Zhao S L, Zhao F, Sha Y G, Chen Q X, Cheng X Q, Huang S M
Department of Nephrology, Children's Hospital of Nanjing Medical University, Nanjing 210008, China.
Zhonghua Er Ke Za Zhi. 2018 Apr 2;56(4):289-293. doi: 10.3760/cma.j.issn.0578-1310.2018.04.010.
To summarize the clinical features and genetic analysis results of 10 children with Dent disease. The clinical data and gene test results of 10 boys aged from 8 months to 12 years with Dent disease diagnosed in Children's Hospital of Nanjing Medical University from January 2014 to July 2017 were analyzed retrospectively. All patients had insidious onset, 5 cases were found to have proteinuria on routine urine examination after hospitalization duo to other diseases, 4 cases were admitted to hospital because increased foams in the urine, and 1 case was found to have proteinuria on health checkup. All cases presented with low molecular weight proteinuria, urine protein electrophoresis showed that the proportion of low molecular weight protein was greater than 50%, 7 cases had nephrotic-range proteinuria, but none had hypoproteinemia. Six cases had hypercalciuria, 3 cases had nephrocalcinosis, 1 case had nephrolithiasis, 2 cases had glomerular microscopic hematuria, in 1 case urine glucose wa weakly positive but blood glucose was normal. All patients had normal renal function, normal serum calcium, no hypophosphoremia and none had rickets. Genetic analysis results showed that 7 patients with variants in the CLCN5 gene, including 2 nonsense variants (p.R637X, p.Y143X), 3 missense variants (p.A540D, p.G135E, p.G703V), 1 deletion variant (exons 9, 10, 11, 12, 13, 1 missing), and 1 frameshift variant (p.T260Tfs*10). Three cases had missense variants of OCRL gene (p.I274T, p.I371T, p.F399S). Except for p.R637X and p.I274T, the other 8 cases had newly discovered variants. Five patients underwent a renal biopsy, the biopsy revealed focal global glomerulosclerosis in 3 patients, mild mesangial proliferative glomerulonephritis in 1 patient and renal minimal change in 1 patient. Mild focal tubular atrophy and interstitial fibrosis were noted in three cases. Mild segmental foot process effacement was noted under electron microscope in all five cases. All the children with Dent disease had insidious onset, low molecular weight proteinuria is the main clinical manifestation, most cases presented with nephrotic-range proteinuria, but there was no hypoalbuminemia, some cases were not associated with hypercalciuria. The pathogenic genes in most cases were CLCN5 and a few were OCRL. The types of genetic variation include missense variant, nonsense variant, deletion variant and frameshift variant. Although Dent disease is a renal tubular disease, renal biopsy suggests that most cases are associated with glomerular lesions.
总结10例丹特病患儿的临床特征及基因分析结果。回顾性分析2014年1月至2017年7月在南京医科大学附属儿童医院确诊的10例年龄8个月至12岁的丹特病男孩的临床资料及基因检测结果。所有患者起病隐匿,5例因其他疾病住院后常规尿检发现蛋白尿,4例因尿中泡沫增多入院,1例在健康体检时发现蛋白尿。所有病例均表现为低分子量蛋白尿,尿蛋白电泳显示低分子量蛋白比例大于50%,7例有肾病范围蛋白尿,但均无低蛋白血症。6例有高钙尿症,3例有肾钙质沉着症,1例有肾结石,2例有肾小球镜下血尿,1例尿糖弱阳性但血糖正常。所有患者肾功能正常,血钙正常,无低磷血症,均无佝偻病。基因分析结果显示,7例患者CLCN5基因有变异,包括2个无义变异(p.R637X、p.Y143X)、3个错义变异(p.A540D、p.G135E、p.G703V)、1个缺失变异(外显子9、10、11、12、13、1缺失)和1个移码变异(p.T260Tfs*10)。3例患者OCRL基因有错义变异(p.I274T、p.I371T、p.F399S)。除p.R637X和p.I274T外,其他8例为新发现的变异。5例患者进行了肾活检,活检显示3例为局灶性球性肾小球硬化,1例为轻度系膜增生性肾小球肾炎,1例为肾微小病变。3例有轻度局灶性肾小管萎缩和间质纤维化。5例电镜下均可见轻度节段性足突融合。所有丹特病患儿起病隐匿,低分子量蛋白尿是主要临床表现,多数病例有肾病范围蛋白尿,但无低白蛋白血症,部分病例无高钙尿症。多数病例致病基因为CLCN5,少数为OCRL。基因变异类型包括错义变异、无义变异、缺失变异和移码变异。尽管丹特病是一种肾小管疾病,但肾活检提示多数病例与肾小球病变有关。
