局灶节段性肾小球硬化患者中低α-半乳糖苷酶A酶活性的患病率意外高。
Unexpectedly High Prevalence of Low Alpha-Galactosidase A Enzyme Activity in Patients with Focal Segmental Glomerulosclerosis.
作者信息
Hasbal Nuri Baris, Caglayan Feyza Bayrakdar, Sakaci Tamer, Ahbap Elbis, Koc Yener, Sevinc Mustafa, Ucar Zuhal Atan, Unsal Abdulkadir, Basturk Taner
机构信息
Nephrology Unit, Hakkari State Hospital, Hakkari, Turkey.
Department of Nephrology Istanbul Taksim Training and Research Hospital, Istanbul, Turkey.
出版信息
Clinics (Sao Paulo). 2020 Sep 28;75:e1811. doi: 10.6061/clinics/2020/e1811. eCollection 2020.
OBJECTIVES
Fabry disease (FD) is a rare disease associated with sphingolipid accumulation. Sphingolipids are components of plasma membranes that are important in podocyte function and accumulate in various glomerular diseases such as focal segmental glomerulosclerosis (FSGS). Both FD and FSGS can cause podocyte damage and are classified as podocytopathies. In this respect, FD and FSGS share the same pathophysiologic pathways. Previous screening studies have shown that a significant proportion of end-stage renal disease (ESRD) patients receiving hemodialysis (HD) have unsuspected FD, and the prevalence of low alpha-galactosidase A (αGLA) enzyme activity in these patients is higher than that in the normal population. We aimed to compare αGLA enzyme activity in patients with biopsy-proven FSGS and ESRD receiving HD.
METHODS
The records of 232 patients [62 FSGS (F/M: 33/29); 170 HD (M/F: 93/79)] were evaluated retrospectively. The screening was performed based on the αGLA enzyme activity on a dried blood spot, with the confirmation of plasma LysoGb3 levels, and the known GLA mutations were tested in patients with low enzyme activities. The two groups were compared using these parameters.
RESULTS
The mean level of αGLA enzyme activity was found to be lower in FSGS patients than in the HD group (2.88±1.2 μmol/L/h versus 3.79±1.9 μmol/L/h, p<0.001). There was no significant relationship between the two groups with regard to the plasma LysoGb3 levels (2.2±1.22 ng/ml versus 1.7±0.66 ng/ml, p: 0.4). In the analysis of GLA mutations, a D313Y mutation [C(937G>T) in exon p] was found in one patient from the FSGS group.
CONCLUSIONS
We found that αGAL activity in patients with FSGS is lower than that in patients undergoing HD. The low enzyme activity in patients with FSGS may be explained by considering the similar pathogenesis of FSGS and FD, which may also lead to sphingolipid deposition and podocyte injury.
目的
法布里病(FD)是一种与鞘脂蓄积相关的罕见病。鞘脂是质膜的组成成分,在足细胞功能中起重要作用,并在多种肾小球疾病如局灶节段性肾小球硬化(FSGS)中蓄积。FD和FSGS均可导致足细胞损伤,二者均被归类为足细胞病。在这方面,FD和FSGS具有相同的病理生理途径。既往筛查研究表明,相当一部分接受血液透析(HD)的终末期肾病(ESRD)患者患有未被怀疑的FD,这些患者中低α - 半乳糖苷酶A(αGLA)酶活性的患病率高于正常人群。我们旨在比较经活检证实的FSGS患者和接受HD的ESRD患者的αGLA酶活性。
方法
回顾性评估232例患者的记录[62例FSGS患者(男/女:33/29);170例HD患者(男/女:93/79)]。基于干血斑上的αGLA酶活性进行筛查,并通过血浆溶血型Gb3水平进行确认,对酶活性低的患者检测已知的GLA突变。使用这些参数对两组进行比较。
结果
发现FSGS患者的αGLA酶活性平均水平低于HD组(2.88±1.2 μmol/L/h对3.79±1.9 μmol/L/h,p<0.001)。两组间血浆溶血型Gb3水平无显著相关性(2.2±1.22 ng/ml对1.7±0.66 ng/ml,p:0.4)。在GLA突变分析中,FSGS组的1例患者发现了D313Y突变[外显子p中的C(937G>T)]。
结论
我们发现FSGS患者的αGAL活性低于接受HD的患者。FSGS患者酶活性低可能是由于FSGS和FD发病机制相似,这也可能导致鞘脂沉积和足细胞损伤。
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