Corticotropin-releasing factor in the mouse central nucleus of the amygdala: Ultrastructural distribution in NMDA-NR1 receptor subunit expressing neurons as well as projection neurons to the bed nucleus of the stria terminalis

Beckerman, Marc A.; Kempen, Tracey A. Van; Justice, Nicholas J.; Milner, Teresa A.; Glass, Michael J.

doi:10.1016/j.expneurol.2012.10.009

Cited by 37 publications

(25 citation statements)

References 77 publications

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“…Most of the effects of the VDRA were restricted to process formation around the cell body; this is similar to the microtubule cytoskeletal system found in the dendritic nucleation assembly. This finding confirms the presence of VDR and its likely restriction to d cell body plus its role in facilitating short dendrite like process formation while NMDA R is located on the processes and facilitates long process formation; similar to the findings of Beckerman et al [37].…”

Section: Resultssupporting

confidence: 90%

VDR Potentiation and NMDA R Inhibition Facilitates Axo-Dendritic Process Formation in Melanocyte Model for Pigmented Cells in Parkinsonism

Michael

Ajonijebu²,

Chris³

et al. 2013

Cell Development Biol

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Background: A major cellular change in dopaminergic neurons leading to Parkinsonism is the alteration of microtubule proteins that causes accumulation of tau protein, α-syn and β-amyloid plaque in the cells. In this study we investigate the role of Vitamin D 3 in relieving the symptoms of Parkinsonism as it is capable of stimulating polymerization of microtubules. The Microtubules (MT) system in the fish scale melanocytes has been modeled for the dopaminergic neurons of the Substantia Nigra (SN). These cells are capable of forming cellular processes similar to what is seen in the dopaminergic neurons; in this study, we investigate the protective effect of Vitamin D 3 Receptor Agonist (VDRA) and N-Methyl-D-Aspartate Receptor (NMDA R) inhibition in process formation, synaptic denervation and melanin loss in fish scale melanocytes modeled as pigmented adrenergic cells.

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Section: Resultssupporting

confidence: 90%

VDR Potentiation and NMDA R Inhibition Facilitates Axo-Dendritic Process Formation in Melanocyte Model for Pigmented Cells in Parkinsonism

Michael

Ajonijebu²,

Chris³

et al. 2013

Cell Development Biol

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“…This study directly measured these 16 parameters and compared them to CRF-R1 lacking neurons (eGFP -). Our results 17 suggest that many CRF + neurons share some of these properties with CRF-R1 neurons 18 suggesting a partial overlap in these populations of genetically identified neurons 19(Beckerman et al, 2013). 20 CRF release in the extended amygdala has typically been associated with high-21 frequency, long duration firing of neurons; along with modulatory actions through G-22 protein coupled receptors (Rainnie et al, 1992; Yu and Shinnick-Gallagher, 1998)that the CRF-R1 antagonist, antalarmin, failed to affect light evoked IPSCs 1 in CRF -neurons in BnST and CeA.…”

mentioning

confidence: 79%

Stress increases GABAergic neurotransmission in CRF neurons of the central amygdala and bed nucleus stria terminalis

et al. 2016

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Corticotrophin Releasing Factor (CRF) is a critical stress-related neuropeptide in major output pathways of the amygdala, including the central nucleus (CeA), and in a key projection target of the CeA, the bed nucleus of the stria terminalis (BnST). While progress has been made in understanding the contributions and characteristics of CRF as a neuropeptide in rodent behavior, little attention has been committed to determine the properties and synaptic physiology of specific populations of CRF-expressing (CRF(+)) and non-expressing (CRF(-)) neurons in the CeA and BnST. Here, we fill this gap by electrophysiologically characterizing distinct neuronal subtypes in CeA and BnST. Crossing tdTomato or channelrhodopsin-2 (ChR2-YFP) reporter mice to those expressing Cre-recombinase under the CRF promoter allowed us to identify and manipulate CRF(+) and CRF(-) neurons in CeA and BnST, the two largest areas with fluorescently labeled neurons in these mice. We optogenetically activated CRF(+) neurons to elicit action potentials or synaptic responses in CRF(+) and CRF(-) neurons. We found that GABA is the predominant co-transmitter in CRF(+) neurons within the CeA and BnST. CRF(+) neurons are highly interconnected with CRF(-) neurons and to a lesser extent with CRF(+) neurons. CRF(+) and CRF(-) neurons differentially express tonic GABA currents. Chronic, unpredictable stress increase the amplitude of evoked IPSCs and connectivity between CRF(+) neurons, but not between CRF(+) and CRF(-) neurons in both regions. We propose that reciprocal inhibition of interconnected neurons controls CRF(+) output in these nuclei.

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“…Further, we and others have reported that CRF antagonism in the bed nucleus of the stria terminalis (BNST) can block the behavioral expression of social defeat (Cooper and Huhman, 2005;Jasnow et al, 2004b). This brain region receives heavy innervation from the CeA by neurons co-expressing CRF and Grin1 (glutamate receptor, ionotropic N-methyl-D-aspartate 1; NR1) receptor subunits (Beckerman et al, 2013). Blockade of this CRF-ergic projection also attenuates the behavioral effects of social defeat (Jasnow et al, 2004b).…”

Section: Introductionmentioning

confidence: 94%

Grin1 deletion in CRF neurons sex-dependently enhances fear, sociability, and social stress responsivity

Gilman

DaMert

Meduri

et al. 2015

Psychoneuroendocrinology

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Corticotropin-releasing factor in the mouse central nucleus of the amygdala: Ultrastructural distribution in NMDA-NR1 receptor subunit expressing neurons as well as projection neurons to the bed nucleus of the stria terminalis

Cited by 37 publications

References 77 publications

VDR Potentiation and NMDA R Inhibition Facilitates Axo-Dendritic Process Formation in Melanocyte Model for Pigmented Cells in Parkinsonism

VDR Potentiation and NMDA R Inhibition Facilitates Axo-Dendritic Process Formation in Melanocyte Model for Pigmented Cells in Parkinsonism

Stress increases GABAergic neurotransmission in CRF neurons of the central amygdala and bed nucleus stria terminalis

Grin1 deletion in CRF neurons sex-dependently enhances fear, sociability, and social stress responsivity

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