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Cell cycle restriction by histone H2AX limits proliferation of adult neural stem cells.


ABSTRACT: Adult neural stem cell proliferation is dynamic and has the potential for massive self-renewal yet undergoes limited cell division in vivo. Here, we report an epigenetic mechanism regulating proliferation and self-renewal. The recruitment of the PI3K-related kinase signaling pathway and histone H2AX phosphorylation following GABA(A) receptor activation limits subventricular zone proliferation. As a result, NSC self-renewal and niche size is dynamic and can be directly modulated in both directions pharmacologically or by genetically targeting H2AX activation. Surprisingly, changes in proliferation have long-lasting consequences on stem cell numbers, niche size, and neuronal output. These results establish a mechanism that continuously limits proliferation and demonstrates its impact on adult neurogenesis. Such homeostatic suppression of NSC proliferation may contribute to the limited self-repair capacity of the damaged brain.

SUBMITTER: Fernando RN 

PROVIDER: S-EPMC3078396 | biostudies-literature | 2011 Apr

REPOSITORIES: biostudies-literature

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Cell cycle restriction by histone H2AX limits proliferation of adult neural stem cells.

Fernando Ruani N RN   Eleuteri Boris B   Abdelhady Shaimaa S   Nussenzweig Andre A   Andäng Michael M   Ernfors Patrik P  

Proceedings of the National Academy of Sciences of the United States of America 20110321 14


Adult neural stem cell proliferation is dynamic and has the potential for massive self-renewal yet undergoes limited cell division in vivo. Here, we report an epigenetic mechanism regulating proliferation and self-renewal. The recruitment of the PI3K-related kinase signaling pathway and histone H2AX phosphorylation following GABA(A) receptor activation limits subventricular zone proliferation. As a result, NSC self-renewal and niche size is dynamic and can be directly modulated in both direction  ...[more]

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