Abstract
Primary coenzyme Q10 (CoQ10) deficiency encompasses a subset of mitochondrial diseases caused by mutations affecting proteins involved in the CoQ10 biosynthetic pathway. One of the most frequent clinical syndromes associated with primary CoQ10 deficiency is the severe infantile multisystemic form, which, until recently, was underdiagnosed. In the last few years, the availability of genetic screening through whole exome sequencing and whole genome sequencing has enabled molecular diagnosis in a growing number of patients with this syndrome and has revealed new disease phenotypes and molecular defects in CoQ10 biosynthetic pathway genes. Early genetic screening can rapidly and non-invasively diagnose primary CoQ10 deficiencies. Early diagnosis is particularly important in cases of CoQ10 deficient steroid-resistant nephrotic syndrome, which frequently improves with treatment. In contrast, the infantile multisystemic forms of CoQ10 deficiency, particularly when manifesting with encephalopathy, present therapeutic challenges, due to poor responses to CoQ10 supplementation. Administration of CoQ10 biosynthetic intermediate compounds is a promising alternative to CoQ10; however, further pre-clinical studies are needed to establish their safety and efficacy, as well as to elucidate the mechanism of actions of the intermediates. Here, we review the molecular defects causes of the multisystemic infantile phenotype of primary CoQ10 deficiency, genotype-phenotype correlations, and recent therapeutic advances.
Highlights
Coenzyme Q10 (ubiquinone; coenzyme Q10 (CoQ10), EC 206-147-9) is a lipid molecule widely but variably distributed among cellular organelles and tissues
Coenzyme Q10 is a lipid molecule widely but variably distributed among cellular organelles and tissues
We focus on the molecular defects in coenzyme Q10 (CoQ10) biosynthetic genes that cause early-onset multisystemic
Summary
Coenzyme Q10 (ubiquinone; CoQ10, EC 206-147-9) is a lipid molecule widely but variably distributed among cellular organelles and tissues. Mutations in the COQ2 gene have been associated with a wide spectrum of phenotypes [Table 1 and Figure 2], which ranges from a rapidly fatal, neonatal-onset, multisystemic disease[15,23,24,25,26,27,28], to a milder form characterized by SRNS in isolation or associated with encephalopathy[23,28,29].
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