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Publication : Forebrain CRF₁ modulates early-life stress-programmed cognitive deficits.

First Author  Wang XD Year  2011
Journal  J Neurosci Volume  31
Issue  38 Pages  13625-34
PubMed ID  21940453 Mgi Jnum  J:177121
Mgi Id  MGI:5294262 Doi  10.1523/JNEUROSCI.2259-11.2011
Citation  Wang XD, et al. (2011) Forebrain CRF modulates early-life stress-programmed cognitive deficits. J Neurosci 31(38):13625-34
abstractText  Childhood traumatic events hamper the development of the hippocampus and impair declarative memory in susceptible individuals. Persistent elevations of hippocampal corticotropin-releasing factor (CRF), acting through CRF receptor 1 (CRF), in experimental models of early-life stress have suggested a role for this endogenous stress hormone in the resulting structural modifications and cognitive dysfunction. However, direct testing of this possibility has been difficult. In the current study, we subjected conditional forebrain CRF knock-out (CRF-CKO) mice to an impoverished postnatal environment and examined the role of forebrain CRF in the long-lasting effects of early-life stress on learning and memory. Early-life stress impaired spatial learning and memory in wild-type mice, and postnatal forebrain CRF overexpression reproduced these deleterious effects. Cognitive deficits in stressed wild-type mice were associated with disrupted long-term potentiation (LTP) and a reduced number of dendritic spines in area CA3 but not in CA1. Forebrain CRF deficiency restored cognitive function, LTP and spine density in area CA3, and augmented CA1 LTP and spine density in stressed mice. In addition, early-life stress differentially regulated the amount of hippocampal excitatory and inhibitory synapses in wild-type and CRF-CKO mice, accompanied by alterations in the neurexin-neuroligin complex. These data suggest that the functional, structural and molecular changes evoked by early-life stress are at least partly dependent on persistent forebrain CRF signaling, providing a molecular target for the prevention of cognitive deficits in adults with a history of early-life adversity.
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