Ataxia with oculomotor apraxia type 2: clinical, biological and genotype/phenotype correlation study of a cohort of 90 patients

被引：172

作者：

Anheim, M. ^{[1
,2
,3
]}

Monga, B. ^{[1
,4
]}

Fleury, M. ^{[2
]}

Charles, P. ^{[3
]}

Barbot, C. ^{[5
,6
]}

Salih, M. ^{[7
]}

Delaunoy, J. P. ^{[8
]}

Fritsch, M. ^{[8
]}

Arning, L. ^{[9
]}

Synofzik, M. ^{[10
,11
]}

Schoels, L. ^{[10
,11
]}

Sequeiros, J. ^{[12
]}

Goizet, C. ^{[13
]}

Marelli, C. ^{[3
]}

Le Ber, I. ^{[3
,14
,15
]}

Koht, J. ^{[3
,14
,16
]}

Gazulla, J. ^{[17
]}

De Bleecker, J. ^{[18
]}

Mukhtar, M. ^{[19
]}

Drouot, N. ^{[1
]}

Ali-Pacha, L. ^{[20
]}

Benhassine, T. ^{[21
]}

Chbicheb, M. ^{[22
]}

M'Zahem, A. ^{[23
]}

Hamri, A. ^{[23
]}

Chabrol, B. ^{[24
]}

Pouget, J. ^{[25
]}

Murphy, R. ^{[26
]}

Watanabe, M. ^{[27
]}

Coutinho, P. ^{[5
,6
]}

Tazir, M. ^{[20
]}

Durr, A. ^{[3
,14
,15
]}

Brice, A. ^{[3
,14
,15
]}

Tranchant, C. ^{[1
,2
]}

Koenig, M. ^{[1
,8
]}

机构：

[1] Univ Strasbourg, CNRS, Inst Genet & Biol Mol & Cellulaire, INSERM, Illkirch Graffenstaden, France

[2] Hop Civil, Dept Neurol, Strasbourg, France

[3] Hop La Pitie Salpetriere, AP HP, Dept Genet & Cytogenet, F-75013 Paris, France

[4] Univ Lubumbashi, Fac Med, Lubumbashi, DEM REP CONGO

[5] Hop S Sebastiao, Dept Neurol, Santa Maria Feira, Portugal

[6] UP, IBMC, UnIGENe, Oporto, Portugal

[7] King Saud Univ, Coll Med, Div Paediat Neurol, Riyadh 11461, Saudi Arabia

[8] Nouvel Hop Civil, Lab Diagnost Genet, Strasbourg, France

[9] Ruhr Univ Bochum, Dept Human Genet, D-44780 Bochum, Germany

[10] Clin Neurogenet Ctr Neurol, Div Res, D-72076 Tubingen, Germany

[11] Hertie Inst Clin Brain Res, D-72076 Tubingen, Germany

[12] Univ Porto, BMC, Inst Mol & Cell Biol, ICBAS, Oporto, Portugal

[13] Univ Bordeaux 2, Lab Genet Humaine, CHU Bordeaux, Serv Genet Med, F-33076 Bordeaux, France

[14] INSERM, CRicm UMRS975, F-75013 Paris, France

[15] Univ Paris 06, CRicm UMRS975, F-75005 Paris, France

[16] Univ Oslo, Fac Med, N-0316 Oslo, Norway

[17] Hosp Univ Miguel Servet, Serv Neurol, Zaragoza, Spain

[18] Ghent Univ Hosp, Dept Neurol, B-9000 Ghent, Belgium

[19] Univ Khartoum, Inst Endem Dis, Fac Med, Khartoum, Sudan

[20] CHU Mustapha, Serv Neurol, Lab Rech Neurosci, Algiers, Algeria

[21] Univ Bab Ezzouar, Biol Cellulaire & Mol Lab, Algiers, Algeria

[22] Hop Narbonne, Serv Neurol, Narbonne, France

[23] Hop Benbadis, CHU Constantine, Serv Neurol, Benbadis, Algeria

[24] Hop La Timone Enfants, Serv Pediat, Marseille, France

[25] CHU Timone, Dept Neurol & Neuromuscular Dis, Marseille, France

[26] Adelaide & Meath Hosp Univ Dublin, Dublin 24, Ireland

[27] Hirosaki Univ, Grad Sch Med, Dept Neurol, Inst Brain Sci, Hirosaki, Aomori 0368562, Japan

来源：

BRAIN | 2009年 / 132卷

关键词：

ataxia; oculomotor apraxia; polyneuropathy; alpha-feto-protein; cerebellar atrophy; AMYOTROPHIC-LATERAL-SCLEROSIS; OCULAR MOTOR APRAXIA; PERIPHERAL NEUROPATHY; SPINOCEREBELLAR ATAXIA; CEREBELLAR ATROPHY; ALPHA-FETOPROTEIN; GENE; SENATAXIN; TELANGIECTASIA; MUTATIONS;

D O I：

10.1093/brain/awp211

中图分类号：

R74 [神经病学与精神病学];

学科分类号：

摘要：

Ataxia with oculomotor apraxia type 2 (AOA2) is an autosomal recessive disease due to mutations in the senataxin gene, causing progressive cerebellar ataxia with peripheral neuropathy, cerebellar atrophy, occasional oculomotor apraxia and elevated alpha-feto-protein (AFP) serum level. We compiled a series of 67 previously reported and 58 novel ataxic patients who underwent senataxin gene sequencing because of suspected AOA2. An AOA2 diagnosis was established for 90 patients, originating from 15 countries worldwide, and 25 new senataxin gene mutations were found. In patients with AOA2, median AFP serum level was 31.0 mu g/l at diagnosis, which was higher than the median AFP level of AOA2 negative patients: 13.8 mu g/l, P = 0.0004; itself higher than the normal level (3.4 mu g/l, range from 0.5 to 17.2 mu g/l) because elevated AFP was one of the possible selection criteria. Polyneuropathy was found in 97.5% of AOA2 patients, cerebellar atrophy in 96%, occasional oculomotor apraxia in 51%, pyramidal signs in 20.5%, head tremor in 14%, dystonia in 13.5%, strabismus in 12.3% and chorea in 9.5%. No patient was lacking both peripheral neuropathy and cerebellar atrophy. The age at onset and presence of occasional oculomotor apraxia were negatively correlated to the progression rate of the disease (P = 0.03 and P = 0.009, respectively), whereas strabismus was positively correlated to the progression rate (P = 0.03). An increased AFP level as well as cerebellar atrophy seem to be stable in the course of the disease and to occur mostly at or before the onset of the disease. One of the two patients with a normal AFP level at diagnosis had high AFP levels 4 years later, while the other had borderline levels. The probability of missing AOA2 diagnosis, in case of sequencing senataxin gene only in non-Friedreich ataxia non-ataxia-telangiectasia ataxic patients with AFP level >= 7 mu g/l, is 0.23% and the probability for a non-Friedreich ataxia non-ataxia-telangiectasia ataxic patient to be affected with AOA2 with AFP levels >= 7 mu g/l is 46%. Therefore, selection of patients with an AFP level above 7 mu g/l for senataxin gene sequencing is a good strategy for AOA2 diagnosis. Pyramidal signs and dystonia were more frequent and disease was less severe with missense mutations in the helicase domain of senataxin gene than with missense mutations out of helicase domain and deletion and nonsense mutations (P = 0.001, P = 0.008 and P = 0.01, respectively). The lack of pyramidal signs in most patients may be explained by masking due to severe motor neuropathy.

引用

页码：2688 / 2698

页数：11

共 41 条

[1] Hereditary persistence of α-fetoprotein is due to both proximal and distal hepatocyte nuclear factor-1 site mutations [J].