Literature DB >> 17726225

Blockage of VIP during mouse embryogenesis modifies adult behavior and results in permanent changes in brain chemistry.

Joanna M Hill1, Janet M Hauser, Lia M Sheppard, Daniel Abebe, Irit Spivak-Pohis, Michal Kushnir, Iris Deitch, Illana Gozes.   

Abstract

Vasoactive intestinal peptide (VIP) regulates growth and development during the early postimplantation period of mouse embryogenesis. Blockage of VIP with a VIP antagonist during this period results in growth restriction, microcephaly, and developmental delays. Similar treatment of neonatal rodents also causes developmental delays and impaired diurnal rhythms, and the adult brains of these animals exhibit neuronal dystrophy and increased VIP binding. These data suggest that blockage of VIP during the development of the nervous system can result in permanent changes to the brain. In the current study, pregnant mice were treated with a VIP antagonist during embryonic days 8 through 10. The adult male offspring were examined in tests of novelty, paired activity, and social recognition. Brain tissue was examined for several measures of chemistry and gene expression of VIP and related compounds. Glial cells from the cortex of treated newborn mice were plated with neurons and examined for VIP binding and their ability to enhance neuronal survival. Treated adult male mice exhibited increased anxiety-like behavior and deficits in social behavior. Brain tissue exhibited regionally specific changes in VIP chemistry and a trend toward increased gene expression of VIP and related compounds that reached statistical significance in the VIP receptor, VPAC-1, in the female cortex. When compared to control astrocytes, astrocytes from treated cerebral cortex produced further increases in neuronal survival with excess synaptic connections and reduced VIP binding. In conclusion, impaired VIP activity during mouse embryogenesis resulted in permanent changes to both adult brain chemistry/cell biology and behavior with aspects of autism-like social deficits.

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Year:  2007        PMID: 17726225     DOI: 10.1385/jmn:31:03:185

Source DB:  PubMed          Journal:  J Mol Neurosci        ISSN: 0895-8696            Impact factor:   3.444


  101 in total

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2.  An antagonist to vasoactive intestinal peptide affects cellular functions in the central nervous system.

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Journal:  Neuroendocrinology       Date:  1988-01       Impact factor: 4.914

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Authors:  I Gozes; G Lilling; R Glazer; A Ticher; I E Ashkenazi; A Davidson; S Rubinraut; M Fridkin; D E Brenneman
Journal:  J Pharmacol Exp Ther       Date:  1995-04       Impact factor: 4.030

Review 6.  Preliminary characterization of the central nervous system in partial trisomy 16 mice.

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8.  Behavioral alterations in rats prenatally exposed to valproic acid: animal model of autism.

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Authors:  H Werner; Y Koch; M Fridkin; J Fahrenkrug; I Gozes
Journal:  Biochem Biophys Res Commun       Date:  1985-11-27       Impact factor: 3.575

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Review 3.  Chemical modification of class II G protein-coupled receptor ligands: frontiers in the development of peptide analogs as neuroendocrine pharmacological therapies.

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7.  Regardless of genotype, offspring of VIP-deficient female mice exhibit developmental delays and deficits in social behavior.

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