Molecular Biology Laboratory, Fundació Puigvert, Universitat Autònoma de Barcelona, REDinREN, Instituto de Investigación Carlos III, Barcelona, Spain.
Clin J Am Soc Nephrol. 2011 May;6(5):1139-48. doi: 10.2215/CJN.05260610. Epub 2011 Mar 17.
The increasing number of podocyte-expressed genes implicated in steroid-resistant nephrotic syndrome (SRNS), the phenotypic variability, and the uncharacterized relative frequency of mutations in these genes in pediatric and adult patients with SRNS complicate their routine genetic analysis. Our aim was to compile the clinical and genetic data of eight podocyte genes analyzed in 110 cases (125 patients) with SRNS (ranging from congenital to adult onset) to provide a genetic testing approach.
DESIGN, SETTING, PARTICIPANTS, & MEASUREMENTS: Mutation analysis was performed by sequencing the NPHS1, NPHS2, TRPC6, CD2AP, PLCE1, INF2, WT1 (exons 8 and 9), and ACTN4 (exons 1 to 10) genes.
We identified causing mutations in 34% (37/110) of SRNS patients, representing 67% (16/24) familial and 25% (21/86) sporadic cases. Mutations were detected in 100% of congenital-onset, 57% of infantile-onset, 24 and 36% of early and late childhood-onset, 25% of adolescent-onset, and 14% of adult-onset patients. The most frequently mutated gene was NPHS1 in congenital onset and NPHS2 in the other groups. A partial remission was observed in 7 of 26 mutation carriers treated with immunosuppressive agents and/or angiotensin-converting enzyme inhibitors. Patients with NPHS1 mutations showed a faster progression to ESRD than patients with NPHS2 mutations. None of these mutation carriers relapsed after kidney transplantation.
We propose a genetic testing algorithm for SRNS based on the age at onset and the familial/sporadic status. Mutation analysis of specific podocyte-genes has a clinical value in all age groups, especially in children.
越来越多的足细胞表达基因与类固醇耐药性肾病综合征(SRNS)有关,这些基因在儿童和成人 SRNS 患者中的表型变异性和突变相对频率尚不清楚,这使得对这些基因进行常规基因分析变得复杂。我们的目的是整理分析 110 例(125 例患者)SRNS(从先天性到成年发病)中 8 个足细胞基因的临床和遗传数据,以提供一种基因检测方法。
设计、地点、参与者和测量方法:通过测序 NPHS1、NPHS2、TRPC6、CD2AP、PLCE1、INF2、WT1(外显子 8 和 9)和 ACTN4(外显子 1 至 10)基因,进行突变分析。
我们在 34%(37/110)的 SRNS 患者中发现了致病突变,分别代表 67%(16/24)的家族性和 25%(21/86)的散发性病例。100%的先天性发病、57%的婴儿期发病、24%和 36%的早发和晚发儿童发病、25%的青少年发病和 14%的成年发病患者检测到突变。在先天性发病中最常突变的基因是 NPHS1,在其他组中最常突变的基因是 NPHS2。在接受免疫抑制剂和/或血管紧张素转换酶抑制剂治疗的 26 名突变携带者中,有 7 人出现部分缓解。与 NPHS2 突变患者相比,NPHS1 突变患者向 ESRD 的进展更快。这些突变携带者在肾移植后均未复发。
我们提出了一种基于发病年龄和家族性/散发性状态的 SRNS 基因检测算法。在所有年龄组,特别是在儿童中,对特定足细胞基因进行突变分析具有临床价值。
