DECODING SEX-SPECIFIC VULNERABILITY TO ADOLESCENT SOCIAL STRESS THROUGH HOMECAGE BEHAVIOR AND SPATIAL PROTEOMICS
Max Delbrück Center for Molecular Medicine
Presentation
Date TBA
Event Information
Poster Board
PS02-07PM-271
Poster
View posterAbstract
Here, we utilize the social instability stress model in adolescent male and female mice to investigate why some individuals develop stress-related behavioral dysregulation later in life, while others remain resilient. For this, we employ a multimodal approach combining classical behavioral phenotyping, continuous homecage monitoring, and spatially resolved single-cell proteomics. This integrative framework enables the identification of behavioral and molecular signatures associated with stress susceptibility and resilience.We demonstrate that stress-susceptible animals exhibit distinct and persistent alterations in homecage behavior during both baseline and challenge conditions.
These findings highlight continuous homecage monitoring as a sensitive tool for detecting early indicators of stress vulnerability and depressive-like phenotypes. Spatial proteomic analyses further reveal cell-type-specific and region-specific molecular differences within the hippocampus that distinguish susceptible from resilient animals. Importantly, these molecular signatures may reflect both stress-induced adaptations and pre-existing biological features that influence individual stress responsiveness.
Together, these findings suggest that adolescent stress interacts with individual biological predispositions to shape behavioral and molecular outcomes. This work advances our understanding of the neurobiological mechanisms underlying stress vulnerability and highlights integrative behavioral and spatial omics approaches as powerful tools for studying psychiatric disease risk.
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