Targeting mitochondrial dynamics of morphine-responsive dopaminergic neurons ameliorates opiate withdrawal
Changyou Jiang, … , Lan Ma, Feifei Wang
Changyou Jiang, … , Lan Ma, Feifei Wang
Published January 18, 2024
Citation Information: J Clin Invest. 2024;134(5):e171995. https://doi.org/10.1172/JCI171995.
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Research Article Neuroscience

Targeting mitochondrial dynamics of morphine-responsive dopaminergic neurons ameliorates opiate withdrawal

Abstract

Converging studies demonstrate the dysfunction of the dopaminergic neurons following chronic opioid administration. However, the therapeutic strategies targeting opioid-responsive dopaminergic ensembles that contribute to the development of opioid withdrawal remain to be elucidated. Here, we used the neuronal activity-dependent Tet-Off system to label dopaminergic ensembles in response to initial morphine exposure (Mor-Ens) in the ventral tegmental area (VTA). Fiber optic photometry recording and transcriptome analysis revealed downregulated spontaneous activity and dysregulated mitochondrial respiratory, ultrastructure, and oxidoreductase signal pathways after chronic morphine administration in these dopaminergic ensembles. Mitochondrial fragmentation and the decreased mitochondrial fusion gene mitofusin 1 (Mfn1) were found in these ensembles after prolonged opioid withdrawal. Restoration of Mfn1 in the dopaminergic Mor-Ens attenuated excessive oxidative stress and the development of opioid withdrawal. Administration of Mdivi-1, a mitochondrial fission inhibitor, ameliorated the mitochondrial fragmentation and maladaptation of the neuronal plasticity in these Mor-Ens, accompanied by attenuated development of opioid withdrawal after chronic morphine administration, without affecting the analgesic effect of morphine. These findings highlighted the plastic architecture of mitochondria as a potential therapeutic target for opioid analgesic-induced substance use disorders.

Authors

Changyou Jiang, Han Huang, Xiao Yang, Qiumin Le, Xing Liu, Lan Ma, Feifei Wang

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Figure 10

Mdivi-1 alleviates withdrawal symptoms and negative affects after chronic morphine administration in both male and female mice.

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Mdivi-1 alleviates withdrawal symptoms and negative affects after chroni...
(A) Experimental scheme to measure the naloxone-precipitated withdrawal symptoms in both male and female mice. (BF) The effects of Mdivi-1 on weight loss (B), diarrhea (C), wet dog shakes (D), body tremor (E), and backward locomotion (F) were analyzed in mice from vehicle and Mdivi-1 groups. Male, 10-12 mice per group; female, 15 mice per group. Unpaired t test or Mann-Whitney test. (GO) The effect of Mdivi-1 on negative affects during spontaneous and chronic morphine withdrawal in both male and female mice. (G) Experimental scheme of the behavioral tests. Immobility time (H and I), morphine withdrawal-induced CPA (J and M), time in the open arm (K and N), and social preference (L and O) were analyzed in vehicle and Mdivi-1 pretreated groups. Male, 11–12 mice per group; female, 14–15 mice per group. Unpaired t test or Mann-Whitney test for 2 groups, 2-way RM ANOVA with Bonferroni’s test in CPA. Data are presented as mean ± SEM; *P < 0.05, **P < 0.01, ***P < 0.001, ****P < 0.0001.