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Clinical signs and symptoms in a large hereditary spastic paraparesis pedigree with a novel spastin mutation.

机译:大的遗传性痉挛性轻瘫的家系中的临床体征和症状,伴有新的spastin突变。

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摘要

The most common form of autosomal dominant hereditary spastic paraparesis (HSP), SPG4, is caused by mutations in the spastin gene on chromosome 2p. This disease is characterized by intra- and interfamilial phenotypic variation. To determine the predictive values of clinical signs and symptoms in SPG4, we examined 43 members of a large pedigree with autosomal dominant HSP. We then identified the genetic etiology of the disorder in this family, a novel nonsense mutation in exon 1 of spastin, carried by 24 of the examined family members. The best clinical predictors of positive gene status were the presence of hyperreflexia in the lower extremities, >2 beats of ankle clonus, pes cavus, bladder symptoms and increased tone in the legs. The mean age of onset was 32.2 +/- 7.4 years, but the age of onset was earlier in children from 10 of 12 child-parent gene-positive pairs, with a mean difference of 10.8 +/- 3.3 years. The finding of leg weakness was especially common in older-onset affected family member with leg hyperreflexia. These results suggest that specific clinical signs and symptoms may be of value in differentiating individuals affected with SPG4 from family members with nonspecific neurological findings.
机译:常染色体显性遗传性遗传性痉挛性轻瘫(HSP)的最常见形式,是由2p号染色体上的spastin基因突变引起的。该疾病的特征是家族内和家族间表型变异。为了确定SPG4中临床体征和症状的预测价值,我们检查了具有常染色体显性HSP的大血统的43名成员。然后,我们确定了该家族中该疾病的遗传病因,这是由24个受检家族成员携带的spastin外显子1中的一个新的无意义突变。阳性基因状态的最佳临床预测指标是下肢存在反射亢进,踝关节阵挛跳动> 2次,盲肠,膀胱症状和腿部音调增加。平均发病年龄为32.2 +/- 7.4岁,但是来自12对儿童-父母基因阳性对中的10对儿童的发病年龄更早,平均差异为10.8 +/- 3.3岁。腿部无力的发现在患有腿部反射亢进的较老发病的家庭成员中尤为常见。这些结果表明,特定的临床体征和症状可能在区分受SPG4影响的个体和具有非特定神经学发现的家庭成员方面具有价值。

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