Wernicke–Korsakoff syndrome associated with mtDNA disease

Introduction: Wernicke encephalopathy (WE) and Wernicke–Korsakoff syndrome (WKS) are well-known disorders caused by thiamine deficiency. In addition to the classical concept of these diseases, some literature data suggest a connection between mitochondrial dysfunction and WE/WKS. Psychotic disorders...

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Bibliographic Details
Published inTherapeutic advances in neurological disorders Vol. 13; p. 1756286420938972
Main Authors Jimoh, Idris Janos, Sebe, Barbara, Balicza, Peter, Fedor, Mariann, Pataky, Ilona, Rudas, Gabor, Gal, Aniko, Inczedy-Farkas, Gabriella, Nemeth, Gyorgy, Molnar, Maria Judit
Format Journal Article
LanguageEnglish
Published London, England SAGE Publications 2020
SAGE PUBLICATIONS, INC
SAGE Publishing
Subjects
Acidosis
Amnesia
Antioxidants
Antipsychotics
Ataxia
Cognitive ability
Dopamine D3 receptors
Emotional behavior
Gait
Genetic screening
Lactic acidosis
Magnetic resonance imaging
Medical treatment
Memory
Mental disorders
Mitochondria
Mitochondrial DNA
Mutation
Neuroimaging
Oxidative phosphorylation
Patients
Phosphorylation
Psychosis
Schizophrenia
Therapeutic s in Neurology
Vomiting
Wernicke's encephalopathy
ataxia
Wernicke Encephalopathy
OXPHOS
MELAS
schizophrenia
cariprazine
encephalopathy
memory impairment
mitochondrial disease
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Summary:Introduction: Wernicke encephalopathy (WE) and Wernicke–Korsakoff syndrome (WKS) are well-known disorders caused by thiamine deficiency. In addition to the classical concept of these diseases, some literature data suggest a connection between mitochondrial dysfunction and WE/WKS. Psychotic disorders and WKS seem to run in families, as the deficiency of the oxidative phosphorylation can be a trigger factor in psychotic events and WE/WKS as well. We present a patient harbouring the m.A3243G mtDNA mutation with the clinical and magnetic resonance imaging (MRI) findings of WKS who developed schizophrenia with predominantly negative symptoms some years later. Case presentation: A 27-year-old woman was referred to our clinic with severe weight loss after severe vomiting episodes, memory dysfunction and gait ataxia. Family history, as well as clinical, imaging and laboratory findings suggested a mitochondrial aetiology of her symptoms. Brain MRI detected bilateral mild thalamic lesions and loss of corpus mammillae, indicating Wernicke encephalopathy. Genetic testing detected an m.A3243G mtDNA mutation, which has been frequently associated with mitochondrial encephalopathy with lactic acidosis and stroke-like episodes. High-dose vitamin B1 supplementation with supportive antioxidant therapy improved the patient’s memory and learning disturbance; however, some months later she developed psychosis with predominantly negative symptoms and her cognitive functions deteriorated again. Both cognitive and negative symptoms responded well to cariprazine monotherapy. Discussion: Mitochondrial disease due to mtDNA alteration can be a rare cause of WE. In addition to vitamin B1 supplementation, cariprazine with significant dopamine D3 receptor binding can be useful to treat the predominantly negative symptoms and cognitive dysfunction in patients with mitochondrial dysfunction. Conclusion: We assume that patients with a mitochondrial disorder might be prone to develop WE/WKS and therefore need tailored supportive therapy during metabolic crisis as well as symptom-based personalized antipsychotic treatment.
ISSN:1756-2864
1756-2856
1756-2864
DOI:10.1177/1756286420938972