With interest, we read the article by Montano et al. about a 42-year-old Italian female with ptosis, ophthalmoparesis, dysphagia, exercise intolerance, and myalgias [1]. The phenotype was attributed to the compound heterozygous mutations c.462T>A and c.707 + 2T>G in the DGUOK gene secondarily causing multiple mtDNA deletions [1]. We have the following comments and concerns.
Since the patient had anxiety disorder, it would be interesting to know if there were any other cerebral abnormalities clinically or on cerebral MRI. Cerebral imaging is crucial as the central nervous system (CNS) in DGUOK-related mitochondrial disorders (MIDs) is frequently affected and may even dominate the phenotype. Cerebral MRI may show abnormal myelination infratentorially and bilateral hyperintensity of the pallidi [2].
Dysphagia may have been due to affection of the smooth muscle cells, autonomic innervation, or due to affection of the brain. Cerebral MRI could be helpful to confirm or exclude a CNS cause of dysphagia. Autonomic testing could be helpful to investigate if there was autonomic compromise.
Though a muscle biopsy was taken, biochemical investigation of the muscle homogenate and detailed descriptions of immunostaining were not provided. Thus, it would be interesting to know which of the respiratory complexes showed reduced activity.
Since DGUOK mutations may also cause mtDNA depletion [3], it is worthwhile to investigate if the amount of mtDNA in a patient carrying a DGUOK mutation is normal or if there is mtDNA depletion. Patients with mtDNA depletion due to DGUOK mutations may have a worse prognosis than those without mtDNA depletion [4].
DGUOK mutations may not only manifest in the skeletal muscle (ptosis, CPEO, generalised myopathy, and rhabdomyolysis) and the brain (psychomotor retardation, cognitive impairment, nystagmus, Parkinsonism, and generalised hypotonia) but also in a number of other organs/tissues, such as the eyes (retinal blindness and cataract), the ears (sensorineural deafness), the liver (coagulation disorder, hypoglycemia, hemochromatosis, cholestasis, hepatomegaly, hepatocellular carcinoma, hepatopathy, portal hypertension, idiopathic hepatitis, liver failure, steatosis, and iron deposits) [5], the intestines, and the kidneys (renal failure). There may be lactic acidosis, elevated ferritin, elevated transferrin saturation, and elevated serum amino acids [6]. Thus, it is worthwhile that patients carrying DGUOK variants are prospectively investigated for clinical or subclinical manifestations described above.
To assess if a DGUOK mutation occurred sporadically or was inherited, it could be helpful that the parents and other first-degree relatives undergo a clinical neurological exam and genetic investigations.
Overall, this interesting case report could be more meaningful if biochemical investigations of the muscle or liver were presented, if cerebral MRI results were shown, if first degree relatives were investigated clinically and for the DGUOK variants, and if the patient was prospectively investigated for subclinical or mildly manifesting multisystem disease.
Conflicts of Interest
The authors declare that there are no conflicts of interest.
References
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