ELEVATED tph2 mRNA EXPRESSION IN A RAT MODEL OF CHRONIC ANXIETY

Donner, Nina C.; Johnson, Philip L.; Fitz, Stephanie D.; Kellen, Karen E.; Shekhar, Anantha; Lowry, Christopher A.

doi:10.1002/da.21925

Cited by 46 publications

(37 citation statements)

References 97 publications

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“…No. 74104, Qiagen, Valencia, USA), and used in an ISHH assay as described previously (Donner and Handa, 2009; Donner et al, 2012). To detect slc6a4 mRNA, a synthetic 50-base antisense oligonucleotide (5′-ACT GCA GAG TAC CCA TTG GAT ATT TGG CTA GGC TCT GCC CTG TCC GCT GT-3′, Integrated DNA Technologies, Coralville, IA, USA), complementary to bases 207–256 of rat slc6a4 mRNA (previously reported as bases 77–126 Fujita et al, 1993; Hansen and Mikkelsen, 1998), based on the published sequence of the rat serotonin transporter cDNA clone (Blakely et al, 1991) of slc6a4 mRNA ( Rattus norvegicus solute carrier family 6 (neurotransmitter transporter, serotonin), member 4, mRNA; GenBank Accession no., NM_013034.3) was used as previously described (Gardner et al, 2009a).…”

Section: Methodsmentioning

confidence: 99%

Development×environment interactions control tph2 mRNA expression

et al. 2013

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Adverse early life experience is thought to increase an individual's susceptibility to mental health disorders, including anxiety and affective disorders, later in life. Our previous studies have shown that post-weaning social isolation of female rats during a critical period of development sensitizes an anxiety-related serotonergic dorsal raphe nucleus (DR) system in adulthood. Therefore, we investigated how post-weaning social isolation, in combination with a challenge with the anxiogenic drug, N-methyl-beta-carboline-3-carboxamide (FG-7142; a partial inverse agonist at the benzodiazepine allosteric site on the GABAA receptor), affects home cage behavior and serotonergic gene expression in the DR of female rats using in situ hybridization histochemistry. Juvenile female rats were reared in isolation or groups of three for a 3-week period from weaning (postnatal day (PD) 21 to mid-adolescence (PD42)), after which all rats were group-reared for an additional 16 days until adulthood. Among vehicle-treated rats, isolation-reared rats had decreased tryptophan hydroxylase 2 (tph2) mRNA expression in ventral and ventrolateral subdivisions of the DR, a pattern observed previously in a rat model of panic disorder. Isolation-reared rats, but not group-reared rats, responded to FG-7142 with increased duration of vigilance and arousal behaviors. In addition, FG-7142 decreased tph2 expression, measured 4 h following treatment, in multiple subregions of the DR of group-reared rats but had no effect in isolation-reared rats. No treatment effects were observed on 5-HT1A receptor or serotonin transporter gene expression. These data suggest that adolescent social isolation alters tph2 expression in specific subregions of the DR and alters the effects of stress-related stimuli on behavior and serotonergic systems.

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Section: Methodsmentioning

confidence: 99%

Development×environment interactions control tph2 mRNA expression

et al. 2013

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“…First, we have shown that amygdala priming (using 5 × daily bilateral infusions of 6 fmol urocortin 1 into the BL) in male rats, which results in a chronic anxiety-like state as measured in the social interaction test, resulted in increased expression of tph2 , encoding Tph2, the rate-limiting enzyme in biosynthesis of serotonin, selectively in the DRVL/VLPAG serotonergic neurons and the caudal DRV serotonergic neurons (which have also been shown to project to the DPAG (Stezhka and Lovick, 1994;Vertes, 1991)), but not in any other subdivision of the DR (Donner et al, 2012). In addition, tph2 mRNA expression was highly correlated with anxiety-like behavior in the social interaction test ( r = 0.729; p = 0.001) (Donner et al, 2012). Second, we have shown that social defeat increases tph2 mRNA expression, but only in the DRVL/VLPAG serotonergic neurons, and only in rats previously exposed to maternal separation (Gardner et al, 2009).…”

Section: The Drvl/vlpag Serotonergic System a Critical Node In Pamentioning

confidence: 99%

“…Priming of the BLA, a structure critical for processing fear-related stimuli and gating output of the CE (Adolphs, 2013;LeDoux et al, 1988), by repeated urocortin 1 (UCN1) injections increases anxiety-like behavior and elevates tph2 mRNA in the DRVL/VLPAG (Donner et al, 2012). Microinjection of urocortin 2 (UCN2), a neuropeptide in the CRH family and a selective CRHR2 agonist, directly into the DR activates serotonergic neurons and increases extracellular 5-HT in DR projection regions like the BLA (Amat et al, 2004).…”

Section: Neuropeptide Modulation Of the Panic Inhibition Systemmentioning

confidence: 99%

“…We and others have found evidence for the following systems: 1) Panic inhibition system , a serotonergic system in the ventrolateral part of the dorsal raphe nucleus (DRVL)/ventrolateral periaqueductal gray (VLPAG), projecting to the DPAG, that a) is activated by panicogenic agents, including sodium lactate (Johnson et al, 2008) and hypercapnia (elevated atmospheric CO2; Johnson et al, 2005), b) selectively responds with increased tph2 mRNA expression following amygdala priming (Donner et al, 2012), a model of vulnerability to sodium lactate-induced panic attacks (Johnson et al, 2013;Sajdyk et al, 1999), and c) is selectively dysregulated in an animal model of vulnerability to lactate-induced panic-like responses (Johnson et al, 2004;Johnson et al, 2007). 2) Conflict anxiety facilitation system , a serotonergic system in the midline dorsal and caudal parts of the dorsal raphe nucleus (DRD/DRC), projecting to the basolateral nucleus of the amygdala (BLA; Abrams et al, 2005), that is activated by anxiogenic drugs (Abrams et al, 2005), anxiety-related neuropeptides (Staub et al, 2005;Staub et al, 2006), and anxiety-provoking stimuli (Spannuth et al, 2011); this system is sensitized following inescapable shock in a model of learned helplessness (Rozeske et al, 2011).…”

Section: Introduction To Panic Disordermentioning

confidence: 99%

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The Deakin/Graeff hypothesis: Focus on serotonergic inhibition of panic

Paul

Johnson

Shekhar

et al. 2014

Neuroscience & Biobehavioral Reviews

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The Deakin/Graeff hypothesis proposes that different subpopulations of serotonergic neurons through topographically organized projections to forebrain and brainstem structures modulate the response to acute and chronic stressors, and that dysfunction of these neurons increases vulnerability to affective and anxiety disorders, including Panic Disorder. We outline evidence supporting the existence of a serotonergic system originally discussed by Deakin/Graeff that is implicated in the inhibition of panic-like behavioral and physiological responses. Evidence supporting this panic inhibition system comes from the following observations: 1) serotonergic neurons located in the ‘ventrolateral dorsal raphe nucleus (DRVL) as well as the ventrolateral periaqueductal gray (VLPAG) inhibit dorsal periaqueductal gray-elicited panic-like responses; 2) chronic, but not acute, antidepressant treatment potentiates serotonin’s panicolytic effect; 3) contextual fear activates a central nucleus of the amygdala-DRVL/VLPAG circuit implicated in mediating freezing and inhibiting panic-like escape behaviors; 4) DRVL/VLPAG serotonergic neurons are central chemoreceptors and modulate the behavioral and cardiorespiratory response to panicogenic agents such as sodium lactate and CO2. Implications of the panic inhibition system are discussed.

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“…After dehydration and coverslipping, sections were photographed under identical camera settings. The outlines of two evenly spaced sections from each animal were manually traced, and their optical density (OD) was measured using NIH ImageJ while control-ling for background color and threshold levels (15,16). OD measurements of two sections from a single animal were averaged to obtain a value for that animal.…”

Section: Testicular Cyp17a1 Icc and Analysismentioning

confidence: 99%