Mood variations decoded from multi-site intracranial human brain activity

Mood state changes are decoded using human neural activity data from electrodes implanted in seven epilepsy patients. The ability to decode mood state over time from neural activity could enable closed-loop systems to treat neuropsychiatric disorders. However, this decoding has not been demonstrated...

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Bibliographic Details
Published inNature biotechnology Vol. 36; no. 10; pp. 954 - 961
Main Authors Sani, Omid G, Yang, Yuxiao, Lee, Morgan B, Dawes, Heather E, Chang, Edward F, Shanechi, Maryam M
Format Journal Article
LanguageEnglish
Published New York Springer New York 01.11.2018
Nature Publishing Group
Subjects
631/378/116/2394
631/378/1457
631/61
639/166/985
9/30
Agriculture
Analysis
Bioinformatics
Biomedical Engineering/Biotechnology
Biomedicine
Biotechnology
Brain
Closed loops
Decoders
Decoding
Drug therapy
Dynamic models
Emotional disorders
Epilepsy
Feedback control
Human performance
Human subjects
Life Sciences
Medical imaging
Mental disorders
Modelling
Mood
Mood disorders
Nervous system diseases
Neural coding
Neuroimaging
Neurophysiology
Sparsity
Variation
United States
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Summary:Mood state changes are decoded using human neural activity data from electrodes implanted in seven epilepsy patients. The ability to decode mood state over time from neural activity could enable closed-loop systems to treat neuropsychiatric disorders. However, this decoding has not been demonstrated, partly owing to the difficulty of modeling distributed mood-relevant neural dynamics while dealing with the sparsity of mood state measurements. Here we develop a modeling framework to decode mood state variations from multi-site intracranial recordings in seven human subjects with epilepsy who self-reported their mood state intermittently over multiple days. We built dynamic neural encoding models of mood state and corresponding decoders for each individual and demonstrated that mood state variations over time can be decoded from neural activity. Across subjects, the decoders largely recruited neural signals from limbic regions, whose spectro-spatial features were tuned to mood variations. The dynamic models also provided an analytical tool to compute the timescales of the decoded mood state. These results provide an initial line of evidence indicating the feasibility of mood state decoding.
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ISSN:1087-0156
1546-1696
1546-1696
DOI:10.1038/nbt.4200