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Annotation


Ziv Y, Ron N, Butovsky O, Landa G, Sudai E, Greenberg N, Cohen H, Kipnis J, Schwartz M. Immune cells contribute to the maintenance of neurogenesis and spatial learning abilities in adulthood. Nat Neurosci. 2006 Feb;9(2):268-75. PubMed Abstract

  
Comments on Paper and Primary News
  Primary News: Do Kinder, Gentler T Cells Promote Neurogenesis?

Comment by:  Joanna Jankowsky
Submitted 21 January 2006  |  Permalink Posted 21 January 2006

The paper by Ziv et al. brings together two often disparate fields of study: immunology and neuroscience. The group of Michal Schwartz is one of a relatively few in the world who draws on tools of both trades to study how the immune and nervous systems intersect to influence brain function.

The authors propose the interesting hypothesis that the hippocampal (and olfactory) neurogenesis required for optimal functioning of the adult brain is dependent on cues from peripheral immune cells. It had been shown previously that inflammatory activation of the peripheral immune system can diminish neurogenesis in the brain. This work suggests that the converse, that is, that neurogenesis depends in some way on immune support, may also hold true.

The authors' use of SCID and nude mice for these studies is quite innovative, and the experiments carefully control for differences in genetic background that are known to influence adult neurogenesis. The decrement in BrdU+ cells, and specifically BrdU/DCX and BrdU/NeuN cells, in the immune-deficient mice is consistent with their...  Read more


  Primary News: Do Kinder, Gentler T Cells Promote Neurogenesis?

Comment by:  Teresita Briones
Submitted 23 January 2006  |  Permalink Posted 23 January 2006

Excellent article, and studies done were well-controlled. This article provides further validation of the communication between the central nervous system and the immune system. In this article, the authors showed that T cells (of the immune system) that reside in the central nervous system (CNS) can influence both neurogenesis and cognitive functioning independently. Under normal conditions, the resident T cells and microglia in the CNS are barely detectable, but when neurogenesis was enhanced by housing rats in an enriched environment, both T cells and microglia were activated. When neurogenesis was examined in mutant mice deficient in T cells, the authors found that neurogenesis was decreased compared to the control mice. It is interesting that even when the mutant mice were housed in the enriched environment, this did not help in increasing neurogenesis, as is usually seen in normal animals. However, when the mutant mice were injected with "splenocytes" containing replenished T cells, increased neurogenesis was seen when compared to mice depleted for T cells. Furthermore, the...  Read more

  Comment by:  Matthew During (Disclosure)
Submitted 1 February 2006  |  Permalink Posted 1 February 2006

This paper supports the general theory of bidirectional and tight communication between the nervous and immune systems. Microglia as components of both organ systems are critical players, presumably translating the T cell presence into a phenotype associated with increased cell proliferation and improved memory. Potential mediators include microglial IGF-1, and neuronally derived BDNF. The use of immune-deficient mouse models, both SCID and nude, coupled with the T cell adoptive transfer experiments and the T/MBP transgenic mouse provides in my mind pretty compelling evidence that brain-directed T cells facilitate neurogenesis and also improve hippocampal function as tested by a standard hippocampal-dependent behavioral task.

This study is also significant because it raises some interesting possibilities for neurodegenerative disorders in addition to the role of the immune system in maintaining "normal" brain function. One intriguing question is whether the brain, during enrichment, expresses signaling or trophic molecules that induce the trafficking of brain-specific T cells...  Read more

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