Abstract
Neurogenesis is known to continuously take place in certain ‘neurogenic’ areas of the adult central nervous system (CNS) and can be induced in ‘non-neurogenic’ areas under traumatic or degenerative conditions. Here we introduce T cells and CNS-resident microglia as important players in the regulation of adult neurogenesis. Under normal conditions, immune deficient mice (SCID and nude) and transgenic mice that most of their T-cell pool is specific for an irrelevant antigen (ovalbumin) exhibited impaired hippocampal neurogenesis. In contrast, mice in which the majority of T cells specifically recognize the CNSabundant antigen myelin basic protein showed normal neurogenesis. CNSspecific T cells were also found to be important for spatial learning abilities and for brain-derived neurotrophic factor expression in the dentate gyrus. Environmental enrichment did not evoke enhanced neurogenesis in immune-deficient animals, whereas in wild-type animals it led to enhanced hippocampal neurogenesis coupled with recruitment of T cells and activation of microglia. The clinical implications of these findings were tested using a rat model of cerebral ischemic insult. We demonstrate that Tcell based immune activation following stroke induces a robust elevation of neurogenesis in the hippocampus as well as in the cerebral cortex. Our results suggest that T cells, acting via resident antigen presenting cells, are important regulators of adult neurogenesis under both physiological and pathological conditions.
Original language | English |
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Pages | 387-391 |
Number of pages | 5 |
Publication status | Published - Sept 2006 |
Event | 8th International Congress of Neuroimmunology - Nagoya, Japan Duration: 15 Oct 2006 → 19 Oct 2006 Conference number: 8th |
Conference
Conference | 8th International Congress of Neuroimmunology |
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Country/Territory | Japan |
City | Nagoya |
Period | 15/10/06 → 19/10/06 |