Amyotrophic onset in GCH1 dopa-responsive dystonia

S. Habibi, A. Albanese, A. Elia, Paria Arfa-fatollahkhani, N. Hashemi
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引用次数: 1

Abstract

Dopa-responsive dystonia (DRD) belongs to combined dystonia syndrome (dystonia-plus syndrome)1 which encompasses non-degenerative and neurometabolic disorders characterized by combination of dystonia as the prominent sign, with another movement manifestation. Parkinsonism and myoclonus are the main disturbances accompany dystonia in the combined dystonia syndrome. Dystonia with parkinsonism includes DRD [DYT5, tyrosine hydroxylase (TH), and sepiapterin reductase (SPR)], dopamine agonist-responsive dystonia, rapid-onset dystonia parkinsonism (DYT12), and early-onset dystonia with parkinsonism (DYT16). However, dystonia combined with myoclonus is just classified as myoclonus dystonia (DYT11).2 DRD can be inherited in either autosomal dominant or autosomal recessive patterns. The autosomal dominant inheritance results in the typical phenotype of DRD, known as DYT5 or Segawa disease, which is caused by heterozygous mutations of guanosine triphosphate (GTP) cyclohydrolase I gene (GCH1). Mutations of the TH and SPR genes are responsible for autosomal recessive types of DRD.3 DYT5 is represented as progressive lower limbs dystonia with childhood-onset at the common age of 2-5 years. It shows diurnal fluctuations, which are aggravated toward the evening and alleviated by sleeping. Excellent and sustained response to the low dose of levodopa is the marked feature of DYT5 disease. Additional parkinsonism and spasticity may present later in life.4 Moreover, hemiatrophy of the brain, body, or both has been reported in patients with DRD, associated with a biochemical lesion located in basal ganglia.5 However, focal atrophy and muscle weakness rarely accompanies DRD. Interestingly, we aimed to introduce weakness and focal muscle atrophy as the onset manifestations of DRD in an elderly man misdiagnosed for about 70 years.
GCH1多巴反应性肌张力障碍的肌萎缩性发作
多巴反应性肌张力障碍(DRD)属于联合肌张力障碍综合征(肌张力障碍加综合征)1,包括非退行性和神经代谢性疾病,其特征是肌张力障碍作为突出症状,与另一种运动表现相结合。帕金森综合征和肌阵挛是合并肌张力障碍综合征中伴随肌张力障碍的主要障碍。肌张力障碍伴帕金森综合征包括DRD[DYT5、酪氨酸羟化酶(TH)和海泡肽还原酶(SPR)]、多巴胺激动剂反应性肌张力障碍、速发型肌张力障碍性帕金森综合征(DYT12)和早发性肌张力症伴帕金森综合症(DYT16)。然而,肌张力障碍合并肌阵挛仅被归类为肌阵挛肌张力障碍(DYT11)。2 DRD可以常染色体显性或常染色体隐性遗传。常染色体显性遗传导致DRD的典型表型,称为DYT5或Segawa病,由三磷酸鸟苷(GTP)环水解酶I基因(GCH1)的杂合突变引起。TH和SPR基因的突变是常染色体隐性遗传型DRD的原因。3 DYT5表现为进行性下肢肌张力障碍,儿童期常见于2-5岁。它显示出昼夜波动,这种波动在晚上加剧,并通过睡眠缓解。对低剂量左旋多巴的良好和持续反应是DYT5疾病的显著特征。在以后的生活中可能会出现额外的帕金森综合征和痉挛。4此外,据报道,DRD患者大脑、身体或两者都出现半萎缩,与基底神经节的生化损伤有关。5然而,DRD很少伴有局灶性萎缩和肌无力。有趣的是,我们的目的是将虚弱和局灶性肌肉萎缩作为一名被误诊约70年的老年人DRD的发病表现。
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来源期刊
Iranian Journal of Neurology
Iranian Journal of Neurology CLINICAL NEUROLOGY-
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