Social isolation disrupts hippocampal neurogenesis in young non-human primates

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Abstract

Social relationships are crucial for the development and maintenance of normal behavior in non-human primates. Animals that are raised in isolation develop abnormal patterns of behavior that persist even when they are later reunited with their parents. In rodents, social isolation is a stressful event and is associated with a decrease in hippocampal neurogenesis but considerably less is known about the effects of social isolation in non-human primates during the transition from adolescence to adulthood. To investigate how social isolation affects young marmosets, these were isolated from other members of the colony for 1 or 3 weeks and evaluated for alterations in their behavior and hippocampal cell proliferation. We found that anxiety-related behaviors like scent-marking and locomotor activity increased after social isolation when compared to baseline levels. In agreement, grooming-an indicative of attenuation of tension-was reduced among isolated marmosets. These results were consistent with increased cortisol levels after 1 and 3 weeks of isolation. After social isolation (1 or 3 weeks), reduced proliferation of neural cells in the subgranular zone of dentate granule cell layer was identified and a smaller proportion of BrdU-positive cells underwent neuronal fate (doublecortin labeling). Our data is consistent with the notion that social deprivation during the transition from adolescence to adulthood leads to stress and produces anxiety-like behaviors that in turn might affect neurogenesis and contribute to the deleterious consequences of prolonged stressful conditions. © 2014 Cinini, Barnabe, Galvão-Coelho, de Medeiros, Perez-Mendes, Sousa, Covolan and Mello.

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Cinini, S. M., Barnabe, G. F., Galvão-Coelho, N., de Medeiros, M. A., Perez-Mendes, P., Sousa, M. B. C., … Mello, L. E. (2014). Social isolation disrupts hippocampal neurogenesis in young non-human primates. Frontiers in Neuroscience, (8 MAR). https://doi.org/10.3389/fnins.2014.00045

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