Research article summary (published 18 Aug 2008):

The p75 neurotrophin receptor regulates hippocampal neurogenesis and related behaviours.

Full Abstract

Although changes to neural circuitry are believed to underlie behavioural characteristics mediated by the hippocampus, the contribution of neurogenesis to this process remains controversial. This is partially because the molecular regulators of neurogenesis remain to be fully elucidated, and experiments generically preventing neurogenesis have, for the most part, depended on paradigms involving irradiation. Here we show that mice lacking the p75 neurotrophin receptor (p75(NTR-/-)) have 25% fewer neuroblasts and 50% fewer newborn neurons in the dentate gyrus, coincident with increased rates of cell death of newly born cells and a significantly smaller granular cell layer and dentate gyrus, than those of p75(NTR+/+) mice. Whereas p75(NTR-/-) mice had increased latency to feed in a novelty-suppressed feeding paradigm they had increased mobility in another test of "depression", the tail-suspension test. p75(NTR-/-) mice also had subtle behavioural impairment in Morris water maze tasks compared to wild-type animals. No difference between genotypes was found in relation to anxiety or exploration behaviour based on the elevated-plus maze, light-dark, hole-board, T-maze or forced-swim tests. Overall, this study demonstrates that p75(NTR) is an important regulator of hippocampal neurogenesis, with concomitant effects on associated behaviours. However, the behavioural attributes of the p75(NTR-/-) mice may be better explained by altered circuitry driven by the loss of p75(NTR) in the basal forebrain, rather than direct changes to neurogenesis.

Author information

Author/s: Catts, Vibeke S (VS); Al-Menhali, Noura (N); Burne, Thomas H J (TH); Colditz, Michael J (MJ); Coulson, Elizabeth J (EJ);

Affiliation: Queensland Brain Institute, The University of Queensland, Brisbane, QLD, Australia.

Journal and publication information

Publication Type: Journal Article; Research Support, Non-U.S. Gov't

Journal: The European journal of neuroscience (Eur J Neurosci), published in France. (Language: eng)

Reference: 2008-Sep; vol 28 (issue 5) : pp 883-92

Dates: Created 2008/10/10; Completed 2009/03/05;

PMID: 18717734, status: MEDLINE (last retrieved date: 3/10/2009)

Sourced from the National Library of Medicine. Abstract text and other information may be subject to copyright.

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MeSH headings (categories)

This article was linked to the MeSH Headings (categories) shown below.

Animals Apoptosis - genetics Basal Nucleus of Meynert - metabolism; physiopathology Behavior, Animal - physiology Cell Count Cell Proliferation Cells, Cultured Dentate Gyrus - cytology; metabolism Depressive Disorder - genetics; metabolism Exploratory Behavior - physiology Hippocampus - cytology; metabolism

Male Maze Learning - physiology Mice Mice, Inbred C57BL Mice, Knockout Neural Pathways - metabolism; physiopathology Neurogenesis - physiology Neurons - cytology; metabolism Receptor, Nerve Growth Factor - genetics Spheroids, Cellular Stem Cells - metabolism

Note: Bold headings indicate primary MeSH headings or qualifiers.

Associated Chemicals: Receptor, Nerve Growth Factor (0)

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