1st Department of Pediatrics, Semmelweis University, Bókay J. u. 53, Budapest 1083, Hungary.
Pediatr Nephrol. 2013 Oct;28(10):2061-4. doi: 10.1007/s00467-013-2542-4. Epub 2013 Jun 26.
The pathogenicity of the NPHS2 homozygous p.R229Q variant in steroid-resistant nephrotic syndrome (SRNS) is doubtful. While it has been reported in unaffected controls, it is enriched in patients with SRNS, suggesting pathogenicity.
CASE-DIAGNOSIS/TREATMENT: A family with three members homozygous for the NPHS2 p.R229Q variant is presented: a 37-year-old patient who was diagnosed with proteinuria at age 7 months, focal segmental glomerulosclerosis (FSGS) at age 20 years, and end-stage renal disease (ESRD) at age 33 years, his 59 year-old father and his 40 year-old brother, both unaffected with no proteinuria. The affected son also harbors a heterozygous de novo, truncating PAX2 mutation (c.76dupG, p.V26Gfs*28), which can explain his chronic renal failure but which is rarely associated with FSGS.
This family provides further evidence that homozygous p.R229Q in itself may not cause FSGS. Nevertheless, the rare association of FSGS to a PAX2 mutation may reflect the modifier effect of p.R229Q in the homozygous state. Such a modifier effect can also explain its enrichment in SRNS patients. Patients with homozygous p.R229Q should be screened for the causative mutation in a second gene.
NPHS2 纯合 p.R229Q 变异在激素抵抗性肾病综合征 (SRNS) 中的致病性是值得怀疑的。虽然它在未受影响的对照中已有报道,但在 SRNS 患者中富集,提示其致病性。
病例诊断/治疗:本文报告了一个 NPHS2 p.R229Q 变异纯合子的家族:一位 37 岁的患者,他在 7 个月大时被诊断为蛋白尿,20 岁时为局灶节段性肾小球硬化 (FSGS),33 岁时发展为终末期肾病 (ESRD);他 59 岁的父亲和 40 岁的哥哥均未受影响且无蛋白尿。受影响的儿子还携带一种新发生的、截断的 PAX2 突变(c.76dupG,p.V26Gfs*28),这可以解释他的慢性肾衰竭,但这种突变很少与 FSGS 相关。
该家族进一步证明了纯合 p.R229Q 本身可能不会导致 FSGS。然而,FSGS 与 PAX2 突变的罕见关联可能反映了 p.R229Q 纯合状态下的修饰效应。这种修饰效应也可以解释它在 SRNS 患者中的富集。纯合 p.R229Q 患者应筛查第二个基因的致病突变。
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