Mbarek Ibtihel Benhaj, Mdimeg Saoussen, Moussa Amira, Zellama Dorsaf, Kaarout Hayat, Abdelmoula Jaouida, Achour Abdellatif, Abroug Saoussen, Omezzine Asma, Bouslama Ali
Biochemistry Department, LR12 SP11, Sahloul University Hospital, 4054, Sousse, Tunisia.
Nephrology Department, LR12 SP11, Sahloul University Hospital, 4054, Sousse, Tunisia.
BMC Nephrol. 2017 Jun 15;18(1):195. doi: 10.1186/s12882-017-0612-8.
Primary hyperoxaluria type 1 (PH1), is a rare and heterogeneous disease and one of major causes of renal insufficiency in Tunisia, caused by mutations in the AGXT gene. 33-34InsC mutation, was mainly described in children with a severe clinical feature leading to early death, but it was uncommonly reported in adult patients.
Common mutations in AGXT were tested using PCR/RFLP technique in 111 patients (68 adult, 43 children) with suspected PH1.
We described 16 cases (eight adult and eight children) with a 33-34InsC mutation with a median age of 24 years [6 months - 73 years]. All children were in end stage renal disease (ESRD) at the median age of 3 years due to lithiasis and/or nephrocalcinosis. Unfortunately, 75% of them died with a median age of 2.5 years. For the majority of adults only spontaneous elimination of urolithiasis were noted, 37.5% preserved until now a normal renal function and 62.5% of them reached ESRD at the median age of 55.8 ± 12.31 years old.
In this study 33-34InsC mutation gives a controversial clinical effect in children and adults. The implication of other genetic and/or environmental factors can play a crucial role in determining the ultimate phenotype.
1型原发性高草酸尿症(PH1)是一种罕见的异质性疾病,是突尼斯肾功能不全的主要原因之一,由AGXT基因突变引起。33-34InsC突变主要在具有严重临床特征并导致早期死亡的儿童中被描述,但在成年患者中报道较少。
使用PCR/RFLP技术对111例疑似PH1的患者(68例成人,43例儿童)进行AGXT常见突变检测。
我们描述了16例(8例成人和8例儿童)携带33-34InsC突变的病例,中位年龄为24岁[6个月-73岁]。所有儿童均因结石和/或肾钙质沉着症在3岁时进入终末期肾病(ESRD)。不幸的是,其中75%在2.5岁时死亡。对于大多数成年人,仅观察到尿石症的自发排出,37.5%至今肾功能正常,62.5%在55.8 ± 12.31岁时进入ESRD。
在本研究中,33-34InsC突变在儿童和成人中产生了有争议的临床效应。其他遗传和/或环境因素的影响在决定最终表型方面可能起关键作用。
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