Riguetti Michelle T P, Varela Patrícia, Fernandes Danilo E, Polito M Goretti, Casimiro Fernanda M, Pesquero João B, Mastroianni-Kirsztajn Gianna
Department of Medicine, Division of Nephrology, Federal University of São Paulo, São Paulo, Brazil.
Center for Research and Molecular Diagnostic of Genetic Diseases - Department of Biophysics, Federal University of São Paulo, São Paulo, Brazil.
Front Genet. 2020 Sep 16;11:533373. doi: 10.3389/fgene.2020.533373. eCollection 2020.
Pathogenic variants in different genes have been described as involved in the development of familial focal segmental glomerulosclerosis (FSGS). A more precise genotype-phenotype correlation would be helpful to better characterize the clinical and laboratorial manifestations of this disease, as well as response to treatment. We analyzed podocin () gene variants in 50 members of four generations of a family with late-onset presentation of glomerular disease.
The gene variants R229Q and/or R291W were detected in several individuals, and the phenotype of FSGS with progressive loss of renal function was observed in all the family members carrying both mutations simultaneously. Patients manifested ongoing proteinuria over the years and progressive loss of renal function, which in three women culminated in renal replacement therapy by the 4th decade of life. In two affected patients with nephrotic syndrome, remission was not reached by the use of corticosteroids and other immunosuppressive drugs. The R229Q variant was pathogenic only when trans-associated with specific mutations, as the R291W variant in this family.
Coexistence of the two variants R229Q and R291W in compound heterozygosis was a determinant of the FSGS phenotype. The presence of these variants alone in heterozygosis did not cause significant proteinuria.
不同基因中的致病变异已被描述为与家族性局灶节段性肾小球硬化症(FSGS)的发生有关。更精确的基因型-表型相关性将有助于更好地描述该疾病的临床和实验室表现,以及对治疗的反应。我们分析了一个四代家族中50名患有迟发性肾小球疾病成员的足突蛋白()基因变异。
在几名个体中检测到基因变异R229Q和/或R291W,在所有同时携带这两种突变的家族成员中均观察到具有进行性肾功能丧失的FSGS表型。患者多年来持续出现蛋白尿和进行性肾功能丧失,三名女性在40岁时最终接受了肾脏替代治疗。在两名患有肾病综合征的受影响患者中,使用皮质类固醇和其他免疫抑制药物未能达到缓解。R229Q变异仅在与特定突变(如该家族中的R291W变异)反式关联时才具有致病性。
复合杂合子中R229Q和R291W这两种变异的共存是FSGS表型的决定因素。杂合子中单独存在这些变异不会导致明显的蛋白尿。
