Transcriptional and functional effects of lithium in bipolar disorder iPSC-derived cortical spheroids

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作者
Jordi Requena Osete
Ibrahim A. Akkouh
Oleksandr Ievglevskyi
Matthieu Vandenberghe
Denis Reis de Assis
Thor Ueland
Elena Kondratskaya
Børge Holen
Attila Szabo
Timothy Hughes
Olav B. Smeland
Vidar Martin Steen
Ole A. Andreassen
Srdjan Djurovic
机构
[1] Oslo University Hospital,Department of Medical Genetics
[2] University of Oslo,NORMENT, Institute of Clinical Medicine
[3] and Division of Mental Health and Addiction,Research Institute of Internal Medicine
[4] Oslo University Hospital,NORMENT, Department of Clinical Science
[5] Oslo University Hospital Rikshospitalet,undefined
[6] University of Bergen,undefined
来源
Molecular Psychiatry | 2023年 / 28卷
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摘要
Lithium (Li) is recommended for long-term treatment of bipolar disorder (BD). However, its mechanism of action is still poorly understood. Induced pluripotent stem cell (iPSC)-derived brain organoids have emerged as a powerful tool for modeling BD-related disease mechanisms. We studied the effects of 1 mM Li treatment for 1 month in iPSC-derived human cortical spheroids (hCS) from 10 healthy controls (CTRL) and 11 BD patients (6 Li-responders, Li-R, and 5 Li non-treated, Li-N). At day 180 of differentiation, BD hCS showed smaller size, reduced proportion of neurons, decreased neuronal excitability and reduced neural network activity compared to CTRL hCS. Li rescued excitability of BD hCS neurons by exerting an opposite effect in the two diagnostic groups, increasing excitability in BD hCS and decreasing it in CTRL hCS. We identified 132 Li-associated differentially expressed genes (DEGs), which were overrepresented in sodium ion homeostasis and kidney-related pathways. Moreover, Li regulated secretion of pro-inflammatory cytokines and increased mitochondrial reserve capacity in BD hCS. Through long-term Li treatment of a human 3D brain model, this study partly elucidates the functional and transcriptional mechanisms underlying the clinical effects of Li, such as rescue of neuronal excitability and neuroprotection. Our results also underscore the substantial influence of treatment duration in Li studies. Lastly, this study illustrates the potential of patient iPSC-derived 3D brain models for precision medicine in psychiatry.
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页码:3033 / 3043
页数:10
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