Correction of Long-Lasting Negative Effects of Neonatal Isolation in White Rats Using Semax

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Abstract

Adverse experience during the early postnatal period induces negative alterations in physiological and neurobiological functions, resulting in long-term disorder in animal behavior. The aim of the present work was to study the long-lasting effects of chronic neonatal stress in white rats and to estimate the possibility of their correction using Semax, an analogue of ACTH fragment (4-10). Early neonatal isolation was used as a model of early-life stress. Rat pups were separated from their mothers and littermates for 5 h daily during postnatal days 1-14. The pups of the control group were left undisturbed with the dams. Half of the rats subjected to neonatal isolation received an intranasal injection of Semax at a dose of 50 μg/kg daily, from postnatal day 15 until day 28. The other animals received intranasal vehicle injections daily at the same time points. It was shown that neonatal isolation leads to a delay in physical development, metabolic disturbances, and a decrease in the corticosterone stress response in white rats. These changes were observed during the first two months of life. Semax administration weakened the influence of neonatal isolation on the animals, body weight , reduced metabolic dysfunction, and led to an increase in stress-induced corticosterone release to the control values. So the chronic intranasal administration of Semax after termination of the neonatal isolation procedure diminishes the negative effects of neonatal stress.

About the authors

M. A. Volodina

Lomonosov Moscow State University

Email: nglevitskaya@gmail.com
Russian Federation

E. A. Sebentsova

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

N. Yu. Glazova

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

D. M. Manchenko

Lomonosov Moscow State University

Email: nglevitskaya@gmail.com
Russian Federation

L. S. Inozemtseva

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

O. V. Dolotov

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

L. A. Andreeva

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

N. G. Levitskaya

Institute of Molecular Genetics, Russian Academy of Sciences

Author for correspondence.
Email: nglevitskaya@gmail.com
Russian Federation

A. A. Kamensky

Lomonosov Moscow State University

Email: nglevitskaya@gmail.com
Russian Federation

N. F. Myasoedov

Institute of Molecular Genetics, Russian Academy of Sciences

Email: nglevitskaya@gmail.com
Russian Federation

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Copyright (c) 2012 Volodina M.A., Sebentsova E.A., Glazova N.Y., Manchenko D.M., Inozemtseva L.S., Dolotov O.V., Andreeva L.A., Levitskaya N.G., Kamensky A.A., Myasoedov N.F.

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