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由HIBCH和ECHS1缺乏引起的缬氨酸代谢疾病中的运动障碍。

Movement disorders in valine métabolism diseases caused by HIBCH and ECHS1 deficiencies.

作者信息

François-Heude Marie-Céline, Lebigot Elise, Roze Emmanuel, Warde Marie Thérèse Abi, Cances Claude, Damaj Lena, Espil Caroline, Fluss Joel, de Lonlay Pascale, Kern Ilse, Lenaers Guy, Munnich Arnold, Meyer Pierre, Spitz Marie-Aude, Torre Stéphanie, Doummar Diane, Touati Guy, Leboucq Nicolas, Roubertie Agathe

机构信息

CHU Montpellier, Département de Neuropédiatrie, Univ Montpellier, Montpellier, France.

Biochemistry Department, APHP Paris Saclay, Bicêtre Hospital, Paris, France.

出版信息

Eur J Neurol. 2022 Nov;29(11):3229-3242. doi: 10.1111/ene.15515. Epub 2022 Aug 9.

DOI:10.1111/ene.15515
PMID:36200804
Abstract

BACKGROUND AND PURPOSE

HIBCH and ECHS1 genes encode two enzymes implicated in the critical steps of valine catabolism, 3-hydroxyisobutyryl-coenzyme A (CoA) hydrolase (HIBCH) and short-chainenoyl-CoA hydratase (ECHS1), respectively. HIBCH deficiency (HIBCHD) and ECHS1 deficiency (ECHS1D) generate rare metabolic dysfunctions, often revealed by neurological symptoms. The aim of this study was to describe movement disorders spectrum in patients with pathogenic variants in ECHS1 and HIBC.

METHODS

We reviewed a series of 18 patients (HIBCHD: 5; ECHS1D: 13) as well as 105 patients from the literature. We analysed the detailed phenotype of HIBCHD (38 patients) and ECHS1D (85 patients), focusing on MDs.

RESULTS

The two diseases have a very similar neurological phenotype, with an early onset before 10 years of age for three clinical presentations: neonatal onset, Leigh-like syndrome (progressive onset or acute neurological decompensation), and isolated paroxysmal dyskinesia. Permanent or paroxysmal MDs were recorded in 61% of HIBCHD patients and 72% of ECHS1D patients. Patients had a variable combination of either isolated or combined MD, and dystonia was the main MD. These continuous MDs included dystonia, chorea, parkinsonism, athetosis, myoclonus, tremors, and abnormal eye movements. Patients with paroxysmal dyskinesia (HIBCHD: 4; ECHS1D: 9) usually had pure paroxysmal dystonia with normal clinical examination and no major impairment in psychomotor development. No correlation could be identified between clinical pattern (especially MD) and genetic pathogenic variants.

CONCLUSIONS

Movement disorders, including abnormal ocular movements, are a hallmark of HIBCHD and ECHS1D. MDs are not uniform; dystonia is the most frequent, and various types of MD are combined in single patient.

摘要

背景与目的

HIBCH和ECHS1基因分别编码参与缬氨酸分解代谢关键步骤的两种酶,即3-羟基异丁酰辅酶A(CoA)水解酶(HIBCH)和短链烯酰CoA水合酶(ECHS1)。HIBCH缺乏症(HIBCHD)和ECHS1缺乏症(ECHS1D)会引发罕见的代谢功能障碍,常表现为神经症状。本研究的目的是描述ECHS1和HIBC基因致病性变异患者的运动障碍谱。

方法

我们回顾了一系列18例患者(HIBCHD:5例;ECHS1D:13例)以及文献中的105例患者。我们分析了HIBCHD(38例患者)和ECHS1D(85例患者)的详细表型,重点关注运动障碍。

结果

这两种疾病具有非常相似的神经表型,在10岁之前有三种临床表现的早期发病:新生儿期发病、类 Leigh 综合征(进行性发病或急性神经功能失代偿)和孤立性阵发性运动障碍。61%的HIBCHD患者和72%的ECHS1D患者记录有永久性或阵发性运动障碍。患者有孤立性或合并性运动障碍的不同组合,且肌张力障碍是主要的运动障碍。这些持续性运动障碍包括肌张力障碍、舞蹈症、帕金森症、手足徐动症、肌阵挛、震颤和异常眼动。阵发性运动障碍患者(HIBCHD:4例;ECHS1D:9例)通常有单纯性阵发性肌张力障碍,临床检查正常且精神运动发育无重大损害。临床模式(尤其是运动障碍)与基因致病性变异之间未发现相关性。

结论

运动障碍,包括异常眼动,是HIBCHD和ECHS1D的一个标志。运动障碍并不一致;肌张力障碍最为常见,且单一患者中可合并多种类型的运动障碍。

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