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Abstract

Background:

The global prevalence of ischemic stroke in young adults is increasing, leading to a significant social impact. Fabry disease is a recognized cause of ischemic stroke in young patients, and although disease-modifying treatments are available, further evidence is needed to confirm their effectiveness in reducing the incidence of ischemic strokes.

Aims:

This study aimed to identify undiagnosed Fabry disease in young adult patients with ischemic stroke in a Taiwanese cohort.

Methods:

This multicenter, prospective cohort study enrolled patients aged 20–55 years who had experienced an ischemic stroke or transient ischemic attack (TIA) within 10 days, from 1 January 2016 to 31 December 2020. Screening for Fabry disease was performed using a dry blood test to measure α-galactosidase activity in male patients and blood globotriaosylsphingosine (lyso-Gb3) levels in female patients. For patients with positive screen results, genetic diagnosis of Fabry disease was pursued through Sanger sequencing of the GLA gene, covering all exons and a segment of intron 4.

Results:

A total of 977 patients (659 male, 68%) were enrolled from seven hospitals across Taiwan. Four patients (0.4%, all male) had positive screening results, and two patients (0.2%) were genetically diagnosed with Fabry disease. Case 1 had the GLA c.658C>T mutation and experienced ischemic stroke in the bilateral occipital regions. Case 2 had the GLA c.640-801G>A mutation and experienced an ischemic stroke in the left superficial watershed area.

Conclusion:

The prevalence of undiagnosed Fabry disease in this cohort of Taiwanese young adults with ischemic stroke or TIA was 0.3% among the young male population. Understanding the prevalence of undiagnosed Fabry disease in young adults with ischemic stroke could help shape future Fabry disease screening policies.

Data access statement:

The collected data will be available upon reasonable request from the corresponding author.

Keywords

Fabry disease competing diagnosis ischemic stroke young stroke epidemiology

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References

Campbell

BCV

Khatri

Stroke. Lancet 2020; 396: 129–142.

Tsao

Aday

Almarzooq

, et al. Heart disease and stroke statistics-2023 update: a report from the American Heart Association. Circulation 2023; 147: e93–e621.

Feigin

Brainin

Norrving

, et al. World Stroke Organization (WSO): global stroke fact sheet 2022. Int J Stroke 2022; 17: 18–29.

Krishnamurthi

Moran

Feigin

, et al. Stroke prevalence, mortality and disability-adjusted life years in adults aged 20-64 years in 1990-2013: data from the Global Burden of Disease 2013 Study. Neuroepidemiology 2015; 45: 190–202.

George

Tong

Bowman

BA.

Prevalence of cardiovascular risk factors and strokes in younger adults. JAMA Neurol 2017; 74: 695–703.

Hathidara

Saini

Malik

AM.

Stroke in the young: a global update. Curr Neurol Neurosci Rep 2019; 19: 91.

Lee

Yang

Lee

, et al. Genomic screening of Fabry disease in young stroke patients: the Taiwan experience and a review of the literature. Eur J Neurol 2019; 26: 553–555.

Sheng

Nalleballe

, et al. Fabry’s disease and stroke: effectiveness of enzyme replacement therapy (ERT) in stroke prevention, a review with meta-analysis. J Clin Neurosci 2019; 65: 83–86.

Hwu

Chien

Lee

, et al. Newborn screening for Fabry disease in Taiwan reveals a high incidence of the later-onset GLA mutation c.936+919G>A (IVS4+919G>A). Hum Mutat 2009; 30: 1397–1405.

10.

National Health Insurance Administration MoHaW. The rate of prescribing antithrombotic medication at discharge for patients with ischemic stroke or transient ischemic attack, https://data.gov.tw/dataset/79567 (2024, accessed August 2024).

11.

Béjot

Daubail

Jacquin

, et al. Trends in the incidence of ischaemic stroke in young adults between 1985 and 2011: the Dijon Stroke Registry. J Neurol Neurosurg Psychiatry 2014; 85: 509–513.

12.

Chien

Lee

Chen

, et al. Newborn screening for Morquio disease and other lysosomal storage diseases: results from the 8-plex assay for 70,000 newborns. Orphanet J Rare Dis 2020; 15: 38.

13.

Johnson

Mascher

, et al. Analysis of lyso-globotriaosylsphingosine in dried blood spots. Ann Lab Med 2013; 33: 274–278.

14.

Meaney

Blanch

Morris

CP.

A nonsense mutation (R220X) in the alpha-galactosidase A gene detected in a female carrier of Fabry disease. Hum Mol Genet 1994; 3: 1019–1020.

15.

Lin

Huang

, et al. Enzyme assay and clinical assessment in subjects with a Chinese hotspot late-onset Fabry mutation (IVS4 + 919G→A). J Inherit Metab Dis 2010; 33: 619–624.

16.

Palhais

Dembic

Sabaratnam

, et al. The prevalent deep intronic c. 639+919 G>A GLA mutation causes pseudoexon activation and Fabry disease by abolishing the binding of hnRNPA1 and hnRNP A2/B1 to a splicing silencer. Mol Genet Metab 2016; 119: 258–269.

17.

Lau

Schulz

, et al. Total small vessel disease score and risk of recurrent stroke: validation in 2 large cohorts. Neurology 2017; 88: 2260–2267.

18.

Tomek

Petra

Paulasová Schwabová

, et al. Nationwide screening for Fabry disease in unselected stroke patients. PLoS ONE 2021; 16: e0260601.

19.

Malavera

Cadilhac

Thijs

, et al. Screening for Fabry disease in young strokes in the Australian Stroke Clinical Registry (AuSCR). Front Neurol 2020; 11: 596420.

20.

Güler

Fabry disease frequency among young cryptogenic stroke patients in the city of Edirne, Turkey. Neurologist 2021; 26: 125–131.

21.

Song

Xue

Zhao

Screening for Fabry’s disease in young patients with ischemic stroke in a Chinese population. Int J Neurosci 2017; 127: 350–355.

22.

Lee

Lin

, et al. High-throughput detection of common sequence variations of Fabry disease in Taiwan using DNA mass spectrometry. Mol Genet Metab 2014; 111: 507–512.

23.

Ortiz

Germain

Desnick

, et al. Fabry disease revisited: management and treatment recommendations for adult patients. Mol Genet Metab 2018; 123: 416–427.

24.

Chien

Lee

Chiang

Desnick

Hwu

W-L.

Fabry disease: incidence of the common later-onset α-galactosidase A IVS4+919G→A mutation in Taiwanese newborns—Superiority of DNA-based to enzyme-based newborn screening for common mutations. Mol Med 2012; 18: 780–784.

25.

Baydakova

Ilyushkina

Moiseev

, et al. α-Galactosidase A/lysoGb3 ratio as a potential marker for Fabry disease in females. Clin Chim Acta 2020; 501: 27–32.

26.

Izhar

Borriello

La Russa

, et al. Fabry disease in women: genetic basis, available biomarkers, and clinical manifestations. Genes (Basel) 2023; 15: 37.

27.

Liao

Huang

Chen

, et al. Plasma globotriaosylsphingosine (lysoGb3) could be a biomarker for Fabry disease with a Chinese hotspot late-onset mutation (IVS4+919G>A). Clin Chim Acta 2013; 426: 114–120.

28.

Huang

Wang

, et al. Improvement in the sensitivity of newborn screening for Fabry disease among females through the use of a high-throughput and cost-effective method, DNA mass spectrometry. J Hum Genet 2018; 63: 1–8.

29.

Moore

Kaneski

Askari

Schiffmann

The cerebral vasculopathy of Fabry disease. J Neurol Sci 2007; 257: 258–263.

30.

Kolodny

Fellgiebel

Hilz

, et al. Cerebrovascular involvement in Fabry disease: current status of knowledge. Stroke 2015; 46: 302–313.

31.

Fellgiebel

Keller

Marin

, et al. Diagnostic utility of different MRI and MR angiography measures in Fabry disease. Neurology 2009; 72: 63–68.

32.

Lee

Hung

Hsu

, et al. Brain MR imaging findings of cardiac-type Fabry disease with an IVS4+919G>A mutation. Am J Neuroradiol 2016; 37: 1044–1049.

33.

Lee

Hsu

Hung

, et al. A comparison of central nervous system involvement in patients with classical Fabry disease or the later-onset subtype with the IVS4+919G>A mutation. BMC Neurol 2017; 17: 25.

34.

Sims

Politei

Banikazemi

Lee

Stroke in Fabry disease frequently occurs before diagnosis and in the absence of other clinical events: natural history data from the Fabry Registry. Stroke 2009; 40: 788–794.

35.

Gomes

Nora

Becker

, et al. Nerve conduction studies, electromyography and sympathetic skin response in Fabry’s disease. J Neurol Sci 2003; 214: 21–25.

36.

Schäfer

Baron

Widmer

, et al. Thirty-four novel mutations of the GLA gene in 121 patients with Fabry disease. Hum Mutat 2005; 25: 412.

37.

Okada

Horinouchi

Yamamura

, et al. All reported non-canonical splice site variants in GLA cause aberrant splicing. Clin Exp Nephrol 2023; 27: 737–746.

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Investigating undiagnosed Fabry disease in young adults with ischemic stroke: A multicenter cohort study

Abstract

Background:

Aims:

Methods:

Results:

Conclusion:

Data access statement:

Keywords

Get full access to this article

References

Supplementary Material