dCREB2-mediated enhancement of memory formation

CREB-responsive transcription has an important role in adaptive responses in all cells and tissue. In the nervous system, it has an essential and well established role in long-term memory formation throughout a diverse set of organisms. Activation of this transcription factor correlates with long-te...

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Veröffentlicht in:The Journal of neuroscience 2013-04, Vol.33 (17), p.7475-7487
Hauptverfasser: Tubon, Jr, Thomas C, Zhang, Jiabin, Friedman, Eugenia L, Jin, Haining, Gonzales, Erin D, Zhou, Hong, Drier, Diana, Gerstner, Jason R, Paulson, Emily A, Fropf, Robin, Yin, Jerry C P
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Sprache:eng
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Zusammenfassung:CREB-responsive transcription has an important role in adaptive responses in all cells and tissue. In the nervous system, it has an essential and well established role in long-term memory formation throughout a diverse set of organisms. Activation of this transcription factor correlates with long-term memory formation and disruption of its activity interferes with this process. Most convincingly, augmenting CREB activity in a number of different systems enhances memory formation. In Drosophila, a sequence rearrangement in the original transgene used to enhance memory formation has been a source of confusion. This rearrangement prematurely terminates translation of the full-length protein, leaving the identity of the "enhancing molecule" unclear. In this report, we show that a naturally occurring, downstream, in-frame initiation codon is used to make a dCREB2 protein off of both transgenic and chromosomal substrates. This protein is a transcriptional activator and is responsible for memory enhancement. A number of parameters can affect enhancement, including the short-lived activity of the activator protein, and the time-of-day when induction and behavioral training occur. Our results reaffirm that overexpression of a dCREB2 activator can enhance memory formation and illustrate the complexity of this behavioral enhancement.
ISSN:0270-6474
1529-2401
1529-2401
DOI:10.1523/JNEUROSCI.4387-12.2013