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Use of a rare disease registry for establishing phenotypic classification of previously unassigned variants: a consensus classification system by a multispecialty Fabry disease genotype-phenotype workgroup.利用罕见病登记处对先前未分配的变异体进行表型分类:多学科法布里病基因型-表型工作组的共识分类系统。
J Med Genet. 2020 Aug;57(8):542-551. doi: 10.1136/jmedgenet-2019-106467. Epub 2020 Mar 11.
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Newborn screening for Fabry disease in the western region of Japan.日本西部地区法布里病的新生儿筛查。
Mol Genet Metab Rep. 2020 Jan 11;22:100562. doi: 10.1016/j.ymgmr.2019.100562. eCollection 2020 Mar.
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ClinVar: improvements to accessing data.ClinVar:访问数据的改进。
Nucleic Acids Res. 2020 Jan 8;48(D1):D835-D844. doi: 10.1093/nar/gkz972.
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High-risk screening for Anderson-Fabry disease in patients with cardiac, renal, or neurological manifestations.对有心脏、肾脏或神经表现的患者进行安德森-法布里病的高危筛查。
J Hum Genet. 2019 Sep;64(9):891-898. doi: 10.1038/s10038-019-0633-1. Epub 2019 Jun 19.
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Consensus recommendations for diagnosis, management and treatment of Fabry disease in paediatric patients.《儿童法布里病诊断、治疗和管理的共识建议》。
Clin Genet. 2019 Aug;96(2):107-117. doi: 10.1111/cge.13546. Epub 2019 Jun 6.
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A Novel α-Galactosidase A Splicing Mutation Predisposes to Fabry Disease.一种新型α-半乳糖苷酶A剪接突变易患法布里病。
Front Genet. 2019 Feb 11;10:60. doi: 10.3389/fgene.2019.00060. eCollection 2019.
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Safety and effectiveness of enzyme replacement therapy with agalsidase alfa in patients with Fabry disease: Post-marketing surveillance in Japan.阿加糖酶阿尔法治疗法在法布瑞氏病患者中的安全性和有效性:日本的上市后监测。
Mol Genet Metab. 2019 Apr;126(4):448-459. doi: 10.1016/j.ymgme.2019.02.005. Epub 2019 Feb 20.
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Fabry disease in a Japanese population-molecular and biochemical characteristics.日本人群中的法布里病——分子和生化特征
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Effectiveness of plasma lyso-Gb3 as a biomarker for selecting high-risk patients with Fabry disease from multispecialty clinics for genetic analysis.血浆溶菌酶糖脂酰基鞘氨醇作为生物标志物用于从多学科诊所选择进行基因分析的法布雷病高危患者的有效性。
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10
Enzyme replacement therapy in a patient of heterozygous Fabry disease: clinical and pathological evaluations by repeat kidney biopsy and a successful pregnancy.杂合子法布里病患者的酶替代疗法:通过重复肾活检进行的临床和病理评估及一次成功妊娠
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通过新生儿和高危筛查检测日本患者中新型法布里病相关致病变异

Detection of novel Fabry disease-associated pathogenic variants in Japanese patients by newborn and high-risk screening.

作者信息

Sawada Takaaki, Kido Jun, Sugawara Keishin, Matsumoto Shirou, Takada Fumio, Tsuboi Kazuya, Ohtake Akira, Endo Fumio, Nakamura Kimitoshi

机构信息

Department of Pediatrics, Graduate School of Medical Sciences, Kumamoto University, Kumamoto, Japan.

Department of Medical Genetics and Genomics, Kitasato University Graduate School of Medical Sciences, Kanagawa, Japan.

出版信息

Mol Genet Genomic Med. 2020 Nov;8(11):e1502. doi: 10.1002/mgg3.1502. Epub 2020 Oct 5.

DOI:10.1002/mgg3.1502
PMID:33016649
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7667298/
Abstract

BACKGROUND

In Japan, newborn and high-risk screening for Fabry disease (FD), an inherited X-linked disorder caused by GLA mutations, using dried blood spots was initiated in 2006. In newborn screening, 599,711 newborns were screened by December 2018, and 57 newborns from 54 families with 26 FD-associated variants were detected. In high-risk screening, 18,235 individuals who had symptoms and/or a family history of FD were screened by March 2019, and 236 individuals from 143 families with 101 FD-associated variants were detected. Totally 3, 116 variants were detected; 41 of these were not registered in Fabry-database.org or ClinVar and 33 were definitely novel. Herein, we report the clinical outcomes and discuss the pathogenicity of the 41 variants.

METHODS

We traced nine newborns and 46 individuals with the 33 novel variants, and nine newborns and 10 individuals with eight other variants not registered in the FD database, and analyzed the information on symptoms, treatments, and outcomes.

RESULTS

Thirty-eight of the 46 individuals with the 33 novel variants showed symptoms and received enzyme-replacement therapy and/or chaperone treatment.

CONCLUSION

Delayed diagnosis should be avoided in patients with FD. Our results will help clinicians diagnose FD and determine the appropriate treatment for patients with these variants.

摘要

背景

在日本,2006年开始使用干血斑对法布里病(FD)进行新生儿和高危筛查,法布里病是一种由GLA突变引起的遗传性X连锁疾病。在新生儿筛查中,截至2018年12月共筛查了599,711名新生儿,检测出54个家庭的57名新生儿携带26种与FD相关的变异。在高危筛查中,截至2019年3月共筛查了18,235名有FD症状和/或家族史的个体,检测出143个家庭的236名个体携带101种与FD相关的变异。总共检测到3116种变异;其中41种未在Fabry-database.org或ClinVar中登记,33种肯定是新的。在此,我们报告临床结果并讨论这41种变异的致病性。

方法

我们追踪了9名携带33种新变异的新生儿和46名个体,以及9名携带8种未在FD数据库中登记的其他变异的新生儿和10名个体,并分析了症状、治疗和结果方面的信息。

结果

46名携带33种新变异的个体中有38名出现症状并接受了酶替代疗法和/或伴侣蛋白治疗。

结论

应避免FD患者的诊断延迟。我们的结果将有助于临床医生诊断FD并确定这些变异患者的适当治疗方法。