A novel missense mutation in ISCA2 causes aberrant splicing and leads to multiple mitochondrial dysfunctions syndrome 4.

IF 3.2 3区 医学 Q2 PSYCHIATRY Frontiers in Psychiatry Pub Date : 2024-10-18 eCollection Date: 2024-01-01 DOI:10.3389/fpsyt.2024.1428175
Zuhair Al-Hassnan, Mazhor AlDosary, Aljouhra AlHargan, Hanan AlQudairy, Rawan Almass, Khaled Omar Alahmadi, Saif AlShahrani, Albandary AlBakheet, Mohammad A Almuhaizea, Robert W Taylor, Dilek Colak, Namik Kaya
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Abstract

Background: Iron-sulfur cluster assembly 2 (ISCA2) deficiency is linked to an autosomal recessive disorder known as multiple mitochondrial dysfunctions syndrome 4 (MMDS4). This disorder is characterized by leukodystrophy and neuroregression. Currently, most of the reported patients are from Saudi Arabia. All these patients carry a homozygous founder variant (NM_194279.2:c.229G>A:p.Gly77Ser) in ISCA2.

Methods: We describe a patient who underwent full clinical evaluation, including metabolic, neurological, and radiological examinations. Standard genetic testing, including whole exome sequencing coupled with autozygome analysis, was undertaken, as were assessments of mitochondrial DNA (mtDNA) copy number and mtDNA sequencing on DNA extracted from blood and cultured fibroblasts. Functional workup consisted of splicing assessment of ISCA2 using RT-PCR, biochemical assessment of complex I status using dipstick assays, and mitochondrial respiration measurements using a Seahorse XFp analyzer.

Results: We present the clinical and functional characterization of a novel homozygous ISCA2 missense variant (NM_194279.3:c.70A>G:p.Arg24Gly), leading to aberrant splicing in a patient presenting with neuroregression, generalized spasticity with exaggerated deep tendon reflexes and head lag, and progressive loss of acquired milestones. The novel variant was fully segregated in a wider family and was absent in a large control cohort, ethnically matching in-house exomes, local databases such as CGMdb and Saudi Human Genome Program, and ClinVar.

Conclusions: Our analyses revealed that the variant is pathogenic, disrupting normal ISCA2 splicing and presumably leading to a truncated protein that disturbs metabolic pathways in patient-derived cells.

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ISCA2中的一种新型错义突变会导致剪接异常,并引发多线粒体功能障碍综合征4。
背景:铁硫簇组装 2(ISCA2)缺乏症与一种常染色体隐性遗传疾病有关,这种疾病被称为多线粒体功能障碍综合征 4(MMDS4)。这种疾病的特征是白营养不良和神经退化。目前,大多数报告的患者来自沙特阿拉伯。所有这些患者都携带 ISCA2 的同源基因变异(NM_194279.2:c.229G>A:p.Gly77Ser):我们对一名患者进行了全面的临床评估,包括代谢、神经和放射学检查。我们还对线粒体 DNA(mtDNA)拷贝数进行了评估,并对从血液和培养成纤维细胞中提取的 DNA 进行了 mtDNA 测序。功能检查包括使用 RT-PCR 评估 ISCA2 的剪接情况,使用浸量棒测定法对复合体 I 状态进行生化评估,以及使用 Seahorse XFp 分析仪测量线粒体呼吸:我们展示了一个新型同卵ISCA2错义变体(NM_194279.3:c.70A>G:p.Arg24Gly)的临床和功能特征,该变体导致患者出现神经退化、全身痉挛、深腱反射亢进和头部滞后,并逐渐丧失获得性发育里程碑。该新型变异在一个更广泛的家族中完全分离,而在一个大型对照队列、人种匹配的内部外显子组、CGMdb 和沙特人类基因组计划等本地数据库以及 ClinVar 中则不存在:我们的分析表明,该变异体是致病的,它破坏了正常的 ISCA2 剪接,并可能导致产生截短蛋白,从而扰乱患者细胞的代谢途径。
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来源期刊
Frontiers in Psychiatry
Frontiers in Psychiatry Medicine-Psychiatry and Mental Health
CiteScore
6.20
自引率
8.50%
发文量
2813
审稿时长
14 weeks
期刊介绍: Frontiers in Psychiatry publishes rigorously peer-reviewed research across a wide spectrum of translational, basic and clinical research. Field Chief Editor Stefan Borgwardt at the University of Basel is supported by an outstanding Editorial Board of international researchers. This multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. The journal''s mission is to use translational approaches to improve therapeutic options for mental illness and consequently to improve patient treatment outcomes.
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