Restoration of Miro1's N-terminal GTPase function alleviates prenatal stress-induced mitochondrial fission via Drp1 modulation

Gee Euhn Choi; Ji Yong Park; Mo Ran Park; Chang Woo Chae; Young Hyun Jung; Jae Ryong Lim; Jee Hyeon Yoon; Ji Hyeon Cho; Ho Jae Han

doi:10.1186/s12964-025-02172-5

Restoration of Miro1's N-terminal GTPase function alleviates prenatal stress-induced mitochondrial fission via Drp1 modulation

Cell Commun Signal. 2025 Apr 2;23(1):166. doi: 10.1186/s12964-025-02172-5.

Authors

Gee Euhn Choi^#^{1

2}, Ji Yong Park^#³, Mo Ran Park^#³, Chang Woo Chae⁴, Young Hyun Jung⁵, Jae Ryong Lim³, Jee Hyeon Yoon³, Ji Hyeon Cho³, Ho Jae Han⁶

Affiliations

¹ Laboratory of Veterinary Biochemistry, College of Veterinary Medicine and Veterinary Medical Research Institute, Jeju National University, Jeju, 63243, South Korea.
² Interdisciplinary Graduate Program in Advanced Convergence Technology & Science, Jeju National University, Jeju, 63243, South Korea.
³ Department of Veterinary Physiology, College of Veterinary Medicine, Research Institute for Veterinary Science, BK21 FOUR Future Veterinary Medicine Leading Education & Research Center, Seoul National University, Seoul, 08826, South Korea.
⁴ Department of Physiology and Medical Science, College of Medicine and Brain Research Institute, Chungnam National University, Daejeon, 35015, South Korea.
⁵ Department of Physiology, College of Medicine, Soonchunhyang University, Cheonan, 31151, Republic of Korea.
⁶ Department of Veterinary Physiology, College of Veterinary Medicine, Research Institute for Veterinary Science, BK21 FOUR Future Veterinary Medicine Leading Education & Research Center, Seoul National University, Seoul, 08826, South Korea. hjhan@snu.ac.kr.

^# Contributed equally.

Abstract

Background: Prenatal stress exposure irreversibly impairs mitochondrial dynamics, including mitochondrial trafficking and morphology in offspring, leading to neurodevelopmental and neuropsychiatric disorders in adulthood. Thus, understanding the molecular mechanism controlling mitochondrial dynamics in differentiating neurons is crucial to prevent the prenatal stress-induced impairments in behavior. We investigated the interplay between mitochondrial transport and fusion/fission in differentiating neurons exposed to prenatal stress, leading to ensuing behavior impairments, and then tried to identify the primary regulator that modulates both phenomena.

Methods: We used primary hippocampal neurons of mice exposed to prenatal stress and human induced-pluripotent stem cell (hiPSC)-derived neurons, for investigating the impact of glucocorticoid on mitochondrial dynamics during differentiation. For constructing mouse models, we used AAV vectors into mouse pups exposed to prenatal stress to regulate protein expressions in hippocampal regions.

Results: We first observed that prenatal exposure to glucocorticoids induced motility arrest and fragmentation of mitochondria in differentiating neurons derived from mouse fetuses (E18) and human induced pluripotent stem cells (hiPSCs). Further, glucocorticoid exposure during neurogenesis selectively downregulated Miro1 and increased Drp1 phosphorylation (Ser616). MIRO1 overexpression restored mitochondrial motility and increased intramitochondrial calcium influx through ER-mitochondria contact (ERMC) formation. Furthermore, we determined that the N-terminal GTPase domain of Miro1 plays a critical role in ERMC formation, which then decreased Drp1 phosphorylation (Ser616). Similarly, prenatal corticosterone exposure led to impaired neuropsychiatric and cognitive function in the offspring by affecting mitochondrial distribution and synaptogenesis, rescued by Miro1^WT, but not N-terminal GTPase active form Miro1^P26V, expression.

Conclusion: Prenatal glucocorticoid-mediated Miro1 downregulation contributes to dysfunction in mitochondrial dynamics through Drp1 phosphorylation (Ser616) in differentiating neurons.

Keywords: ER-mitochondria contacts; Miro; Mitochondrial dynamics; Neurodegeneration; Prenatal glucocorticoid.

MeSH terms

Animals
Dynamins* / metabolism
Female
Glucocorticoids / pharmacology
Hippocampus / metabolism
Humans
Induced Pluripotent Stem Cells / cytology
Induced Pluripotent Stem Cells / metabolism
Mice
Mitochondria / metabolism
Mitochondrial Dynamics* / drug effects
Mitochondrial Proteins* / metabolism
Neurons / metabolism
Phosphorylation
Pregnancy
Prenatal Exposure Delayed Effects* / metabolism
Stress, Physiological*
rho GTP-Binding Proteins* / chemistry
rho GTP-Binding Proteins* / metabolism

Substances

Dynamins
rho GTP-Binding Proteins
Dnm1l protein, mouse
Miro-1 protein, mouse
Mitochondrial Proteins
Glucocorticoids

Grants and funding

RS-2023-00208475/National Research Foundation of Korea