Variants in DTNA cause a mild, dominantly inherited muscular dystrophy

IF 9.3 1区医学 Q1 CLINICAL NEUROLOGY

Acta Neuropathologica Pub Date : 2023-02-17 DOI:10.1007/s00401-023-02551-7

Andres Nascimento, Christine C. Bruels, Sandra Donkervoort, A. Reghan Foley, Anna Codina, Jose C. Milisenda, Elicia A. Estrella, Chengcheng Li, Jordi Pijuan, Isabelle Draper, Ying Hu, Seth A. Stafki, Lynn S. Pais, Vijay S. Ganesh, Anne O’Donnell-Luria, Safoora B. Syeda, Laura Carrera-García, Jessica Expósito-Escudero, Delia Yubero, Loreto Martorell, Iago Pinal-Fernandez, Hart G. W. Lidov, Andrew L. Mammen, Josep M. Grau-Junyent, Carlos Ortez, Francesc Palau, Partha S. Ghosh, Basil T. Darras, Cristina Jou, Louis M. Kunkel, Janet Hoenicka, Carsten G. Bönnemann, Peter B. Kang, Daniel Natera-de Benito

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Abstract

DTNA encodes α-dystrobrevin, a component of the macromolecular dystrophin–glycoprotein complex (DGC) that binds to dystrophin/utrophin and α-syntrophin. Mice lacking α-dystrobrevin have a muscular dystrophy phenotype, but variants in DTNA have not previously been associated with human skeletal muscle disease. We present 12 individuals from four unrelated families with two different monoallelic DTNA variants affecting the coiled-coil domain of α-dystrobrevin. The five affected individuals from family A harbor a c.1585G > A; p.Glu529Lys variant, while the recurrent c.1567_1587del; p.Gln523_Glu529del DTNA variant was identified in the other three families (family B: four affected individuals, family C: one affected individual, and family D: two affected individuals). Myalgia and exercise intolerance, with variable ages of onset, were reported in 10 of 12 affected individuals. Proximal lower limb weakness with onset in the first decade of life was noted in three individuals. Persistent elevations of serum creatine kinase (CK) levels were detected in 11 of 12 affected individuals, 1 of whom had an episode of rhabdomyolysis at 20 years of age. Autism spectrum disorder or learning disabilities were reported in four individuals with the c.1567_1587 deletion. Muscle biopsies in eight affected individuals showed mixed myopathic and dystrophic findings, characterized by fiber size variability, internalized nuclei, and slightly increased extracellular connective tissue and inflammation. Immunofluorescence analysis of biopsies from five affected individuals showed reduced α-dystrobrevin immunoreactivity and variably reduced immunoreactivity of other DGC proteins: dystrophin, α, β, δ and γ-sarcoglycans, and α and β-dystroglycans. The DTNA deletion disrupted an interaction between α-dystrobrevin and syntrophin. Specific variants in the coiled-coil domain of DTNA cause skeletal muscle disease with variable penetrance. Affected individuals show a spectrum of clinical manifestations, with severity ranging from hyperCKemia, myalgias, and exercise intolerance to childhood-onset proximal muscle weakness. Our findings expand the molecular etiologies of both muscular dystrophy and paucisymptomatic hyperCKemia, to now include monoallelic DTNA variants as a novel cause of skeletal muscle disease in humans.

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DTNA变异导致轻度显性遗传性肌营养不良

DTNA编码α-肌营养不良短肽，这是大分子肌营养不良蛋白-糖蛋白复合物（DGC）的一种成分，与肌营养不良/肌营养不良和α-合成营养不良结合。缺乏α-肌短肽的小鼠具有肌营养不良表型，但DTNA的变体以前与人类骨骼肌疾病无关。我们报道了来自四个不相关家族的12个人，他们有两个不同的单等位基因DTNA变体，影响α-肌短肽的卷曲螺旋结构域。来自A家庭的五名受影响者携带约1585G >； A.p.Glu529Lys变体，而复发的c.1567_1587del；p.Gln523_Glu529del DTNA变体在其他三个家族（家族B：四个受影响的个体，家族C：一个受影响个体，家族D：两个受影响个人）中被鉴定。据报道，12名患者中有10人出现肌痛和运动不耐受，发病年龄各不相同。三名患者在生命的第一个十年出现近端下肢无力。12名患者中有11人血清肌酸激酶（CK）水平持续升高，其中1人在20岁时出现横纹肌溶解症。据报道，有四名c.1567_1587缺失的个体患有自闭症谱系障碍或学习障碍。8名受影响个体的肌肉活检显示出肌病和营养不良的混合表现，其特征是纤维大小变异、细胞核内化以及细胞外结缔组织和炎症轻微增加。对五名受影响个体的活检组织进行免疫荧光分析，结果显示α-肌萎缩蛋白免疫反应性降低，其他DGC蛋白的免疫反应性也不同程度地降低：肌萎缩蛋白、α、β、δ和γ-肌聚糖以及α和β-肌萎缩聚糖。DTNA缺失破坏了α-肌营养不良蛋白和合成营养因子之间的相互作用。DTNA卷曲螺旋结构域中的特定变体导致外显率可变的骨骼肌疾病。受影响的个体表现出一系列临床表现，严重程度从高肌酸激酶血症、肌痛、运动不耐受到儿童期发作的近端肌无力。我们的研究结果扩展了肌营养不良和少症状性高肌酸激酶血症的分子病因，现在将单等位基因DTNA变体作为人类骨骼肌疾病的新病因。

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来源期刊

Acta Neuropathologica 医学-病理学

CiteScore

23.70

自引率

3.90%

发文量

118

审稿时长

4-8 weeks

期刊介绍： Acta Neuropathologica publishes top-quality papers on the pathology of neurological diseases and experimental studies on molecular and cellular mechanisms using in vitro and in vivo models, ideally validated by analysis of human tissues. The journal accepts Original Papers, Review Articles, Case Reports, and Scientific Correspondence (Letters). Manuscripts must adhere to ethical standards, including review by appropriate ethics committees for human studies and compliance with principles of laboratory animal care for animal experiments. Failure to comply may result in rejection of the manuscript, and authors are responsible for ensuring accuracy and adherence to these requirements.