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1. Neuroimmune mechanisms connecting violence with internalizing symptoms: A high‐dimensional multimodal mediation analysis

   https://doi.org/10.1002/hbm.26615  

   Butler, Ellyn R. ; Samia, Noelle ; White, Stuart ; Gratton, Caterina ; Nusslock, Robin ( February 2024 , Human Brain Mapping)

   Violence exposure is associated with worsening anxiety and depression symptoms among adolescents. Mechanistically, social defeat stress models in mice indicate that violence increases peripherally derived macrophages in threat appraisal regions of the brain, which have been causally linked to anxious behavior. In the present study, we investigate if there is a path connecting violence exposure with internalizing symptom severity through peripheral inflammation and amygdala connectivity. Two hundred and thirty‐three adolescents, ages 12–15, from the Chicago area completed clinical assessments, immune assays and neuroimaging. A high‐dimensional multimodal mediation model was fit, using violence exposure as the predictor, 12 immune variables as the first set of mediators and 288 amygdala connectivity variables as the second set, and internalizing symptoms as the primary outcome measure. 56.2% of the sample had been exposed to violence in their lifetime. Amygdala–hippocampus connectivity mediated the association between violence exposure and internalizing symptoms (, ). There was no evidence that inflammation or inflammation and amygdala connectivity in tandem mediated the association. Considering the amygdala and the hippocampus work together to encode, consolidate, and retrieve contextual fear memories, violence exposure may be associated with greater connectivity between the amygdala and the hippocampus because it could be adaptive for the amygdala and the hippocampus to be in greater communication following violence exposure to facilitate evaluation of contextual threat cues. Therefore, chronic elevations of amygdala–hippocampal connectivity may indicate persistent vigilance that leads to internalizing symptoms.

    

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2. Social buffering diminishes fear response but does not equal improved fear extinction

   https://doi.org/10.1093/cercor/bhac395  

   Gorkiewicz, Tomasz ; Danielewski, Konrad ; Andraka, Karolina ; Kondrakiewicz, Kacper ; Meyza, Ksenia ; Kaminski, Jan ; Knapska, Ewelina ( October 2022 , Cerebral Cortex)

   Social support during exposure-based psychotherapy is believed to diminish fear and improve therapy outcomes. However, some clinical trials challenge that notion. Underlying mechanisms remain unknown, hindering the understanding of benefits and pitfalls of such approach. To study social buffering during fear extinction, we developed a behavioral model in which partner’s presence decreases response to fear-associated stimuli. To identify the neuronal background of this phenomenon, we combined behavioral testing with c-Fos mapping, optogenetics, and chemogenetics. We found that the presence of a partner during fear extinction training causes robust inhibition of freezing; the effect, however, disappears in subjects tested individually on the following day. It is accompanied by lowered activation of the prelimbic (PL) and anterior cingulate (ACC) but not infralimbic (IL) cortex. Accordingly, blocking of IL activity left social buffering intact. Similarly, inhibition of the ventral hippocampus–PL pathway, suppressing fear response after prolonged extinction training, did not diminish the effect. In contrast, inhibition of the ACC–central amygdala pathway, modulating social behavior, blocked social buffering. By reporting that social modulation of fear inhibition is transient and insensitive to manipulation of the fear extinction-related circuits, we show that the mechanisms underlying social buffering during extinction are different from those of individual extinction.

    

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3. Proximal threats promote enhanced acquisition and persistence of reactive fear-learning circuits

   https://doi.org/10.1073/pnas.2004258117  

   Faul, Leonard ; Stjepanović, Daniel ; Stivers, Joshua M. ; Stewart, Gregory W. ; Graner, John L. ; Morey, Rajendra A. ; LaBar, Kevin S. ( June 2020 , Proceedings of the National Academy of Sciences)

   Physical proximity to a traumatic event increases the severity of accompanying stress symptoms, an effect that is reminiscent of evolutionarily configured fear responses based on threat imminence. Despite being widely adopted as a model system for stress and anxiety disorders, fear-conditioning research has not yet characterized how threat proximity impacts the mechanisms of fear acquisition and extinction in the human brain. We used three-dimensional (3D) virtual reality technology to manipulate the egocentric distance of conspecific threats while healthy adult participants navigated virtual worlds during functional magnetic resonance imaging (fMRI). Consistent with theoretical predictions, proximal threats enhanced fear acquisition by shifting conditioned learning from cognitive to reactive fear circuits in the brain and reducing amygdala–cortical connectivity during both fear acquisition and extinction. With an analysis of representational pattern similarity between the acquisition and extinction phases, we further demonstrate that proximal threats impaired extinction efficacy via persistent multivariate representations of conditioned learning in the cerebellum, which predicted susceptibility to later fear reinstatement. These results show that conditioned threats encountered in close proximity are more resistant to extinction learning and suggest that the canonical neural circuitry typically associated with fear learning requires additional consideration of a more reactive neural fear system to fully account for this effect.

    

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4. A special role for Anterior Cingulate Cortex, but not Orbitofrontal Cortex or Basolateral Amygdala, in choices involving information

   González, V. V. ( January 2023 , bioRxiv)

   Humans and other animals make decisions under uncertainty. Choosing an option that provides information can improve decision making. However, subjects often choose information that does not increase the chances of obtaining reward. In a procedure that promotes such paradoxical choice, animals choose between two alternatives: The richer option is followed by a cue that is rewarded 50% of the time (No-info) and the leaner option is followed by one of two cues, one always rewarded (100%), and the other never rewarded, 0% (Info). Since decisions involve comparing the subjective value of options after integrating all their features perhaps including information value, preference for information may rely on cortico-amygdalar circuitry. To test this, male and female Long-Evans rats were prepared with bilateral inhibitory DREADDs in the anterior cingulate cortex (ACC), orbitofrontal cortex (OFC), basolateral amygdala (BLA), or null virus infusions as a control. Using a counterbalanced design, we inhibited these regions after stable preference was acquired and during learning of new Info and No-info cues. We found that inhibition of ACC, but not OFC or BLA, selectively destabilized choice preference in female rats without affecting latency to choose or the response rate to cues. A logistic regression fit revealed that the previous choice strongly predicted preference in control animals, but not in female rats following ACC inhibition. BLA inhibition tended to decrease the learning of new cues that signaled the Info option, but had no effect on preference. The results reveal a causal, sex-dependent role for ACC in decisions involving information. 

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5. Chronic intranasal oxytocin increases acoustic eavesdropping and adult neurogenesis

   https://doi.org/10.1016/j.yhbeh.2023.105443  

   Monari, Patrick K. ; Herro, Zachary J. ; Bymers, Jessica ; Marler, Catherine A. ( November 2023 , Hormones and Behavior)

   Social information gathering is a complex process influenced by neuroendocrine-modulated neural plasticity. Oxytocin (OXT) is a key regulator of social decision-making processes such as information gathering, as it contextually modulates social salience and can induce long-term structural plasticity, including neurogenesis. Understanding the link between OXT-induced plasticity and communicative awareness is crucial, particularly because OXT is being considered for treatment of social pathologies. We investigated the role of chronic OXT-dependent plasticity in attention to novel social information by manipulating the duration of time following cessation of intranasal treatment to allow for the functional integration of adult-born neurons resulting from OXT treatment. Following a 3-week delay, chronic intranasal OXT (IN-OXT) increased approach behavior of both female and male mice towards aggressive vocal playbacks of two unseen novel conspecifics, while no effect was observed after a 3-day delay. Immature neurons increased in the ventral hippocampus of females and males treated with chronic IN-OXT after the 3-week delay, indicating a potential association between ventral hippocampal neurogenesis and approach/acoustic eavesdropping. The less the mouse approached, the higher the level of neurogenesis. Contrary to expectations, the correlation between ventral hippocampal neurogenesis and approach behavior was not affected by IN-OXT, suggesting that other plasticity mechanisms underlie the long-term effects of chronic OXT on social approach. Furthermore, we found a negative correlation between ventral hippocampal neurogenesis and freezing behavior. Overall, our results demonstrate that chronic IN-OXT-induced long-term plasticity can influence approach to vocal information and we further reinforced the link between neurogenesis and anxiety. 

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