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

被引:0
作者
Al-Hassnan, Zuhair [1 ,2 ]
Aldosary, Mazhor [3 ]
Alhargan, Aljouhra [3 ]
Alqudairy, Hanan [3 ]
Almass, Rawan [1 ]
Alahmadi, Khaled Omar [4 ]
AlShahrani, Saif [1 ]
Albakheet, Albandary [3 ]
Almuhaizea, Mohammad A. [2 ,5 ]
Taylor, Robert W. [6 ,7 ]
Colak, Dilek [8 ]
Kaya, Namik [2 ,3 ]
机构
[1] King Faisal Specialist Hosp & Res Ctr, Ctr Genom Med, Dept Med Genom, Riyadh, Saudi Arabia
[2] Alfaisal Univ, Coll Med, Riyadh, Saudi Arabia
[3] King Faisal Specialist Hosp & Res Ctr, Ctr Genom Med, Translat Genom Dept, Riyadh, Saudi Arabia
[4] King Faisal Specialist Hosp & Res Ctr, Dept Radiol, Riyadh, Saudi Arabia
[5] King Faisal Specialist Hosp & Res Ctr, Neurosci Ctr, Riyadh, Saudi Arabia
[6] Newcastle Univ, Translat & Clin Res Inst, Fac Med Sci, Mitochondrial Res Grp, Newcastle Upon Tyne, England
[7] Newcastle Upon Tyne Hosp Natl Hlth Serv NHS Fdn Tr, Natl Hlth Serv NHS Highly Specialised Mitochondria, Newcastle Upon Tyne, England
[8] King Faisal Specialist Hosp & Res Ctr, Mol Oncol Dept, Riyadh, Saudi Arabia
来源
FRONTIERS IN PSYCHIATRY | 2024年 / 15卷
关键词
ISCA2 founder variant; novel splicing variant; mtDNA; depletion; leukodystrophy; neuroregression; SULFUR-PROTEIN BIOGENESIS; IRON; CLUSTER; FIBROBLASTS; MATURATION; MACHINERY;
D O I
10.3389/fpsyt.2024.1428175
中图分类号
R749 [精神病学];
学科分类号
100205 ;
摘要
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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页数:10
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