Lin Hsiang-Yu, Chong Kah-Wai, Hsu Ju-Hui, Yu Hsiao-Chi, Shih Chun-Che, Huang Cheng-Hung, Lin Shing-Jong, Chen Chen-Huan, Chiang Chuan-Chi, Ho Huey-Jane, Lee Pi-Chang, Kao Chuan-Hong, Cheng Kang-Hsiang, Hsueh Chuen, Niu Dau-Ming
Institute of Clinical Medicine, National Yang-Ming University, Taipei, Taiwan.
Circ Cardiovasc Genet. 2009 Oct;2(5):450-6. doi: 10.1161/CIRCGENETICS.109.862920. Epub 2009 Jul 24.
Fabry disease is a treatable lysosomal storage disorder, which is often misdiagnosed or belatedly diagnosed.
To determine the disease incidence in the Taiwan Chinese population, a Fabry disease newborn screening study was initiated. A total of 110 027 newborns were screened by assaying the alpha-galactosidase A (alpha-Gal A) activity using dry blood spots. Low plasma alpha-Gal A activity and presence of a Fabry mutation was demonstrated in 45 neonates (3 females). Eight different mutations were identified, including 3 known missense mutations (R112H, A143T, and R356W), 4 novel missense mutations (G104V, M296L, G360C, and K391T), and one known intronic mutation (IVS4+919G-->A). The IVS4+919G-->A mutation was most common (82% of patients). A total of 20 maternal grandparents of infants harboring this intronic mutation were evaluated by echocardiography, mutation analysis and alpha-Gal A activity assay. The intronic mutation was found in 9 grandfathers and 11 grandmothers. Of these grandparents, 3 grandfathers (33%) but none of the grandmothers had hypertrophic cardiomyopathy. Additionally, 16 males who had been diagnosed with idiopathic hypertrophic cardiomyopathy were screened by mutation analysis and alpha-Gal A activity; 4 (25%) showed deficient plasma alpha-Gal A activity in combination with the intronic mutation.
We found an unexpected high prevalence of the cardiac variant Fabry mutation IVS4+919G-->A among both newborns (approximately 1 in 1600 males) and patients with idiopathic hypertrophic cardiomyopathy in the Taiwan Chinese population. The early identification of undiagnosed patients allows timely therapeutic intervention providing a better clinical outcome.
法布里病是一种可治疗的溶酶体贮积症,常被误诊或诊断延迟。
为确定台湾华裔人群中的疾病发病率,启动了一项法布里病新生儿筛查研究。通过使用干血斑检测α - 半乳糖苷酶A(α - Gal A)活性,对总共110027名新生儿进行了筛查。45名新生儿(3名女性)表现出低血浆α - Gal A活性及法布里突变。鉴定出8种不同突变,包括3种已知错义突变(R112H、A143T和R356W)、4种新错义突变(G104V、M296L、G360C和K391T)以及1种已知内含子突变(IVS4 + 919G→A)。IVS4 + 919G→A突变最为常见(占患者的82%)。通过超声心动图、突变分析和α - Gal A活性测定,对总共20名携带此内含子突变婴儿的祖父母进行了评估。在9名祖父和11名祖母中发现了该内含子突变。在这些祖父母中,3名祖父(33%)患有肥厚型心肌病,而祖母中无人患病。此外,对16名已诊断为特发性肥厚型心肌病的男性进行了突变分析和α - Gal A活性筛查;4名(25%)表现出血浆α - Gal A活性不足并伴有内含子突变。
我们发现,在台湾华裔人群的新生儿(约每1600名男性中有1例)和特发性肥厚型心肌病患者中,心脏变异型法布里突变IVS4 + 919G→A的患病率出乎意料地高。对未确诊患者的早期识别可实现及时的治疗干预,从而带来更好的临床结果。
