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Expanding the phenotype of mitochondrial disease: Novel pathogenic variant in ISCA1 leading to instability of the iron-sulfur cluster in the protein

Mitochondrion. 2020; 
E Lebigot, M Hully, L Amazit, P Gaignard, T Michel, M Rio, M Lombès, P Thérond, A Boutron, M P Golinelli-Cohen
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Bacterial Expression … MD). 2.6. Expression and purification of mature ISCA1. The mature form of human ISCA1 (NCBI Q9BUE6, residues 24–129) and the p.Tyr101Cys mutated form were expressed in E. coli using the pET28a vector (GenScript) … Get A Quote

摘要

We report a patient carrying a novel pathogenic variant p.(Tyr101Cys) in ISCA1 leading to MMDS type 5. He initially presented a psychomotor regression with loss of gait and language skills and a tetrapyramidal spastic syndrome. Biochemical analysis of patient fibroblasts revealed impaired lipoic acid synthesis and decreased activities of complex I and II of respiratory chain. While ISCA1 is involved in the mitochondrial machinery for iron-sulfur cluster biogenesis, these dysfunctions are secondary to impaired maturation of mitochondrial proteins containing the [4Fe-4S] clusters. Expression and purification of the human ISCA1 showed a decreased stability of the [2Fe-2S] cluster in the mutated protein.

关键词

ISCA1, Iron-sulfur cluster, Lipoic acid, MMDS, PDH