Nucleus accumbens dopaminergic neurotransmission switches its modulatory action in chronification of inflammatory hyperalgesia

Dias, Elayne Vieira; Sartori, César Renato; Marião, Paula Ramos; Vieira, André Schwambach; Camargo, Lilian Calili; Athié, Maria Carolina Pedro; Pagliusi, Marco; Tambeli, Cláudia Herrera; Parada, Carlos Amílcar

doi:10.1111/ejn.13015

Cited by 24 publications

(29 citation statements)

References 48 publications

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“…Recent data from our group demonstrated that chronic stimulation of the mesolimbic dopaminergic system by intra‐NAc administration of a dopamine reuptake inhibitor facilitated the development of persistent hyperalgesia induced by PGE2 administered in peripheral tissue (Dias et al., ). This study also demonstrated that acute stimulation of the mesolimbic dopaminergic system induces analgesia via dopamine D2 receptor activation, while chronic stimulation of this system may induce plastic changes which lead to persistent hyperalgesia.…”

Section: Discussionmentioning

confidence: 98%

“…The NAc seems to play an important role in pain modulation (Altier & Stewart, ; Gear, Aley, & Levine, ; Magnusson & Martin, ; Tambeli, Parada, Levine, & Gear, ; Tambeli, Quang, Levine, & Gear, ; Taylor, Joshi, & Uppal, ). Our group recently demonstrated that the NAc has a facilitatory role in persistent inflammatory hyperalgesia that contributes to the chronification of pain in a dependent manner of the dopaminergic neurotransmission (Dias et al., ). Moreover, there is a robust body of evidence indicating the involvement of the dopaminergic mesolimbic system in depressive‐like behavior.…”

Section: Introductionmentioning

confidence: 99%

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Social defeat stress induces hyperalgesia and increases truncated BDNF isoforms in the nucleus accumbens regardless of the depressive‐like behavior induction in mice

Pagliusi

Bonet

Dias

et al. 2018

Eur J of Neuroscience

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Epidemiological studies have shown a close association between pain and depression. There is evidence showing this association as patients with depression show a high chronic pain prevalence and vice versa. Considering that social stress is critical for the development of depression in humans, we used a social defeat stress (SDS) model which induces depressive-like behavior in mice. In this model, mice are exposed to an aggressor mouse for ten days, suffering brief periods of agonistic contact and long periods of sensory contact. Some mice display social avoidance, a depressive-like behavior, and are considered susceptible, while some mice do not, and are considered resilient. Thus, we investigated the nociceptive behavior of mice submitted to SDS and the neuroplastic changes in dopaminergic mesolimbic system. Our results showed that the stressed mice (resilient and susceptible) presented a higher sensitivity to pain than the control mice in chemical and mechanical tests. We also verified that susceptible mice have higher Bdnf mRNA in the VTA compared to the resilient and control mice. The stressed mice had less mature BDNF and more truncated BDNF protein in the NAc compared with control mice. Although social stress may trigger the development of depression and hyperalgesia, these two conditions may manifest independently as social stress induced hyperalgesia even in mice that did not display depressive-like behavior. Also, increased Bdnf in the VTA seems to be associated with depressive-like behavior, whereas high levels of truncated BDNF and low mature BDNF appear to be associated with hyperalgesia induced by social defeat stress.

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Section: Discussionmentioning

confidence: 98%

Section: Introductionmentioning

confidence: 99%

Social defeat stress induces hyperalgesia and increases truncated BDNF isoforms in the nucleus accumbens regardless of the depressive‐like behavior induction in mice

Pagliusi

Bonet

Dias

et al. 2018

Eur J of Neuroscience

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“…Briefly, the original model showed that 14 successive days of intraplantar injection of PGE2 was sufficient to induce persistent hyperalgesia in rodents for more than 30 days after the last PGE2 injection (Ferreira et al, 1990;Villarreal et al, 2009). Here we used a PGE2-induced PH-ST protocol with only seven successive days of intraplantar injection of PGE2, which is not enough to produce persistent hyperalgesia (Ferreira et al, 1990;Dias et al, 2015). Pharmacological studies revealed the role of noninflammatory agents during the hyperalgesia induction, such as PKA (protein kinase A), PKCε (protein kinase C isoform ε), AC (adenylyl cyclase) (Sachs et al, 2009;Villarreal et al, 2009), and NF-κB (nuclear factor kappa-B) (Souza et al, 2015).…”

Section: Prostaglandin E2-induced Persistent Hyperalgesia Short-term mentioning

confidence: 99%

Physical Activity Induces Nucleus Accumbens Genes Expression Changes Preventing Chronic Pain Susceptibility Promoted by High-Fat Diet and Sedentary Behavior in Mice

et al. 2020

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Recent findings from rodent studies suggest that high-fat diet (HFD) increases hyperalgesia independent of obesity status. Furthermore, weight loss interventions such as voluntary physical activity (PA) for adults with obesity or overweight was reported to promote pain reduction in humans with chronic pain. However, regardless of obesity status, it is not known whether HFD intake and sedentary (SED) behavior is underlies chronic pain susceptibility. Moreover, differential gene expression in the nucleus accumbens (NAc) plays a crucial role in chronic pain susceptibility. Thus, the present study used an adapted model of the inflammatory prostaglandin E2 (PGE2)induced persistent hyperalgesia short-term (PH-ST) protocol for mice, an HFD, and a voluntary PA paradigm to test these hypotheses. Therefore, we performed an analysis of differential gene expression using a transcriptome approach of the NAc. We also applied a gene ontology enrichment tools to identify biological processes associated with chronic pain susceptibility and to investigate the interaction between the factors studied: diet (standard diet vs. HFD), physical activity behavior (SED vs. PA) and PH-ST (PGE vs. saline). Our results demonstrated that HFD intake and sedentary behavior promoted chronic pain susceptibility, which in turn was prevented by voluntary physical activity, even when the animals were fed an HFD. The transcriptome of the NAc found 2,204 differential expression genes and gene ontology enrichment analysis revealed 41 biologic processes implicated in chronic pain susceptibility. Taking these biological processes together, our results suggest that genes related to metabolic and mitochondria stress were up-regulated in the chronic pain susceptibility group (SED-HFD-PGE), whereas genes related to neuroplasticity were up-regulated in the non-chronic pain susceptibility group (PA-HFD-PGE). These findings provide pieces of evidence that HFD intake and sedentary behavior provoked gene expression changes in the NAc related to promotion of chronic pain susceptibility, whereas voluntary physical activity provoked gene expression changes in the NAc related to prevention of chronic

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“…Briefly, the original model showed that 14 successive days of 10 intraplantar injection of PGE2 was sufficient to induce persistent hyperalgesia in rodents for more 11 than thirty days after the last PGE2 injection (Ferreira et al, 1990;Villarreal et al, 2009). However, 12 here we used a PH-ST protocol with only seven successive days of intraplantar injection of PGE2, 13 which was not enough to produce persistent hyperalgesia (Dias et al, 2015;Ferreira et al, 1990). 14 This model was advantageous compare to others' CP models because further pharmacological studies 15 revealed a key role of non-inflammatory agents in the chronification process, such as PKA (protein 16 kinase A), PKCε (protein kinase C isoform ε), AC (adenylyl cyclase) (Sachs et al, 2009;Villarreal 17 et al, 2009) and NF-κB (nuclear factor kappa-B) (Souza et al, 2015).…”

Section: Prostaglandin E2-induced Persistent Hyperalgesia Short-term mentioning

confidence: 99%

“…These findings support a study by Song et al (2017) when they found an increase of pain behaviors 22 promoted by an HFD regardless of weight gain. Although the authors found an increased macrophage 23 density in the dorsal root ganglia and increased pain behaviors (Song et al, 2017), they did not 24 investigate any potential effect of an HFD and sedentary behavior in the NAc, a key structure in the 25 CP susceptibility (Dias et al, 2015;Schwartz et al, 2017;Zhang et al, 2019). 26 Furthermore, we reported here that the voluntary PA prevented CP susceptibility promoted by an 27 HFD and sedentary behavior.…”

Section: Differential Gene Expression In the Nucleus Accumbens -Transmentioning

confidence: 99%

Physical Activity Induces Nucleus Accumbens Genes Expression Changes Preventing Chronic Pain Susceptibility Promoted by High-Fat Diet and Sedentary Behavior in Mice

Brandão¹,

Bonet

Pagliusi³

et al. 2019

Preprint

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4High-fat diet (HFD)-induced obesity was reported to increase pain behavior independent of obesity 5 status in rats, whereas weight loss interventions such as voluntary physical activity (PA) for adults 6 with overweight or obesity was reported to promote pain reduction in humans with chronic pain (CP). 7 However, is unknown whether an HFD and sedentary (SED) behavior is underlying to CP 8 susceptibility and whether voluntary PA can prevent it. Moreover, differential gene expression in the 9 nucleus accumbens (NAc) is considered to play a crucial role in CP susceptibility. The present study 10 used an adapted model of the inflammatory prostaglandin E2 (PGE)-induced persistent hyperalgesia 11 (PH-ST) protocol for mice, an HFD, and a voluntary PA paradigm to test these hypotheses. In 12 addition, we performed a transcriptome in the NAc and a gene ontology enrichment tools to 13 investigate the differential gene expression and identify the biological processes associated with CP 14 susceptibility tested here. Our results demonstrated that HFD and sedentary behavior promoted CP 15 susceptibility, which in turn was prevented by voluntary PA, even when the animals were fed an 16 HFD. Transcriptome in the NAc found 2,204 differential expression genes related CP susceptibility 17 promoted by HFD and sedentary behavior and prevented by voluntary PA. The gene ontology 18 enrichment revealed 41 biological processes implicated in CP susceptibility. Analyzing collectively 19 those biological processes, our results suggested that genes related to metabolic and mitochondria 20 stress were up-regulated in the CP susceptibility group, whereas genes related to neuroplasticity and 21 axonogenesis were up-regulated in the CP prevented group. These findings provide pieces of 22 evidence that an HFD and sedentary behavior promoted gene expression changes in the NAc related 23 to neurodegeneration and those changes were also underlying to CP susceptibility. Additionally, our 24 findings confirmed other findings supporting the crucial role of voluntary PA to prevent CP 25 susceptibility and add novel insights of differential gene expression in the NAc related to 26 neuroplasticity. 27 28

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Nucleus accumbens dopaminergic neurotransmission switches its modulatory action in chronification of inflammatory hyperalgesia

Cited by 24 publications

References 48 publications

Social defeat stress induces hyperalgesia and increases truncated BDNF isoforms in the nucleus accumbens regardless of the depressive‐like behavior induction in mice

Social defeat stress induces hyperalgesia and increases truncated BDNF isoforms in the nucleus accumbens regardless of the depressive‐like behavior induction in mice

Physical Activity Induces Nucleus Accumbens Genes Expression Changes Preventing Chronic Pain Susceptibility Promoted by High-Fat Diet and Sedentary Behavior in Mice

Physical Activity Induces Nucleus Accumbens Genes Expression Changes Preventing Chronic Pain Susceptibility Promoted by High-Fat Diet and Sedentary Behavior in Mice

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