Mitochondrial Response to Psychological Stress and Its Medial Prefrontal Biomarker Correlates

  1. A. Ankeeta
  2. Ashutosh Tripathi
  3. Yizhou Ma
  4. Bindu Pillai
  5. Joshua J. Chiappelli
  6. Jennifer N. Jernberg
  7. Alia Warner
  8. Keiko Kunitoki
  9. Bhim M. Adhikari
  10. Si Gao
  11. Xiaoming Du
  12. Loise Kabui
  13. Francisco Pallares Solano
  14. Oluwabunmi Akindona
  15. Zhenyao Ye
  16. Shuo Chen
  17. Mohammad Milad
  18. Peter Kochunov
  19. Anilkumar Pillai
  20. L Elliot Hong
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Abstract

Background

Stress response obligates increased mitochondrial activities to meet stress-induced high energy requirement. This stress–mitochondrial response process involves glucocorticoid but also multiple alternative pathways that are top-down regulated by the medial prefrontal cortex (mPFC). These pathways are important for many neuropsychiatric conditions that are sensitive to stress. However, the field lacks a reliable, clinically accessible stress–mitochondrial response paradigm to study the process in humans.

Method

We used an established psychological stress challenge combined with assaying salivary cell-free mitochondrial DNA (cf-mtDNA), thought to reflect heightened mitochondrial changes or disruptions, in 35 healthy individuals (21 males). We also explored if these stress-induced cf-mtDNA marker elevations were associated brain metabolites as measured by magnetic resonance spectroscopy (MRS), as well as high-resolution brain imaging based cortical thickness focusing on the mPFC.

Results

We found that salivary cf-mtDNA was significant elevated immediately after the stress challenge (p=2.0×10 -7 ) and gradually declined after. Exploratory causal analysis showed that this cf-mtDNA response was not primarily driven by cortisol response. Instead, individuals with higher baseline dACC lactate+ levels, thought to in part reflect mitochondrial dysfunctions, was significantly associated with the cf-mtDNA response (r=0.80, p<0.001). Higher mtDNA response was also significantly associated with thinner dorsomedial prefrontal cortex (r=-0.52, p=0.01). Age had a U-shape effect such that cf-mtDNA response trended lower in earlier adulthood but higher in older people, explaining 33.8% of the ct-mtDNA response variance (p=0.003).

Conclusion

This stress challenge-salivary cf-mtDNA assay paradigm may offer a new, non-invasive approach to evaluate the stress-mitochondrial pathway functioning in aging, psychopharmacology, and neuropsychiatric conditions where psychological stress plays a role.

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  1. Version published to 10.1101/2025.07.30.667787 on bioRxiv