Savarese Marco, Vihola Anna, Jokela Manu E, Huovinen Sanna Pauliina, Gerevini Simonetta, Torella Annalaura, Johari Mridul, Scarlato Marina, Jonson Per Harald, Onore Maria Elena, Hackman Peter, Gautel Mathias, Nigro Vincenzo, Previtali Stefano Carlo, Udd Bjarne
Folkhälsan Research Center (M. Savarese, A.V., M.J., P.H.J., P.H., B.U.), Helsinki; Department of Medical Genetics (M. Savarese, A.V., M.J., P.H.J., P.H., B.U.), Medicum, University of Helsinki; Neuromuscular Research Center (A.V.), Department of Genetics, Fimlab Laboratories, Tampere; Division of Clinical Neurosciences (M.E.J.), Department of Neurology, Turku University and University Hospital; Neuromuscular Research Center (S.P.H.), Department of Pathology, Fimlab Laboratories, Tampere, Finland; Neuroradiology Unit (S.G.), ASST Papa Giovanni XXIII, Bergamo; Dipartimento di Medicina di Precisione (A.T., M.E.O., V.N.), Università degli Studi della Campania "Luigi Vanvitelli," Napoli; Telethon Institute of Genetics and Medicine (A.T., V.N.), Pozzuoli; Division of Neuroscience and U.O. Neurologia (M. Scarlato, S.C.P.), IRCCS Ospedale San Raffaele, Milano, Italy; Randall Centre for Cell and Molecular Biophysics (M.G.), King's College London BHF Centre of Research Excellence, United Kingdom; Department of Neurology (B.U.), Vaasa Central Hospital; and Neuromuscular Research Center (M.E.J., B.U.), Department of Neurology, Tampere University and University Hospital, Finland.
Neurol Genet. 2021 Aug 10;7(5):e619. doi: 10.1212/NXG.0000000000000619. eCollection 2021 Oct.
To clinically, genetically, and histopathologically characterize patients presenting with an unusual combination of distal myopathy and facial weakness, without involvement of upper limb or shoulder girdle muscles.
Two families with a novel form of actininopathy were identified. Patients had been followed up over 10 years. Their molecular genetic diagnosis was not clear after extensive investigations, including analysis of candidate genes and FSHD1-related D4Z4 repeats.
Patients shared a similar clinical phenotype and a common pattern of muscle involvement. They presented with a very slowly progressive myopathy involving anterior lower leg and facial muscles. Muscle MRI finding showed complete fat replacement of anterolateral compartment muscles of the lower legs with variable involvement of soleus and gastrocnemius but sparing thigh muscles. Muscle biopsy showed internalized nuclei, myofibrillar disorganization, and rimmed vacuoles. High-throughput sequencing identified in each proband a heterozygous single nucleotide deletion (c.2558del and c.2567del) in the last exon of the gene. The deletions are predicted to lead to a novel but unstructured slightly extended C-terminal amino acid sequence.
Our findings indicate an unusual form of actininopathy with specific molecular and clinical features. Actininopathy should be considered in the differential diagnosis of distal myopathy combined with facial weakness.
对表现为远端肌病与面部肌无力异常组合且不累及上肢或肩胛带肌肉的患者进行临床、遗传学及组织病理学特征分析。
识别出两个患有新型辅肌动蛋白病的家系。对患者进行了超过10年的随访。经过包括候选基因分析及与FSHD1相关的D4Z4重复序列分析在内的广泛研究后,其分子遗传学诊断仍不明确。
患者具有相似的临床表型及共同的肌肉受累模式。他们表现为累及小腿前侧和面部肌肉的进展非常缓慢的肌病。肌肉MRI检查结果显示小腿前外侧肌间隙肌肉完全被脂肪替代,比目鱼肌和腓肠肌受累情况不一,但大腿肌肉未受累。肌肉活检显示有核内移、肌原纤维紊乱及镶边空泡。高通量测序在每个先证者的该基因最后一个外显子中鉴定出一个杂合单核苷酸缺失(c.2558del和c.2567del)。这些缺失预计会导致一种新的但无结构的略延长的C末端氨基酸序列。
我们的研究结果表明存在一种具有特定分子和临床特征的不寻常形式的辅肌动蛋白病。在鉴别诊断远端肌病合并面部肌无力时应考虑辅肌动蛋白病。
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