Overview of the central amygdala role in feeding behaviour

Izadi, Mina Sadat; Radahmadi, Maryam

doi:10.1017/s0007114521002312

Cited by 20 publications

(11 citation statements)

References 76 publications

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“…The basomedial nucleus and lateral zone of the posterior part of the cortical nucleus receive inputs from the main olfactory system, and each contains MC3R neurons that project to dorsal and ventral components of the anterior division of the BST, which contain very high densities of labeled axons but few MC3R cell bodies. Many MC3R neurons are located in the central amygdaloid nucleus (lateral part), which projects to the anterolateral area of the BST and plays an important role in multiple aspects of consummatory behavior and autonomic regulation (Cai et al., 2014; Dong et al., 2001; Hulsman et al., 2021; Izadi & Radahmadi, 2021; Kafami & Nasimi, 2016; Petrovich & Swanson, 1997; Saha, 2005). Notably, amygdalar cell groups that do not project directly to the BST (lateral and anterior basolateral nuclei) appear to lack MC3R neurons.…”

Section: Discussionmentioning

confidence: 99%

Organization of neural systems expressing melanocortin‐3 receptors in the mouse brain: Evidence for sexual dimorphism

Bedenbaugh

Brener

Maldonado

et al. 2022

J of Comparative Neurology

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The central melanocortin system is fundamentally important for controlling food intake and energy homeostasis. Melanocortin-3 receptor (MC3R) is one of two major receptors of the melanocortin system found in the brain. In contrast to the well-characterized melanocortin-4 receptor (MC4R), little is known regarding the organization of MC3R-expressing neural circuits. To increase our understanding of the intrinsic organization of MC3R neural circuits, identify specific differences between males and females, and gain a neural systems level perspective of this circuitry, we conducted a brain-wide mapping of neurons labeled for MC3R and characterized the distribution of their projections. Analysis revealed MC3R neuronal and terminal

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Section: Discussionmentioning

confidence: 99%

Organization of neural systems expressing melanocortin‐3 receptors in the mouse brain: Evidence for sexual dimorphism

Bedenbaugh

Brener

Maldonado

et al. 2022

J of Comparative Neurology

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“…What has been an open question in the field is how appetitive CeA neurons become activated. They could be activated via their afferent inputs, some of which have been characterized anatomically, but not functionally, including the basolateral amygdala (BLA), hypothalamus, substantia nigra, parasubthalamic nucleus (PSTN), and ventral tegmental area (VTA) (Douglass et al ., 2017; Izadi and Radahmadi, 2022; Kim et al ., 2017). Additionally, appetitive CeA neurons may be under hormonal control.…”

Section: Introductionmentioning

confidence: 99%

Transcriptomics reveals amygdala neuron regulation by fasting and ghrelin thereby promoting feeding

Peters

Fermani

et al. 2022

Preprint

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SUMMARYThe central amygdala (CeA) consists of numerous genetically-defined inhibitory neurons that control defensive and appetitive behaviors including feeding. Transcriptomic signatures of cell types and their links to function remain poorly understood. Using single-nucleus RNA-sequencing, we describe nine CeA cell clusters, of which four are mostly associated with appetitive and two with aversive behaviors. To analyze the activation mechanism of appetitive CeA neurons, we characterized Serotonin receptor 2a (Htr2a)-expressing neurons (CeAHtr2a) that comprise three appetitive clusters and were previously shown to promote feeding. In vivo calcium imaging revealed that CeAHtr2aneurons are activated by fasting, the hormone ghrelin, and the presence of food. Moreover, these neurons are required for the orexigenic effects of ghrelin. Appetitive CeA neurons responsive to fasting and ghrelin project to the parabrachial nucleus (PBN) causing inhibition of target PBN neurons. These results illustrate how the transcriptomic diversification of CeA neurons relates to fasting and hormone-regulated feeding behavior.HighlightsTranscriptomics reveals four appetitive, two aversive and three unknown CeA clustersGhrelin and fasting activate CeAHtr2aneurons comprising three appetitive clustersGhrelin’s orexigenic effects require the activity of appetitive CeA neuronsCeA-→PBN inhibition is necessary for ghrelin/fasting induced feeding

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“…Although the activation of DREADD H4 receptors did not affect consumption, activation of DREADD H3 receptors substantially decreased consumption. Again, this finding likely reflects complex differential effects of CeA manipulation; thought to modulate feeding behaviors, subpopulations within the CeA have been shown to enhance or inhibit consumption depending on the cell types affected (Cai et al, 2014; Douglass et al, 2017; for review, see Izadi & Radahmadi, 2021). Enhanced PIT was also accompanied by significantly higher prefeeding consumption in CIE animals relative to Air animals.…”

Section: Discussionmentioning

confidence: 99%

Effects of central amygdala chemogenetic manipulation and prior chronic alcohol exposure on Pavlovian‐to‐instrumental transfer

Shields

Gremel

2022

Alcoholism Clin & Exp Res

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Background Recent work suggests that a history of chronic alcohol exposure can enhance the influence of nondrug reward cues on ongoing actions. This is often modeled in Pavlovian‐to‐instrumental transfer (PIT) tasks that examine the interaction between Pavlovian and instrumental learning processes, usually reflected as an increase in action vigor during the presentation of a reward‐associated cue. Though prior chronic alcohol exposure strengthens this type of cue‐guided behavior, the neural mechanisms underlying such enhancements are not known. Methods In the present work, we examined the contribution of the central amygdala (CeA), a region strongly implicated in PIT behaviors and functionally altered by chronic alcohol exposure. We utilized Designer Receptors Exclusively Activated by Designer Drugs (DREADDs) to examine the impact of inhibitory and excitatory CeA manipulation on PIT behaviors in alcohol‐naïve mice and mice with a history of chronic intermittent ethano vapor exposure and withdrawal (CIE). Results Replicating previous work, we found that a history of CIE strengthened baseline PIT, in the absence of any CeA manipulation. We also found that activation of both inhibitory and excitatory DREADDs expressed in CeA enhanced PIT in alcohol‐naïve mice, though the latter markedly reduced response rates. However, in mice exposed to CIE, activation of excitatory DREADD receptors expressed in CeA appeared to weaken PIT. Conclusions These results suggest that alcohol‐induced disruptions in amygdala function may contribute to changes in appetitive behaviors, such as cue‐guided responding, following chronic exposure to alcohol. Better elucidating the neural mechanisms that underlie disrupted cue‐guided behavior following chronic alcohol exposure may help to understand and treat deficits in adaptive behavior associated with chronic alcohol use in humans.

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Overview of the central amygdala role in feeding behaviour

Cited by 20 publications

References 76 publications

Organization of neural systems expressing melanocortin‐3 receptors in the mouse brain: Evidence for sexual dimorphism

Organization of neural systems expressing melanocortin‐3 receptors in the mouse brain: Evidence for sexual dimorphism

Transcriptomics reveals amygdala neuron regulation by fasting and ghrelin thereby promoting feeding

Effects of central amygdala chemogenetic manipulation and prior chronic alcohol exposure on Pavlovian‐to‐instrumental transfer

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