Screening for Fabry disease in patients on Hemodialysis.

IF 0.8 Q3 MEDICINE, GENERAL & INTERNAL
Gaurav Batta, R Vishnuprasad, Anshita Batta, D Santhanalakshmi, Aradhana Dwivedi
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引用次数: 0

Abstract

Background: Fabry disease is an under-recognized X-linked lysosomal storage disorder characterized by the accumulation of trihexosylceramides in multifarious tissues, leading to end-organ damage, including progressive renal failure. Antecedent screening studies worldwide have shown inconsistent prevalence in the hemodialysis population. We conducted this study to screen for Fabry disease in patients undergoing dialysis at a tertiary care hospital.

Materials and methods: All patients undergoing dialysis were screened with a gal assay using dried blood spots (DBS) on filter paper using the fluorescence method. Patients with positive DBS test results were further tested for underlying mutations.

Results: A total of 112 patients (64.3% males and 35.7% females) on dialysis were screened. Nineteen patients (13 males and 6 females) were found to have low enzyme activity on DBS. Further mutation analysis confirmed that one female patient had Fabry disease. The mutation detected was a heterozygous missense variation in exon 7 of the GLA gene, which resulted in the amino acid substitution of histidine for arginine at codon 363 (p.Arg363His). Subsequent screening of the family members revealed that the son of the patient was asymptomatic and carried the same genotypic mutation. Genetic counseling was performed, and enzyme replacement therapy was offered to both patients.

Conclusions: Fabry disease remains underdiagnosed, especially in high-risk populations such as those undergoing dialysis. DBS is a convenient and effective screening tool for Fabry disease. Facilities should be augmented for similar screening studies in the dialysis population.

筛查血液透析患者的法布里病。
背景:法布里病是一种未得到充分认识的 X 连锁溶酶体贮积症,其特征是三己基甘油三酯在多种组织中蓄积,导致终末器官损伤,包括进行性肾功能衰竭。世界范围内的先期筛查研究显示,血液透析人群中的患病率并不一致。我们进行了这项研究,以筛查一家三级医院透析患者中的法布里病:所有接受透析的患者均使用滤纸上的干血斑(DBS)以荧光法进行 gal 检测。对 DBS 检测结果呈阳性的患者进一步检测潜在的基因突变:共筛查了 112 名透析患者(男性占 64.3%,女性占 35.7%)。19 名患者(13 名男性和 6 名女性)在 DBS 检测中发现酶活性较低。进一步的突变分析证实,一名女性患者患有法布里病。检测到的突变是 GLA 基因第 7 外显子的杂合性错义变异,导致第 363 密码子处的组氨酸被精氨酸取代(p.Arg363His)。随后对家庭成员进行的筛查发现,患者的儿子没有症状,但携带相同的基因型突变。我们为两位患者提供了遗传咨询和酶替代疗法:结论:法布里病仍未得到充分诊断,尤其是在高危人群中,如接受透析的人群。DBS 是一种方便有效的法布里病筛查工具。在透析人群中进行类似的筛查研究时应增加设备。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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