Chronic Glucocorticoids Increase Hippocampal Vulnerability to Neurotoxicity under Conditions That Produce CA3 Dendritic Retraction But Fail to Impair Spatial Recognition Memory

Conrad, Cheryl D.; McLaughlin, Katie J.; Harman, James S.; Foltz, Cainan H.; Wieczorek, Lindsay; Lightner, Elizabeth N.; Wright, Ryan L.

doi:10.1523/jneurosci.2121-07.2007

Cited by 128 publications

(89 citation statements)

References 41 publications

(50 reference statements)

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“…Histological quantification, involving the measurement of CA3 or amygdala dendritric branch length for selected neurons, was performed with AxioVision 4.7 software and a Zeiss Imager M1 microscope. For each rat, total dendrite length was measured for amygdala neuron and separately for the apical branch and the basal sections of the CA3 neuron, as described by McLaughlin et al (2005) and Conrad et al (2007). We selected three to five hippocampal neurons per rat for measurement by an investigator blind to the origin of the experimental animal.…”

Section: Golgi Stainingmentioning

confidence: 99%

Vulnerability to Depression: From Brain Neuroplasticity to Identification of Biomarkers

Blugeot¹,

Rivat²,

Bouvier³

et al. 2011

J. Neurosci.

161

147

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A stressful event increases the risk of developing depression later in life, but the possible predisposing factors remain unknown. Our study aims to characterize latent vulnerability traits underlying the development of depressive disorders in adult animals. Four weeks after a priming stressful event, serum corticosterone concentration returned to control values in all animals, whereas the other biological parameters returned to basal level in only 58% of animals (called nonvulnerable). In contrast, 42% of animals displayed persistent decreased serum and hippocampus BDNF concentrations, reduced hippocampal volume and neurogenesis, CA3 dendritic retraction and decrease in spine density, as well as amygdala neuron hypertrophy, constituting latent vulnerability traits to depression. In this group, called vulnerable, a subsequent mild stress evoked a rise of serum corticosterone levels and a "depressive" phenotype, in contrast to nonvulnerable animals. Intracerebroventricular administration of 7,8-dihydroxyflavone, a selective TrkB receptor agonist, dampened the development of the "depressive" phenotype. Our results thus characterize the presence of latent vulnerability traits that underlie the emergence of depression and identify the association of low BDNF with normal corticosterone serum concentrations as a predictive biomarker of vulnerability to depression.

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Section: Golgi Stainingmentioning

confidence: 99%

Vulnerability to Depression: From Brain Neuroplasticity to Identification of Biomarkers

Blugeot¹,

Rivat²,

Bouvier³

et al. 2011

J. Neurosci.

161

147

View full text Add to dashboard Cite

show abstract

“…All brains were removed and processed at the same time (72 hours following the last injection). The staining procedure was the same as described previously by our lab (Bellani et al, 2006;Conrad et al, 2007;Kleen et al, 2006;McLaughlin et al, 2005;McLaughlin et al, 2007).…”

Section: Golgimentioning

confidence: 99%

Assessment of estradiol influence on spatial tasks and hippocampal CA1 spines: Evidence that the duration of hormone deprivation after ovariectomy compromises 17β-estradiol effectiveness in altering CA1 spines

McLaughlin

Bimonte‐Nelson

Neisewander

et al. 2008

Hormones and Behavior

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Two pulses of 17β-estradiol (10µg) are commonly used to increase hippocampal CA1 apical dendritic spine density and alter spatial performance in ovariectomized (OVX) female rats, but rarely are the measures combined. The goal of this study was to use this two-pulse injection protocol repeatedly with intervening wash-out periods in the same rats to: 1) measure spatial ability using different tasks that require hippocampal function and 2) determine whether ovarian hormone depletion for an extended 10-week period reduces 17β-estradiol's effectiveness in elevating CA1 apical dendritic spine density. Results showed that two injections of 10µg 17β-estradiol (72 and 48 hrs prior to testing and timed to maximize CA1 apical spine density at behavioral assessment) corresponded to improved spatial memory performance on object placement. In contrast, two injections of 5µg 17β-estradiol facilitated spatial learning on the water maze compared to rats given two injections of 10µg 17β-estradiol or the sesame oil vehicle. Neither 17β-estradiol dose altered Y-maze performance. As expected, the intermittent two-pulse injection protocol increased CA1 apical spine density, but ten weeks of OVX without estradiol treatment decreased the effectiveness of 10µg 17β-estradiol to increase CA1 apical spine density. Moreover, two pulses of 5µg 17β-estradiol injected intermittently failed to alter CA1 apical spine density and decreased basal spine density. These results demonstrate that extended time without ovarian hormones reduces 17β-estradiol's effectiveness to increase CA1 apical spine density. Collectively, these findings highlight the complex interactions among estradiol, CA1 spine density/morphology, and task requirements, all of which contribute to behavioral outcomes.

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“…Several lines of evidence indicate that prolonged elevation of glucocorticoid makes the hippocampus vulnerable to neurotoxic challenges (12,13). In addition to the finding that an acute treatment with TMT temporally increases the concentration of plasma corticosterone in rats (14), it has been demonstrated that a reduction in the level of circulating corticosterone by metyrapone, an inhibitor of corticosterone synthesis, prevents TMT from damaging the hippocampal neurons and eliciting learning impairment and hyperactivity in rats (15).…”

Section: Introductionmentioning

confidence: 99%

Endogenous and Exogenous Glucocorticoids Prevent Trimethyltin From Causing Neuronal Degeneration of the Mouse Brain In Vivo: Involvement of Oxidative Stress Pathways

et al. 2009

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Abstract. The organotin trimethyltin (TMT) is known to cause neuronal degeneration in the murine brain. Earlier studies indicate that TMT-induced neuronal degeneration is enhanced by adrenalectomy. However, no evaluation has been attempted to determine the mechanism underlying the enhancement of TMT neurotoxicity by adrenalectomy and its implications in neuronal degeneration. To assess the implications and determine the mechanism of adrenalectomyelicited enhancement of TMT neurotoxicity, we examined neuronal degeneration and associated signaling pathways in adrenalectomized mice. Adrenalectomy dramatically enhanced the TMTinduced neuronal damage in certain brain regions including the dentate gyrus, olfactory bulb, and anterior olfactory nucleus, in addition to exacerbating the behavioral abnormalities. TMTinduced activation of caspase-3 and calpain was also enhanced by adrenalectomy. The above events elicited by TMT were almost entirely prevented by treatment with dexamethasone. In addition to the above events, adrenalectomy clearly enhanced the activation of c-Jun-N-terminal kinases and the formation of 4-hydroxynonenal in the dentate gyrus following TMT treatment. The dentate granule cell damage induced by TMT was exacerbated by mifepristone, a glucocorticoid-receptor antagonist. Taken together, our data suggest that endogenous and exogenous glucocorticoids prevent neurodegeneration induced by TMT in the central nervous system by attenuating intensive oxidative stress and associated signaling pathways.

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Chronic Glucocorticoids Increase Hippocampal Vulnerability to Neurotoxicity under Conditions That Produce CA3 Dendritic Retraction But Fail to Impair Spatial Recognition Memory

Cited by 128 publications

References 41 publications

Vulnerability to Depression: From Brain Neuroplasticity to Identification of Biomarkers

Vulnerability to Depression: From Brain Neuroplasticity to Identification of Biomarkers

Assessment of estradiol influence on spatial tasks and hippocampal CA1 spines: Evidence that the duration of hormone deprivation after ovariectomy compromises 17β-estradiol effectiveness in altering CA1 spines

Endogenous and Exogenous Glucocorticoids Prevent Trimethyltin From Causing Neuronal Degeneration of the Mouse Brain In Vivo: Involvement of Oxidative Stress Pathways

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