Prefrontal Cortex Response to Prenatal Insult and Postnatal Opioid Exposure

Rymut, Haley E; Rund, Laurie A.; Southey, Bruce R.; Johnson, Rodney W.; Sweedler, Jonathan V.; Rodríguez-Zas, Sandra L.

doi:10.3390/genes13081371

Cited by 4 publications

(3 citation statements)

References 74 publications

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“…The gene expression profiles suggest an antagonistic interaction between the stressors, opposite to that observed in the reproductive system's processes. The profiles observed in the present study were consistent with the over-expression of prefrontal cortex genes in the chemokine signaling pathway of the pigs exposed to MIA [49], and the under-expression of the genes annotated to the inflammation-associated pathways in the amygdala and hippocampus of the weaned pigs [16,46]. The importance of changes in the immune system pathway of the pituitary gland, in response to prenatal and weaning challenges, can also be related to the established immuno-enhancing role of many hormones secreted by the pituitary gland (e.g., prolactin, growth hormone, insulin growth factor-1, and thyroid hormones) in susceptibility to stressinduced disease [50].…”

Section: Discussionsupporting

confidence: 89%

Genes Participating in the Ensheathment of Neurons Are Affected by Postnatal Stress and Maternal Immune Activation in the Pituitary Gland

Alsegehy

Southey

Rund

et al. 2023

Genes

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Immune challenges during gestation are associated with neurodevelopmental disorders and can interact with stress later in life. The pituitary gland participates in endocrine- and immune-related processes that influence development, growth, and reproduction and can modulate physiological and behavioral responses to challenges. The objective of this study was to investigate the effect of stressors at different time points on the molecular mechanisms of the pituitary gland and detect sex differences. RNA sequencing was used to profile the pituitary glands of female and male pigs exposed to weaning stress and virally induced maternal immune activation (MIA), relative to unchallenged groups. Significant effects (FDR-adjusted p-value < 0.05) of MIA and weaning stress were detected in 1829 and 1014 genes, respectively. Of these, 1090 genes presented significant interactions between stressors and sex. The gene ontology biological process of the ensheathment of neurons (GO:0007272), substance abuse, and immuno-related pathways, including the measles disease (ssc05162), encompasses many genes with profiles impacted by MIA and weaning stress. A gene network analysis highlighted the under-expression of myelin protein zero (Mpz) and inhibitors of DNA binding 4 (Id4) among the non-stressed males exposed to MIA, relative to the control and non-MIA males exposed to weaning stress, relative to non-stressed pigs. The detection of changes in the molecular mechanisms of the pituitary gland could advance our understanding of disruptions in the formation of the myelin sheath and the transmission of neuron-to-neuron signals in behavioral disorders associated with maternal immune activation and stress.

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Section: Discussionsupporting

confidence: 89%

Genes Participating in the Ensheathment of Neurons Are Affected by Postnatal Stress and Maternal Immune Activation in the Pituitary Gland

Alsegehy

Southey

Rund

et al. 2023

Genes

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“…7D), with several GO terms represented (e.g, phospholipid processes, histone acetylation, and calcium signaling) (Table 1). Indeed, several of these genes (e.g, SMAD3 , HTR7 , PPP1R17 ) 56–60 and their upstream regulators (e.g., STAT3, AR, mir-124) have previously been associated with cocaine exposure 61–64 (Fig. 7E).…”

Section: Resultsmentioning

confidence: 92%

Transcriptional characterization of cocaine withdrawal versus extinction within nucleus accumbens

Martínez-Rivera,

Holt,

Minier-Toribio

et al. 2024

Preprint

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Substance use disorder is characterized by a maladaptive imbalance wherein drug seeking persists despite negative consequences or drug unavailability. This imbalance correlates with neurobiological alterations some of which are amplified during forced abstinence, thereby compromising the capacity of extinction-based approaches to prevent relapse. Cocaine use disorder (CUD) exemplifies this phenomenon in which neurobiological modifications hijack brain reward regions such as the nucleus accumbens (NAc) to manifest craving and withdrawal-like symptoms. While increasing evidence links transcriptional changes in the NAc to specific phases of addiction, genome-wide changes in gene expression during withdrawal vs. extinction (WD/Ext) have not been examined in a context- and NAc-subregion-specific manner. Here, we used cocaine self-administration (SA) in rats combined with RNA-sequencing (RNA-seq) of NAc subregions (core and shell) to transcriptionally profile the impact of experiencing withdrawal in the home cage or in the previous drug context or experiencing extinction training. As expected, home-cage withdrawal maintained drug seeking in the previous drug context, whereas extinction training reduced it. By contrast, withdrawal involving repetitive exposure to the previous drug context increased drug-seeking behavior. Bioinformatic analyses of RNA-seq data revealed gene expression patterns, networks, motifs, and biological functions specific to these behavioral conditions and NAc subregions. Comparing transcriptomic analysis of the NAc of patients with CUD highlighted conserved gene signatures, especially with rats that were repetitively exposed to the previous drug context. Collectively, these behavioral and transcriptional correlates of several withdrawal-extinction settings reveal fundamental and translational information about potential molecular mechanisms to attenuate drug-associated memories.

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“…This Special Issue presents the results of another experiment by the same group of authors, which aimed to study the impact of proinflammatory challenges caused by maternal immune activation (MIA) and postnatal exposure to drugs of abuse (morphine) on the prefrontal cortex molecular pathways [ 8 ]. The range of interacting effects on the prefrontal cortex pathways were uncovered, providing new insights into the interplay between the effects of MIA and morphine.…”

mentioning

confidence: 99%