IRCCS Fondazione Ca' Granda Ospedale Maggiore Policlinico, Neurology Unit, Milan, Italy.
Dino Ferrari Center, Department of Pathophysiology and Transplantation, University of Milan, Milan, Italy.
Skelet Muscle. 2022 Sep 29;12(1):23. doi: 10.1186/s13395-022-00306-8.
Choline kinase beta (CHKB) catalyzes the first step in the de novo biosynthesis of phosphatidyl choline and phosphatidylethanolamine via the Kennedy pathway. Derangement of this pathway might also influence the homeostasis of mitochondrial membranes. Autosomal recessive CHKB mutations cause a rare form of congenital muscular dystrophy known as megaconial congenital muscular dystrophy (MCMD).
We describe a novel proband presenting MCMD due to unpublished CHKB mutations. The patient is a 6-year-old boy who came to our attention for cognitive impairment and slowly progressive muscular weakness. He was the first son of non-consanguineous healthy parents from Sri Lanka. Neurological examination showed proximal weakness at four limbs, weak osteotendinous reflexes, Gowers' maneuver, and waddling gate. Creatine kinase levels were mildly increased. EMG and brain MRI were normal. Left quadriceps skeletal muscle biopsy showed a myopathic pattern with nuclear centralizations and connective tissue increase. Histological and histochemical staining suggested subsarcolemmal localization and dimensional increase of mitochondria. Ultrastructural analysis confirmed the presence of enlarged ("megaconial") mitochondria. Direct sequencing of CHKB identified two novel defects: the c.1060G > C (p.Gly354Arg) substitution and the c.448-56_29del intronic deletion, segregating from father and mother, respectively. Subcloning of RT-PCR amplicons from patient's muscle RNA showed that c.448-56_29del results in the partial retention (14 nucleotides) of intron 3, altering physiological splicing and transcript stability. Biochemical studies showed reduced levels of the mitochondrial fission factor DRP1 and the severe impairment of mitochondrial respiratory chain activity in patient's muscle compared to controls.
This report expands the molecular findings associated with MCMD and confirms the importance of considering CHKB variants in the differential diagnosis of patients presenting with muscular dystrophy and mental retardation. The clinical outcome of MCMD patients seems to be influenced by CHKB molecular defects. Histological and ultrastructural examination of muscle biopsy directed molecular studies and allowed the identification and characterization of an intronic mutation, usually escaping standard molecular testing.
胆碱激酶β(CHKB)通过 Kennedy 途径催化从头合成磷脂酰胆碱和磷脂酰乙醇胺的第一步。该途径的紊乱也可能影响线粒体膜的内稳态。常染色体隐性 CHKB 突变导致一种罕见的先天性肌肉营养不良症,称为巨大先天性肌肉营养不良症(MCMD)。
我们描述了一名因未发表的 CHKB 突变导致 MCMD 的新先证者。该患者是一名 6 岁男孩,因认知障碍和进行性肌无力而引起我们的注意。他是来自斯里兰卡的非近亲健康父母的第一个儿子。神经系统检查显示四肢近端无力、弱腱反射、Gowers 征和鸭步。肌酸激酶水平轻度升高。EMG 和脑 MRI 正常。左股四头肌骨骼肌活检显示肌病模式,有核中央化和结缔组织增加。组织学和组织化学染色提示亚肌膜定位和线粒体尺寸增加。超微结构分析证实存在增大的(“巨大”)线粒体。CHKB 的直接测序发现了两个新缺陷:c.1060G>C(p.Gly354Arg)取代和 c.448-56_29del 内含子缺失,分别从父亲和母亲遗传。来自患者肌肉 RNA 的 RT-PCR 扩增子的亚克隆显示,c.448-56_29del 导致内含子 3 的部分保留(14 个核苷酸),改变了生理剪接和转录稳定性。生化研究表明,与对照组相比,患者肌肉中的分裂因子 DRP1 水平降低,线粒体呼吸链活性严重受损。
本报告扩展了与 MCMD 相关的分子发现,并证实了在表现为肌肉营养不良和智力迟钝的患者的鉴别诊断中考虑 CHKB 变体的重要性。MCMD 患者的临床结局似乎受 CHKB 分子缺陷的影响。肌肉活检的组织学和超微结构检查指导了分子研究,并允许鉴定和表征通常逃避标准分子检测的内含子突变。
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