AI Article Synopsis

  • The study investigates the link between mitochondrial health, inflammation (specifically NLRP3 inflammasome activation), and white matter integrity in adolescents with mood disorders (bipolar disorder and major depressive disorder) compared to healthy controls.* -
  • Findings indicate that adolescents with mood disorders have lower white matter integrity and altered mitochondrial gene expression, particularly showing greater sensitivity to inflammation in those with bipolar disorder compared to those with major depressive disorder.* -
  • The results highlight potential biological markers that could help in understanding the development and pathophysiology of mood disorders during adolescence, a critical period for brain development.*

Article Abstract

Adolescence is a particularly important period for brain development and is also when mood disorders typically emerge. Several psychiatric illnesses exhibit mitochondrial dysfunction, elevated inflammation, and impaired white matter integrity. This study explored the intersection of mitochondrial health, NLRP3 inflammasome activation, and white matter integrity in a small cohort of 29 adolescent patients with mood disorders (bipolar disorder (BD): n = 11, major depressive disorder (MDD): n = 19) and 19 healthy controls. In this sample, adolescents with mood disorders showed lower fractional anisotropy of the ventral cingulum bundle than healthy controls. Across all adolescents, we demonstrated a significant relationship between mitochondrial electron transport chain gene expression, and NLRP3 inflammasome gene expression and activation. Furthermore, circulating cell free mitochondrial DNA was associated with lower white matter integrity in the anterior thalamic radiation. Exploratory subgroup analyses revealed that adolescents with bipolar disorder exhibited lower levels of mitochondrial gene expression and volume, along with increased sensitivity to NLRP3 inflammasome activation compared to adolescents with unipolar depression. Overall, our results reveal relationships between peripherally-measured endpoints of mitochondrial health and NLRP3 inflammasome activation, and centrally measured endpoints of white matter integrity in adolescents. Together with subtle patterns of aberrant neural and biological structure and function in association with mood disorder diagnoses, these results may shed light on the pathophysiology of disease in this early phase of illness.

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Source
http://dx.doi.org/10.1016/j.jad.2023.08.039DOI Listing

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