Vulnerability to lasting anxiogenic effects of brief exposure to predator stimuli: Sex, serotonin and other factors—Relevance to PTSD

Adamec, Robert E.; Holmes, Andrew; Blundell, Jacqueline

doi:10.1016/j.neubiorev.2008.05.005

Cited by 53 publications

(30 citation statements)

References 96 publications

(117 reference statements)

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“…3A), demonstrating that CRF1 receptors in the BLA are required for the development of this stress-induced BLA NE neuroplasticity. Prevention of some long-term effects of a single predator stress have been reported previously with systemic CRF1-R antagonist (Adamec et al, 2010); our present results, for the first time, suggest a possible anatomical site for this phenomenon (the BLA). In contrast, the NEinduced PPI deficit was not altered by the administration of NBI27914 30 min after each ferret exposure ( p Ͻ 0.05 for mock2 vs NE challenge; Fig.…”

Section: Subsequent Intra-bla Ne Challengesupporting

confidence: 86%

“…Because the intent was to model in rats the intense psychogenic stress that is hypothesized to trigger cognitive deterioration in schizophrenia and PTSD (Walker and Diforio, 1997;Yehuda, 2004), a predator stress paradigm was used. This paradigm is considered to capture many of the precipitating features of psychological trauma and is used to study PTSD-like effects in animal models Adamec et al, 2008;Zoladz et al, 2008). Thus, rats (N ϭ 8) with BLA cannulae underwent three exposures to a ferret (one exposure per day); a mock injection into BLA (injectors lowered without infusion) occurred before and after the stress regimen.…”

Section: Resultsmentioning

confidence: 99%

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Predator Stress-Induced CRF Release Causes Enduring Sensitization of Basolateral Amygdala Norepinephrine Systems that Promote PTSD-Like Startle Abnormalities

2015

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The neurobiology of post-traumatic stress disorder (PTSD) remains unclear. Intense stress promotes PTSD, which has been associated with exaggerated startle and deficient sensorimotor gating. Here, we examined the long-term sequelae of a rodent model of traumatic stress (repeated predator exposure) on amygdala systems that modulate startle and prepulse inhibition (PPI), an operational measure of sensorimotor gating. We show in rodents that repeated psychogenic stress (predator) induces long-lasting sensitization of basolateral amygdala (BLA) noradrenergic (NE) receptors (␣1) via a corticotropin-releasing factor receptor 1 (CRF-R1)-dependent mechanism, and that these CRF1 and NE ␣1 receptors are highly colocalized on presumptive excitatory output projection neurons of the BLA. A profile identical to that seen with predator exposure was produced in nonstressed rats by intra-BLA infusions of CRF (200 ng/0.5 l), but not by repeated NE infusions (20 g/0.5 l). Infusions into the adjacent central nucleus of amygdala had no effect. Importantly, the predator stress-or CRF-induced sensitization of BLA manifested as heightened startle and PPI deficits in response to subsequent subthreshold NE system challenges (with intra-BLA infusions of 0.3 g/0.5 l NE), up to 1 month after stress. This profile of effects closely resembles aspects of PTSD. Hence, we reveal a discrete neural pathway mediating the enhancement of NE system function seen in PTSD, and we offer a model for characterizing potential new treatments that may work by modulating this BLA circuitry.

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Section: Subsequent Intra-bla Ne Challengesupporting

confidence: 86%

Section: Resultsmentioning

confidence: 99%

Predator Stress-Induced CRF Release Causes Enduring Sensitization of Basolateral Amygdala Norepinephrine Systems that Promote PTSD-Like Startle Abnormalities

2015

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“…Relatively little is known about molecular and neural substrates of such individual differences in coping (47). However correlational behavioral research implicates a variety of possible factors, including personality traits (28;36), interaction of genetic factors and experiential factors, such as reduced functioning polymorphisms in the serotonin transporter (5-HTTLPR), and life stress or social support at the time of stress (4;27;31). Moreover, reactivity of amygdala to environmental threat is modulated by 5-HTTLPR (27) which has also been implicated in PTSD (31;34).…”

Section: Introductionmentioning

confidence: 99%

Resilience against predator stress and dendritic morphology of amygdala neurons

Mitra

Adamec

Sapolsky

2009

Behavioural Brain Research

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Individual differences in coping response lie at the core of vulnerability to conditions like post traumatic stress disorder (PTSD). Like humans, not all animals exposed to severe stress show lasting change in affect. Predator stress is a traumatic experience inducing long-lasting fear, but not in all rodents. Thus, individual variation may be a cross species factor driving responsiveness to stressful events. The present study investigated neurobiological bases of variation in coping with severe stress. The amygdala was studied because it modulates fear and its function is affected by stress. Moreover, stress-induced plasticity of the amygdala has been related to induction of anxiety, a comorbid symptom of psychiatric conditions like PTSD. We exposed rodents to predator stress and grouped them according to their adaptability based on a standard anxiety test (the elevated plus maze). Subsequently we investigated if well-adapted (less anxious) and mal-adapted (extremely anxious) stressed animals differed in the structure of dendritic trees of their output neurons of the right basolateral amygdala (BLA). Two weeks after exposure to stress, well-adapted animals showed low anxiety levels comparable to unstressed controls, whereas mal-adapted animals were highly anxious. In these same animals, Golgi analysis revealed that BLA neurons of well-adapted rats exhibited more densely packed and shorter dendrites than neurons of mal-adapted or unstressed control animals, which did not differ. These data suggest that dendritic hypotrophy in the BLA may be a resilience marker against lasting anxiogenic effects of predator stress.

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“…Gene-environment interactions may unmask unrecognized phenotypes that are important in understanding complex diseases such as psychiatric disorders with known environmental risk factors (110,111). The mechanism of risk conferral for many of these environmental factors, such as exposure to environmental pathogens, maternal stress during pregnancy, or maternal substance abuse during pregnancy, may be investigated by using animal models in a controlled laboratory setting to reveal latent phenotypes and resolve gene-environment interactions ( Figure 3C) (112)(113)(114)(115)(116).…”

Section: Animal Models and Lncrna Functionmentioning

confidence: 99%