Anheim Mathieu, Mariani Louise-Laure, Calvas Patrick, Cheuret Emmanuel, Zagnoli Fabien, Odent Sylvie, Seguela Claire, Marelli Cecilia, Fritsch Marlène, Delaunoy Jean-Pierre, Brice Alexis, Dürr Alexandra, Koenig Michel
Université Pierre et Marie Curie, Centre de Recherche de l’Institut du Cerveau et de la Moelle épinière, Institut National de la Santé et de la Recherche Médicale, France.
Arch Neurol. 2012 Jul;69(7):912-6. doi: 10.1001/archneurol.2011.834.
Friedreich ataxia (FA) is the most frequent type of autosomal recessive cerebellar ataxia, occurring at a mean age of 16 years. Nearly 98% of patients with FA present with homozygous GAA expansions in the FXN gene. The remaining patients are compound heterozygous for an expansion and a point mutation. Patients who are compound heterozygous for an exonic deletion and an expansion are exquisitely rare.
To describe 6 patients affected with FA due to an exonic deletion mutation (FAexdel) and to compare these 6 patients with FAexdel with 46 patients consecutively diagnosed with typical FA due to homozygous GAA expansion and whose small expansions were within the same range as that of the expansions of the patients with FAexdel.
Description of a series.
Academic research.
Six patients with FAexdel and 46 patients with typical FA.
FXN gene analysis, including assessments of GAA expansion and exon sequencing and determination of exonic copy numbers using multiplex ligation-dependent probe amplification.
We identified 6 patients with FA who presented with the combination of 1 GAA expansion and 1 FXN exonic deletion. The mean (SD) age at onset of the disease was earlier for patients with FAexdel (7 [4] years [range, 3-12 years]) than for patients with typical FA (15 [5] years [range, 6-30 years]) (P = .001), and the median time to confinement to wheelchair was shorter for patients with FAexdel (20 years) than for patients with typical FA (28 years) (P = .002). There was no difference between the mean (SD) size of the expansion for the patients with FAexdel (780 [256] GAA triplet repeat sequences [range, 340-1070 GAA triplet repeat sequences]) and the mean (SD) size of the short expansion for the patients with typical FA (634 [163] GAA triplet repeat sequences [range, 367-1000 GAA triplet repeat sequences]) (P = .10). The mean disease duration before becoming wheelchair bound was shorter for patients with FAexdel (9 years) than for patients with typical FA (13 years), and the incidence of cardiomyopathy was higher for patients with FAexdel (84%) than for patients with typical FA (68%). However, these differences were not significant, probably owing to the small size of the FAexdel group. The other extraneurological signs, such as scoliosis or diabetes mellitus, were particularly frequently observed in the FAexdel group. One patient presented at 9 years of age with severe angina and marked cardiomyopathy that confined her to a wheelchair. Three patients had disabling autonomic disturbances. It appears that exonic deletion significantly contributes to the clinical picture of patients with FA.
Friedreich ataxia due to an exonic deletion mutation corresponds to an early onset and severe variant of FA. FXN should be investigated for exonic deletion in patients with early-onset FA in which only 1 GAA expansion without a point mutation is found. Patients with FAexdel have to be carefully observed using cardiological, orthopaedic, endocrinological, gastroenterological, and ophthalmological data. Friedreich ataxia due to an exonic deletion mutation should be suspected in young patients presenting with severe scoliosis.
弗里德赖希共济失调(FA)是常染色体隐性小脑共济失调最常见的类型,平均发病年龄为16岁。近98%的FA患者FXN基因存在纯合GAA扩增。其余患者为扩增与点突变的复合杂合子。外显子缺失与扩增的复合杂合子患者极为罕见。
描述6例因外显子缺失突变导致的FA患者(FAexdel),并将这6例FAexdel患者与46例因纯合GAA扩增连续诊断为典型FA且小扩增范围与FAexdel患者相同的患者进行比较。
系列病例描述。
学术研究机构。
6例FAexdel患者和46例典型FA患者。
FXN基因分析,包括GAA扩增评估、外显子测序以及使用多重连接依赖探针扩增法测定外显子拷贝数。
我们鉴定出6例FA患者,其表现为1个GAA扩增和1个FXN外显子缺失的组合。FAexdel患者的疾病平均(标准差)发病年龄(7 [4]岁[范围3 - 12岁])早于典型FA患者(15 [5]岁[范围6 - 30岁])(P = 0.001),FAexdel患者使用轮椅的中位时间(20年)短于典型FA患者(28年)(P = 0.002)。FAexdel患者的扩增平均(标准差)大小(780 [256]个GAA三联体重复序列[范围340 - 1070个GAA三联体重复序列])与典型FA患者短扩增的平均(标准差)大小(634 [163]个GAA三联体重复序列[范围367 - 1000个GAA三联体重复序列])之间无差异(P = 0.10)。FAexdel患者在使用轮椅前的平均疾病持续时间(9年)短于典型FA患者(13年),FAexdel患者的心肌病发病率(84%)高于典型FA患者(68%)。然而,这些差异不显著,可能是由于FAexdel组规模较小。其他非神经学体征,如脊柱侧凸或糖尿病,在FAexdel组中尤为常见。1例患者9岁时出现严重心绞痛和明显心肌病,需依赖轮椅。3例患者有严重的自主神经功能障碍。外显子缺失似乎对FA患者的临床表现有显著影响。
外显子缺失突变导致的弗里德赖希共济失调是FA的一种早发且严重的变异型。对于早发FA且仅发现1个无点突变的GAA扩增的患者,应检测FXN基因的外显子缺失情况。必须使用心脏、骨科、内分泌、胃肠和眼科数据对FAexdel患者进行仔细观察。对于出现严重脊柱侧凸的年轻患者,应怀疑为外显子缺失突变导致的弗里德赖希共济失调。
