AI Article Synopsis

  • Emotional arousal significantly impacts memory strength and retrieval, with the dopaminergic and noradrenergic systems playing key roles in evaluating stimuli for rewards and threats.
  • Sex differences in the arousal system suggest that tailored therapeutic strategies might be more effective for neurological disorders related to learning and memory.
  • The interplay between catecholamines and the salience network highlights the need for sex-specific treatments for conditions like PTSD and opiate use disorder, with a focus on leveraging the endogenous cannabinoid system for therapeutic benefits.

Article Abstract

Emotional arousal is one of several factors that determine the strength of a memory and how efficiently it may be retrieved. The systems at play are multifaceted; on one hand, the dopaminergic mesocorticolimbic system evaluates the rewarding or reinforcing potential of a stimulus, while on the other, the noradrenergic stress response system evaluates the risk of threat, commanding attention, and engaging emotional and physical behavioral responses. Sex-specific patterns in the anatomy and function of the arousal system suggest that sexually divergent therapeutic approaches may be advantageous for neurological disorders involving arousal, learning, and memory. From the lens of the triple network model of psychopathology, we argue that post-traumatic stress disorder and opiate substance use disorder arise from maladaptive learning responses that are perpetuated by hyperarousal of the salience network. We present evidence that catecholamine-modulated learning and stress-responsive circuitry exerts substantial influence over the salience network and its dysfunction in stress-related psychiatric disorders, and between the sexes. We discuss the therapeutic potential of targeting the endogenous cannabinoid system; a ubiquitous neuromodulator that influences learning, memory, and responsivity to stress by influencing catecholamine, excitatory, and inhibitory synaptic transmission. Relevant preclinical data in male and female rodents are integrated with clinical data in men and women in an effort to understand how ideal treatment modalities between the sexes may be different.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8351794PMC
http://dx.doi.org/10.1111/ejn.14714DOI Listing

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