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Publication : Selective deletion of the oxytocin gene remodels the number and shape of dendritic spines in the medial amygdala of males with and without sexual experience.

First Author  Becker RO Year  2017
Journal  Neurosci Lett Volume  660
Pages  155-159 PubMed ID  28889007
Mgi Jnum  J:250589 Mgi Id  MGI:5925123
Doi  10.1016/j.neulet.2017.08.075 Citation  Becker RO, et al. (2017) Selective deletion of the oxytocin gene remodels the number and shape of dendritic spines in the medial amygdala of males with and without sexual experience. Neurosci Lett 660:155-159
abstractText  Oxytocin has central actions that modulate synaptic plasticity and the occurrence of social behavior in rodents. The posterodorsal medial amygdala (MePD) composes a sexually dimorphic neural circuit for the display of male sexual behavior. Local dendritic spines are notably plastic and affected by context-dependent social stimuli. Here, we examined the effects of the selective deletion of the OT gene (OTKO) in the number and shape of Golgi-impregnated dendritic spines in the MePD of naive and sexually experienced (SexExp) male mice (n=6 each group). Compared to the control wild-type mice (WT), OTKO naive mice did not differ in the density of dendritic spines, but there was a significant and more intense reduction in the number of spines in the WT/SexExp ( approximately 40%) than in the OTKO/SexExp ( approximately 25%). This structural change had a spine-specific feature. That is, sexual experience induced a decrease in the number of thin ( approximately 50%) and mushroom-like spines ( approximately 35%) at the same time that increased ( approximately 30%) the number of stubby/wide spines. In addition, the OTKO/SexExp animals have more thin and mushroom spines than the WT/SexExp ones ( approximately 25% and 55%, respectively; p <0.01 in all cases). In conjunction, these novel data indicate that OT participates in the spine remodeling, synaptic refinement, and social stimuli-dependent plasticity in the MePD of male mice.
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