Delayed-onset Friedreich's ataxia revisited

被引:46
|
作者
Lecocq, Claire [1 ]
Charles, Perrine [2 ]
Azulay, Jean-Philippe [3 ]
Meissner, Wassilios [4 ,5 ]
Rai, Myriam [6 ]
N'Guyen, Karine [3 ]
Pereon, Yann [7 ]
Fabre, Nelly [8 ]
Robin, Elsa [3 ]
Courtois, Sylvie [9 ]
Guyant-Marechal, Lucie [10 ]
Zagnoli, Fabien [11 ]
Rudolf, Gabrielle [1 ]
Renaud, Mathilde [1 ]
Sevin-Allouet, Mathieu [12 ]
Lesne, Fabien [13 ,14 ]
Alaerts, Nick [6 ]
Goizet, Cyril [15 ]
Calvas, Patrick [8 ,16 ]
Eusebio, Alexandre [3 ]
Guissart, Claire [17 ]
Derkinderen, Pascal [12 ]
Tison, Francois [5 ,18 ]
Brice, Alexis [2 ,13 ,14 ]
Koenig, Michel [17 ,19 ]
Pandolfo, Massimo [6 ,20 ]
Tranchant, Christine [1 ,19 ,21 ]
Duerr, Alexandra [2 ,13 ,14 ]
Anheim, Mathieu [1 ,19 ,21 ]
机构
[1] CHU Strasbourg, Hop Hautepierre, Dept Neurol, F-67000 Strasbourg, France
[2] Hop La Pitie Salpetriere, AP HP, Dept Genet & Cytogenet, Paris, France
[3] Hop La Timone, Dept Neurol & Pathol Mouvement, Marseille, France
[4] Univ Bordeaux, Inst Malad Neurodegnerat, CNRS UMR 5293, Bordeaux, France
[5] CHU Bordeaux, Hop Pellegrin, Dept Neurol, Bordeaux, France
[6] Univ Libre Bruxelles, Lab Neurol Expt, Brussels, Belgium
[7] CHU Nantes, Hotel Dieu, Ctr Reference Malad Neuromusculaires Nantes, Lab Explorat Fonct, F-44035 Nantes 01, France
[8] CHU Toulouse, Hop Purpan, Dept Neurol, Toulouse, France
[9] Hop Emile Muller, Dept Neurol, Mulhouse, France
[10] CHU Rouen, Hop Charles Nicolle, Serv Neurophysiol, Rouen, France
[11] CHU Brest, Dept Neurol, F-29285 Brest, France
[12] CHU Nantes, Hop GR Laennec, Dept Neurol, F-44035 Nantes 01, France
[13] Univ Paris 06, Hop La Pitie Salpetriere, Inst Cerveau & Moelle, UMR S975,Ctr Rech,CNRS 7225, Paris, France
[14] INSERM, UMR S975, Paris, France
[15] Univ Bordeaux, CHU Bordeaux, Serv Genet Med, Lab Malad Rares Genet & Metab MRGM,EA4576, Bordeaux, France
[16] CHU Toulouse, Hop Purpan, Serv Genet Med, Toulouse, France
[17] Univ Montpellier, CHU Montpellier, Inst Univ Rech Clin, Genet Mol Lab, F-34059 Montpellier, France
[18] Univ Bordeaux, Inst Malad Neurodegenerat, CNRS UMR 5293, Bordeaux, France
[19] Univ Strasbourg, CNRS UMR7104, INSERM U964, Inst Genet & Biol Mol & Cellulaire, Illkirch Graffenstaden, France
[20] Free Univ Brussels, Hop Erasme, Dept Neurol, 808 Route Lennik, B-1070 Brussels, Belgium
[21] Univ Strasbourg, Federat Med Translat Strasbourg, Strasbourg, France
来源
MOVEMENT DISORDERS | 2016年 / 31卷 / 01期
关键词
Friedreich's ataxia; genetics; corticospinal tract; peripheral neuropathy; imaging; GAA TRIPLET REPEAT; CLINICAL-FEATURES; MOLECULAR-GENETICS; CEREBELLAR-ATAXIA; POINT MUTATIONS; TENDON REFLEXES; SPASTIC ATAXIA; EXPANSION; DISEASE; AGE;
D O I
10.1002/mds.26382
中图分类号
R74 [神经病学与精神病学];
学科分类号
摘要
BackgroundFriedreich's ataxia usually occurs before the age of 25. Rare variants have been described, such as late-onset Friedreich's ataxia and very-late-onset Friedreich's ataxia, occurring after 25 and 40 years, respectively. We describe the clinical, functional, and molecular findings from a large series of late-onset Friedreich's ataxia and very-late-onset Friedreich's ataxia and compare them with typical-onset Friedreich's ataxia. MethodsPhenotypic and genotypic comparison of 44 late-onset Friedreich's ataxia, 30 very late-onset Friedreich's ataxia, and 180 typical Friedreich's ataxia was undertaken. ResultsDelayed-onset Friedreich's ataxia (late-onset Friedreich's ataxia and very-late-onset Friedreich's ataxia) had less frequently dysarthria, abolished tendon reflexes, extensor plantar reflexes, weakness, amyotrophy, ganglionopathy, cerebellar atrophy, scoliosis, and cardiomyopathy than typical-onset Friedreich's ataxia, along with less severe functional disability and shorter GAA expansion on the smaller allele (P<0.001). Delayed-onset Friedreich's ataxia had lower scale for the assessment and rating of ataxia and spinocerebellar degeneration functional scores and longer disease duration before wheelchair confinement (P<0.001). Both GAA expansions were negatively correlated to age at disease onset (P<0.001), but the smaller GAA expansion accounted for 62.9% of age at onset variation and the larger GAA expansion for 15.6%. In this comparative study of late-onset Friedreich's ataxia and very-late-onset Friedreich's ataxia, no differences between these phenotypes were demonstrated. ConclusionTypical- and delayed-onset Friedreich's ataxia are different and Friedreich's ataxia is heterogeneous. Late-onset Friedreich's ataxia and very-late-onset Friedreich's ataxia appear to belong to the same clinical and molecular continuum and should be considered together as delayed-onset Friedreich's ataxia. As the most frequently inherited ataxia, Friedreich's ataxia should be considered facing compatible pictures, including atypical phenotypes (spastic ataxia, retained reflexes, lack of dysarthria, and lack of extraneurological signs), delayed disease onset (even after 60 years of age), and/or slow disease progression.
引用
收藏
页码:62 / 69
页数:8
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