Combined Neuropeptide S and D-Cycloserine Augmentation Prevents the Return of Fear in Extinction-Impaired Rodents: Advantage of Dual versus Single Drug Approaches

Sartori, Simone; Maurer, Verena; Murphy, Conor P.; Schmuckermair, Claudia; Muigg, Patrik; Neumann, Inga D.; Whittle, Nigel; Singewald, Nicolas

doi:10.1093/ijnp/pyv128

Cited by 25 publications

(11 citation statements)

References 74 publications

(116 reference statements)

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“…Injections of NPS into the cerebral ventricle or into the amygdala, the central site of the brain fear circuitry, reduce conditioned fear (e.g., Jüngling et al, 2008;Fendt et al, 2010), in line with the idea that NPS-deficient mice seem to be more anxious than wildtype mice (Liu et al, 2017). Moreover, NPS injections rescue stress-induced fear extinction deficits (Chauveau et al, 2012) and boost the beneficial effects of D-cycloserine on fear extinction (Sartori et al, 2016). Interestingly, exposure to forced swim stress induces an increase of amygdaloid NPS levels (Ebner et al, 2011).…”

Section: Introductionsupporting

confidence: 57%

Corticosterone Treatment and Incubation Time After Contextual Fear Conditioning Synergistically Induce Fear Memory Generalization in Neuropeptide S Receptor-Deficient Mice

Kolodziejczyk

Fendt

2020

Front. Neurosci.

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Fear memory generalization is a learning mechanism that promotes flexible fear responses to novel situations. While fear generalization has adaptive value, overgeneralization of fear memory is a characteristic feature of the pathology of anxiety disorders. The neuropeptide S (NPS) receptor (NPSR) has been shown to be associated with anxiety disorders and has recently been identified as a promising target for treating anxiety disorders. Moreover, stress hormones play a role in regulating both physiological and pathological fear memories and might therefore also be involved in anxiety disorders. However, little is known about the interplay between stress hormone and the NPS system in the development of overgeneralized fear. Here, we hypothesize that NPSR-deficient mice with high corticosterone (CORT) levels during the fear memories consolidation are more prone to develop generalized fear. To address this hypothesis, NPSR-deficient mice were submitted to a contextual fear conditioning procedure. Immediately after conditioning, mice received CORT injections (2.5 or 5 mg/kg). One day and 1 month later, the mice were tested for the specificity and strength of their fear memory, their anxiety level, and their startle response. Moreover, CORT blood levels were monitored throughout the experiment. Using this protocol, a specific contextual fear memory was observed in all experimental groups, despite the 5-mg/kg CORTtreated NPSR-deficient mice. This group of mice showed a generalization of contextual fear memory and a decreased startle response, and the females of this group had significantly less body weight gain. These findings indicate that interplay between CORT and the NPS system during the consolidation of fear memories is critical for the generalization of contextual fear.

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Section: Introductionsupporting

confidence: 57%

Corticosterone Treatment and Incubation Time After Contextual Fear Conditioning Synergistically Induce Fear Memory Generalization in Neuropeptide S Receptor-Deficient Mice

Kolodziejczyk

Fendt

2020

Front. Neurosci.

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“…Conversely, the synthetic NPSR antagonist SHA 68 (Okamura et al ., ) was able to attenuate fear extinction (Jüngling et al ., ). Two recent studies further confirmed NPS’ role in extinction of conditioned fear in models of rats and mice with high trait anxiety as well as a mouse model of attenuated fear extinction, respectively (Slattery et al ., ; Sartori et al ., ). These observations may be attributed to a profound memory‐enhancing effect of NPS, as we have previously described that activation of central NPS signaling can promote consolidation of long‐term memory, independent of emotional content of the memory trace, by interacting with noradrenergic signaling in the brain (Okamura et al ., ), and these memory‐enhancing effects were later replicated in rats and mice (Lukas & Neumann, ; Han et al ., ).…”

Section: Introductionmentioning

confidence: 97%

Neuropeptide S precursor knockout mice display memory and arousal deficits

Liu

Wei

Garau

et al. 2017

Eur J of Neuroscience

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Activation of neuropeptide S (NPS) signaling has been found to produce arousal, wakefulness, anxiolytic-like behaviors, and enhanced memory formation. In order to further study physiological functions of the NPS system, we generated NPS precursor knockout mice by homologous recombination in embryonic stem cells. NPS mice were viable, fertile, and anatomically normal, when compared to their wild-type and heterozygous littermates. The total number of NPS neurons-although no longer synthesizing the peptide - was not affected by the knockout, as analyzed in NPS /NPS double transgenic mice. Analysis of behavioral phenotypes revealed significant deficits in exploratory activity in NPS mice. NPS precursor knockout mice displayed attenuated arousal in the hole board test, visible as reduced total nose pokes and number of holes inspected, that was not confounded by increased repetitive or stereotypic behavior. Importantly, long-term memory was significantly impaired in NPS mice in the inhibitory avoidance paradigm. NPS precursor knockout mice displayed mildly increased anxiety-like behaviors in three different tests measuring responses to stress and novelty. Interestingly, heterozygous littermates often presented behavioral deficits similar to NPS mice or displayed intermediate phenotype. These observations may suggest limited ligand availability in critical neural circuits. Overall, phenotypical changes in NPS mice are similar to those observed in NPS receptor knockout mice and support earlier findings that suggest major functions of the NPS system in arousal, regulation of anxiety and stress, and memory formation.

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“…Our findings mirror these results as we demonstrated a within-session enhancement of CR extinction with the highest d-cycloserine dose that did not develop until an excess of 20 extinction trials were presented. Importantly, these studies in rodents also demonstrated that effects of d-cycloserine did not last long-term or prevent fear renewal (Bouton et al, 2008; Sartori et al, 2016). In agreement, our results from the extinction retention test one week later in the highest dose group showed no carryover of the extinction enhancement but rather showed an increase in responding at the beginning of the retention test compared to the terminal level at the end of extinction.…”

Section: Discussionmentioning

confidence: 90%

“…Similarly, in studies in rats, d-cycloserine was only beneficial when subjects exhibited some extinction learning (Bouton et al, 2008), and enhancement could be improved if more trials were presented under the drug (Bouton et al, 2008; Lee et al, 2006). In another example, d-cycloserine treatment in mice did not facilitate extinction in an extinction-resistant strain but did in strains able to demonstrate some extinction learning (Sartori et al, 2016). Our findings mirror these results as we demonstrated a within-session enhancement of CR extinction with the highest d-cycloserine dose that did not develop until an excess of 20 extinction trials were presented.…”

Section: Discussionmentioning

confidence: 99%

Effects of systemic glutamatergic manipulations on conditioned eyeblink responses and hyperarousal in a rabbit model of post-traumatic stress disorder

Burhans

Smith-Bell²,

Schreurs³

2017

Behavioural Pharmacology

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Glutamatergic dysfunction is implicated in many neuropsychiatric conditions including post-traumatic stress disorder (PTSD). Glutamate antagonists have shown some utility in treating PTSD symptoms while glutamate agonists may facilitate cognitive behavioral therapy outcomes. We have developed an animal model of PTSD, based on conditioning of the rabbit's eyeblink response, that addresses two key features: conditioned responses (CRs) to cues associated with an aversive event and a form of conditioned hyperarousal referred to as conditioning-specific reflex modification (CRM). The optimal treatment to reduce both CRs and CRM is unpaired extinction. The goals of the study were to examine whether treatment with the NMDA glutamate receptor antagonist ketamine could reduce CRs and CRM, and if the NMDA agonist d-cycloserine combined with unpaired extinction treatment could enhance extinction of both. Administration of a single-dose of subanesthetic ketamine had no significant immediate or delayed effect on CRs or CRM. Combining d-cycloserine with a single day of unpaired extinction facilitated extinction of CRs short-term while having no impact on CRM. These results caution that treatments may improve one aspect PTSD-symptomology while having no significant effects on other symptoms, stressing the importance of a multiple-treatment approach to PTSD and animal models that address multiple symptoms.

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Combined Neuropeptide S and D-Cycloserine Augmentation Prevents the Return of Fear in Extinction-Impaired Rodents: Advantage of Dual versus Single Drug Approaches

Cited by 25 publications

References 74 publications

Corticosterone Treatment and Incubation Time After Contextual Fear Conditioning Synergistically Induce Fear Memory Generalization in Neuropeptide S Receptor-Deficient Mice

Corticosterone Treatment and Incubation Time After Contextual Fear Conditioning Synergistically Induce Fear Memory Generalization in Neuropeptide S Receptor-Deficient Mice

Neuropeptide S precursor knockout mice display memory and arousal deficits

Effects of systemic glutamatergic manipulations on conditioned eyeblink responses and hyperarousal in a rabbit model of post-traumatic stress disorder

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