由于LAMA2基因突变引起的肢带肌营养不良:新的突变扩大了临床谱,仍然具有挑战性的诊断。

Q3 Medicine
Francesca Magri, Roberta Brusa, Luca Bello, Lorenzo Peverelli, Roberto Del Bo, Alessandra Govoni, Claudia Cinnante, Irene Colombo, Francesco Fortunato, Roberto Tironi, Stefania Corti, Nadia Grimoldi, Monica Sciacco, Nereo Bresolin, Elena Pegoraro, Maurizio Moggio, Giacomo Pietro Comi
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引用次数: 5

摘要

编码美罗红蛋白的LAMA2基因突变通常是导致严重先天性肌营养不良(CMD型1A)的原因,其特征是严重无力,肌肉分析中美罗红蛋白缺失,脑磁共振成像(MRI)显示白质改变。最近,LAMA2突变被认为是LGMD R23的原因,尽管只有少数病例报道缓慢进展的成人发病和部分美罗红蛋白缺乏症。我们描述了5名独立的意大利受试者,他们表现为进行性肢带肌无力、脑白质异常、美罗红蛋白缺乏和LAMA2基因突变。我们检测到7种不同的突变,其中6种是新的。所有患者均表现出正常的心理运动发育和缓慢进行性无力,发病时间跨度为儿童期至四十岁。肌酸激酶水平中度升高。1例患者表现为扩张型心肌病。肌肉MRI可以评估所有患者肌肉受累的程度和模式。脑MRI是解决和/或支持分子诊断的基础,在t2加权序列中显示典型的广泛的白质高信号。有趣的是,这些改变与3名癫痫和偏头痛患者的中枢神经系统受损伤有关。肌肉活检通常但不一定显示营养不良的特征。免疫印迹法检测梅红素缺乏症通常比免疫化学法更准确。这些病例的描述进一步扩大了lama2相关疾病的临床谱。此外,它支持将LGMD R23纳入LGMD的新分类。中枢神经系统受累是诊断的基础,对于未确诊的LGMD应始终包括在诊断检查中。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Limb girdle muscular dystrophy due to <i>LAMA2</i> gene mutations: new mutations expand the clinical spectrum of a still challenging diagnosis.

Limb girdle muscular dystrophy due to <i>LAMA2</i> gene mutations: new mutations expand the clinical spectrum of a still challenging diagnosis.

Limb girdle muscular dystrophy due to <i>LAMA2</i> gene mutations: new mutations expand the clinical spectrum of a still challenging diagnosis.

Limb girdle muscular dystrophy due to LAMA2 gene mutations: new mutations expand the clinical spectrum of a still challenging diagnosis.

Mutations in LAMA2 gene, encoding merosin, are generally responsible of a severe congenital-onset muscular dystrophy (CMD type 1A) characterized by severe weakness, merosin absence at muscle analysis and white matter alterations at brain Magnetic Resonance Imaging (MRI). Recently, LAMA2 mutations have been acknowledged as responsible of LGMD R23, despite only few cases with slowly progressive adult-onset and partial merosin deficiency have been reported. We describe 5 independent Italian subjects presenting with progressive limb girdle muscular weakness, brain white matter abnormalities, merosin deficiency and LAMA2 gene mutations. We detected 7 different mutations, 6 of which are new. All patients showed normal psicomotor development and slowly progressive weakness with onset spanning from childhood to forties. Creatin-kinase levels were moderately elevated. One patient showed dilated cardiomyopathy. Muscle MRI allowed to evaluate the degree and pattern of muscular involvement in all patients. Brain MRI was fundamental in order to address and/or support the molecular diagnosis, showing typical widespread white matter hyperintensity in T2-weighted sequences. Interestingly these alterations were associated with central nervous system involvement in 3 patients who presented epilepsy and migraine. Muscle biopsy commonly but not necessarily revealed dystrophic features. Western-blot was usually more accurate than immunohystochemical analysis in detecting merosin deficiency. The description of these cases further enlarges the clinical spectrum of LAMA2-related disorders. Moreover, it supports the inclusion of LGMD R23 in the new classification of LGMD. The central nervous system involvement was fundamental to address the diagnosis and should be always included in the diagnostic work-up of undiagnosed LGMD.

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来源期刊
Acta Myologica
Acta Myologica Medicine-Cardiology and Cardiovascular Medicine
CiteScore
3.70
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