimarchi
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引用次数: 22

Abstract

Chronic kidney disease is a prevalent condition that affects millions of people worldwide and is a major risk factor of cardiovascular morbidity and mortality. The main diseases that lead to chronic kidney disease are frequent entities as diabetes mellitus, hypertension and glomerulopathies. One of the clinical markers of kidney disease progression is proteinuria. Moreover, the histological hallmark of kidney disease is sclerosis, located both in the glomerular and in the interstitial compartments. Glomerulosclerosis underscores an irreversible lesion that is clinically accompanied by proteinuria. In this regard, proteinuria and glomerular sclerosis are linked by the cell that has been conserved phylogenetically not only to prevent the loss of proteins in the urine, but also to maintain the health of the glomerular filtration barrier: The podocyte. It can then be concluded that the link between proteinuria, kidney disease progression and chronic kidney disease is mainly related to the podocyte. What is this situation due to? The podocyte is unable to proliferate under normal conditions, and a complex molecular machinery exists to avoid its detachment and eventual loss. When the loss of podocytes in the urine, or podocyturia, is taking place and its glomerular absolute number decreased, glomerulosclerosis is the predominant histological feature in a kidney biopsy. Therefore, tissular podocyte shortage is the cause of proteinuria and chronic kidney disease. In this regard, podocyturia has been demonstrated to precede proteinuria, showing that the clinical management of proteinuria cannot be considered an early intervention. The identification of urinary podocytes could be an additional tool to be considered by nephrologists to assess the activity of glomerulopathies, for follow-up purposes and also to unravel the pathophysiology of podocyte detachment in order to tailor the therapy of glomerular diseases more appropriately.

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足细胞术:潜在的应用和当前的限制。
慢性肾脏疾病是一种影响全世界数百万人的普遍疾病,是心血管发病率和死亡率的主要危险因素。导致慢性肾脏疾病的主要疾病是糖尿病、高血压和肾小球疾病等常见疾病。蛋白尿是肾脏疾病进展的临床标志之一。此外,肾脏疾病的组织学标志是硬化,位于肾小球和间质室。肾小球硬化是一种不可逆的病变,临床上伴有蛋白尿。在这方面,蛋白尿和肾小球硬化是由一种细胞联系在一起的,这种细胞在系统发育上是保守的,不仅可以防止尿中蛋白质的损失,还可以维持肾小球滤过屏障的健康:足细胞。由此可以得出结论,蛋白尿、肾脏疾病进展和慢性肾脏疾病之间的联系主要与足细胞有关。这种情况是由于什么造成的?足细胞在正常条件下无法增殖,存在复杂的分子机制以避免其脱离和最终丢失。当尿中足细胞减少或足细胞尿症发生时,肾小球绝对数量减少,肾小球硬化是肾活检的主要组织学特征。因此,组织足细胞缺乏是蛋白尿和慢性肾脏疾病的原因。在这方面,足尿症已被证明先于蛋白尿,这表明蛋白尿的临床管理不能被认为是早期干预。尿足细胞的鉴定可以作为肾病学家评估肾小球病变活动的额外工具,用于随访目的,也可以揭示足细胞脱离的病理生理学,以便更适当地定制肾小球疾病的治疗。
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