Combined neonatal stress and young‐adult glucocorticoid stimulation in rats reduce BDNF expression in hippocampus: Effects on learning and memory

Choy, Kwok Ho Christopher; Visser, Yvonne de; Nichols, Nancy R.; Buuse, Maarten van den

doi:10.1002/hipo.20425

Cited by 122 publications

(80 citation statements)

References 62 publications

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“…The Y maze assesses hippocampal spatial recognition memory and consists of a three-armed chamber, with the arms at a 1201 angle from each other. Each arm is 35 cm long, 5.0 cm wide, and 10 cm high (Choy et al, 2008). Phase 1.…”

Section: Behavioral Analysismentioning

confidence: 99%

Effects of Centrally Administered Etanercept on Behavior, Microglia, and Astrocytes in Mice Following a Peripheral Immune Challenge

Camara

Corrigan

Jaehne

et al. 2014

Neuropsychopharmacol

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Section: Behavioral Analysismentioning

confidence: 99%

Effects of Centrally Administered Etanercept on Behavior, Microglia, and Astrocytes in Mice Following a Peripheral Immune Challenge

Camara

Corrigan

Jaehne

et al. 2014

Neuropsychopharmacol

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“…41 DNA-methylation has been shown to persist from early developmental stages into adulthood 25 and thus is the most likely candidate mechanism for persistent memory trace between childhood experiences and adult depression. Epigenetic modifications resulting from adverse childhood experiences are likely to modify through the life course the expression and inducibility by stress of key proteins in the hypothalamus-pituitaryadrenal axis, 24,25 neurotrophins, 42 immune system 43 and serotonergic neurotransmission, 44,45 and thus shape the vulnerability to depression.…”

Section: Principles Of Gene-environment Interactionsmentioning

confidence: 99%

The implications of gene–environment interactions in depression: will cause inform cure?

Uher

2008

Mol Psychiatry

133

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In a number of human diseases, including depression, interactions between genetic and environmental factors have been identified in the absence of direct genotype-disorder associations. The lack of genes with major direct pathogenic effect suggests that genotype-specific vulnerabilities are balanced by adaptive advantages and implies aetiological heterogeneity. A model of depression is proposed that incorporates the interacting genetic and environmental factors over the life course and provides an explanatory framework for the heterogeneous aetiology of depression. Early environmental influences act on the genome to shape the adaptability to environmental changes in later life. The possibility is explored that genotype-and epigenotype-related traits can be harnessed to develop personalized therapeutic interventions. As diagnosis of depression alone is a weak predictor of response to specific treatments, aetiological subtypes can be used to inform the choice between treatments. As a specific application of this notion, a hypothesis is proposed regarding relative responsiveness of aetiological subtypes of depression to psychological treatment and antidepressant medication. Other testable predictions are likely to emerge from the general framework of interacting genetic, epigenetic and environmental mechanisms in depression.

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“…It is involved in many functional processes critical for the brain development and experience-dependent neuroplasticity, such as neuronal survival, neural migration, differentiation, synapse formation, and modulation of neurotransmitter synthesis [2][3][4]. It also plays an important role in stress response, learning and memory, and actions of psychoactive drugs [5][6][7]. Accumulating clinical evidence indicates that abnormal BDNF expressions may contribute to pathophysiology of schizophrenia, as the levels of BDNF have been found decreased in peripheral (blood) and central (brain) systems of patients with schizophrenia [8][9][10][11].…”

Section: Introductionmentioning

confidence: 99%

Is Brain-derived Neurotrophic Factor a Possible Mechanism Underlying Risperidone Sensitization in Adolescent Rats?

Shu¹

2013

Biochem & Pharmacol

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IntroductionBrain-derived neurotrophic factor (BDNF) is a member of the neurotrophin family that is widely distributed in the brain with the highest levels found in the hippocampus and other cortical areas [1]. It is involved in many functional processes critical for the brain development and experience-dependent neuroplasticity, such as neuronal survival, neural migration, differentiation, synapse formation, and modulation of neurotransmitter synthesis [2][3][4]. It also plays an important role in stress response, learning and memory, and actions of psychoactive drugs [5][6][7]. Accumulating clinical evidence indicates that abnormal BDNF expressions may contribute to pathophysiology of schizophrenia, as the levels of BDNF have been found decreased in peripheral (blood) and central (brain) systems of patients with schizophrenia [8][9][10][11]. Antipsychotic drugs can also alter the brain levels of BDNF, and prevent the stress-induced decrease in the levels of BDNF, indicating that it may also regulate the action of antipsychotic drugs [12][13][14][15][16][17].In recent years, we have used the Conditioned Avoidance Response (CAR) and phencyclidine (PCP)-induced hyperlocomotion to examine the long-term treatment effects of antipsychotic drugs [18][19][20][21][22][23]. Both tests are known for their high predictive validity for antipsychotic efficacy, as antipsychotic drugs show a robust suppression of avoidance response and PCP-induced hyperlocomotion upon acute drug administration [24,25]. Testing an antipsychotic drug in two independent tests of antipsychotic activity is necessary to ensure that any observed antipsychotic effect is not an artifact of any particular model but reflects the generality of the treatment effect. We have been particularly interested in how repeated antipsychotic treatment alters this suppression over time. Such alterations can be manifested as either tolerance, which is characterized by decreased responsiveness to a certain drug effect, or sensitization, which is characterized by increased responsiveness to a drug effect [26]. The typical paradigm that we developed to study antipsychotic sensitization and tolerance consists of an induction phase, in which rats are repeatedly treated with an antipsychotic drug or vehicle for several days and tested for their avoidance responses and PCP-induced hyperlocomotion, and an expression phase, in which all rats are given a challenge dose of the drug and their avoidance and motor activity under PCP is tested again [18,19,21,22,27]. Using such a paradigm, we show that repeated treatment of haloperidol or olanzapine progressively increases its suppression of avoidance responding across the test sessions in the induction phase, and makes animals more sensitive to these drugs AbstractRisperidone is one of the most widely used atypical antipsychotic drugs and is approved for the treatment of mental disorders (eg. schizophrenia, autism) in children and adolescents. The present study investigated the repeated treatment effect of risperidone and associa...

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Combined neonatal stress and young‐adult glucocorticoid stimulation in rats reduce BDNF expression in hippocampus: Effects on learning and memory

Cited by 122 publications

References 62 publications

Effects of Centrally Administered Etanercept on Behavior, Microglia, and Astrocytes in Mice Following a Peripheral Immune Challenge

Effects of Centrally Administered Etanercept on Behavior, Microglia, and Astrocytes in Mice Following a Peripheral Immune Challenge

The implications of gene–environment interactions in depression: will cause inform cure?

Is Brain-derived Neurotrophic Factor a Possible Mechanism Underlying Risperidone Sensitization in Adolescent Rats?

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