Temporal Cognitive and Brain Changes in Korsakoff Syndrome.

Neurology

From Normandie Université (A.M., A.L., N.C., C.B., F.E., F.V., S.S., A.-L.P.), UNICAEN, PSL Université Paris, EPHE, INSERM, U1077, CHU de Caen, GIP Cyceron, Neuropsychologie et Imagerie de la Mémoire Humaine; Service d'addictologie (N.C., C.B., F.V.), Centre Hospitalier Universitaire de Caen; Normandie Université (G.C.), UNICAEN, INSERM, U1237, PhIND "Physiopathology and Imaging of Neurological Disorders," Institut Blood and Brain at Caen-Normandie, Cyceron, Caen; Service d'addictologie (L.U.), Centre Hospitalier de Roubaix; and Institut Universitaire de France (A.-L.P.), Paris.

Published: April 2021

AI Article Synopsis

  • The study examined cognitive and brain changes in patients with Korsakoff syndrome (KS) shortly after diagnosis and up to 10 years later, using neuropsychological and imaging methods.
  • No significant cognitive, motor, or brain deterioration was observed over time in KS patients, although there was some modest recovery in specific brain circuit areas.
  • While episodic memory remained severely impaired throughout all evaluations, other aspects such as inhibition abilities showed some preservation, indicating that the structural and metabolic changes in KS are stable and resistant to recovery.

Article Abstract

Objective: To investigate cognitive and brain changes in patients with Korsakoff syndrome (KS) over months and up to 10 years after the diagnosis.

Methods: Two groups of 8 patients with KS underwent neuropsychological, motor, and neuroimaging investigations, including structural MRI and F-fluorodeoxyglucose-PET. The KS group, recruited at Caen University Hospital, was examined early after the KS diagnosis (KS-T1) and 1 year later (KS-T2). The KS group, recruited at nursing home at Roubaix, was evaluated 10 years after the diagnosis. Longitudinal comparisons in KS explored short-term changes, while cross-sectional comparisons between KS-T1 and KS informed about long-term changes.

Results: No cognitive, motor, or brain deterioration occurred over time in patients with KS. There was no clear improvement either, with only modest recovery in the frontocerebellar circuit. Compared to the norms, KS-T1 had severe episodic memory impairments, ataxia, and some executive dysfunctions. They also presented widespread atrophy and hypometabolism as well as cerebellar hypermetabolism compared to 44 healthy matched controls. Episodic memory remained significantly impaired in KS-T2 and KS. Contrary to KS at T1 and T2, KS had preserved inhibition abilities. Atrophy was similar but less extended in KS-T2 and even more limited in KS. At all times, the thalamus, hypothalamus, and fornix remained severely atrophied. Hypometabolism was still widespread in KS-T2 and KS, notably affecting the diencephalon. Cerebellar metabolism decreased over time and normalized in KS, whereas motor dysfunction persisted.

Conclusion: In KS, structural and metabolic alterations of the Papez circuit persisted over time, in accordance with the irreversible nature of amnesia. There was neither significant recovery as observed in patients with alcohol use disorder nor progressive decline as in neurodegenerative diseases.

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http://dx.doi.org/10.1212/WNL.0000000000011749DOI Listing

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