D313Y mutation in the differential diagnosis of white matter lesions: Experiences from a multiple sclerosis outpatient clinic

被引：9

作者：

Becker, Jana ^{[1
]}

Rolfs, Arndt ^{[2
]}

Karabul, Nesrin ^{[3
]}

Berlit, Peter ^{[1
]}

Kraemer, Markus ^{[1
]}

机构：

[1] Alfried Krupp Hosp, Dept Neurol, Alfried Krupp Str 21, D-45117 Essen, Germany

[2] Univ Rostock, Albrecht Kossel Inst, Rostock, Germany

[3] Univ Bochum, Child Neurol Clin, Bochum, Germany

来源：

MULTIPLE SCLEROSIS JOURNAL | 2016年 / 22卷 / 11期

关键词：

Genetics; magnetic resonance imaging; multiple sclerosis; T2; lesions; ANDERSON-FABRY DISEASE; ALPHA-GALACTOSIDASE;

D O I：

10.1177/1352458516638747

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

White matter lesions (WML) in younger patients might be due to a variety of neurological disorders. Fabry disease (FD), an x-linked inherited lysosomal storage disorder, happens to be misdiagnosed as multiple sclerosis (MS). In two middle-aged female patients, presenting bilateral WML, diagnosis of MS turned out to be doubtful. Human genetic analysis presented the Fabry mutation D313Y, in which clinical impact is still unclear. Disease manifestations outside the central nervous system were not detected. Our findings support the suspicion that Fabry mutation D313Y may be involved in neural damage resulting in WML.

引用

页码：1502 / 1505

页数：4

共 8 条

[1] Fabry Disease - Underestimated in the Differential Diagnosis of Multiple Sclerosis? [J].

Boettcher, Tobias ;

Rolfs, Arndt ;

Tanislav, Christian ;

Bitsch, Andreas ;

Koehler, Wolfgang ;

Gaedeke, Jens ;

Giese, Anne-Katrin ;

Kolodny, Edwin H. ;

Duning, Thomas .

PLOS ONE, 2013, 8 (08)

[2] Newborn Screening for Fabry Disease in Taiwan Reveals a High Incidence of the Later-Onset GLA Mutation c.936+919G > A (IVS4+919G > A) [J].

Hwu, Wuh-Liang ;

Chien, Yin-Hsiu ;

Lee, Ni-Chung ;

Chiang, Shu-Chuan ;

Dobrovolny, Robert ;

Huang, Ai-Chu ;

Yeh, Hui-Ying ;

Chao, May-Chin ;

Lin, Shio-Jean ;

Kitagawa, Teruo ;

Desnick, Robert J. ;

Hsu, Li-Wen .

HUMAN MUTATION, 2009, 30 (10) :1397-1405

[3] s Multifocal White Matter Lesions Associated with the D313Y Mutation of the α-Galactosidase A Gene [J].

Lenders, Malte ;

Duning, Thomas ;

Schelleckes, Michael ;

Schmitz, Boris ;

Stander, Sonja ;

Rolfs, Arndt ;

Brand, Stefan-Martin ;

Brand, Eva .

PLOS ONE, 2013, 8 (02)

[4]

Niemann M, 2013, JIMD REP, V7, P99, DOI 10.1007/8904_2012_154

[5]

Scolding N, 2001, J NEUROL NEUROSUR PS, V71, pII9

[6] High incidence of later-onset Fabry disease revealed by newborn screening [J].

Spada, Marco ;

Pagliardini, Severo ;

Yasuda, Makiko ;

Tukel, Turgut ;

Thiagarajan, Geetha ;

Sakuraba, Hitoshi ;

Ponzone, Alberto ;

Desnick, Robert J. .

AMERICAN JOURNAL OF HUMAN GENETICS, 2006, 79 (01) :31-40

[7] A family with various symptomatology suggestive of Anderson-Fabry disease and a genetic polymorphism of alpha galactosidase A gene [J].

Tuttolomondo, Antonino ;

Duro, Giovanni ;

Pecoraro, Rosaria ;

Simonetta, Irene ;

Miceli, Salvatore ;

Colomba, Paolo ;

Zizzo, Carmela ;

Di Chiara, Tiziana ;

Scaglione, Rosario ;

Della Corte, Vittoriano ;

Corpora, Francesca ;

Pinto, Antonio .

CLINICAL BIOCHEMISTRY, 2015, 48 (1-2) :55-62

[8] Neurological Complications of Anderson-Fabry Disease [J].

Tuttolomondo, Antonino ;

Pecoraro, Rosaria ;

Simonetta, Irene ;

Miceli, Salvatore ;

Arnao, Valentina ;

Licata, Giuseppe ;

Pinto, Antonio .

CURRENT PHARMACEUTICAL DESIGN, 2013, 19 (33) :6014-6030

← 1 →