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PKA-activated ApAF–ApC/EBP heterodimer is a key downstream effector of ApCREB and is necessary and sufficient for the consolidation of long-term facilitation

Authors :
Deok-Jin Chang
Bong-Kiun Kaang
Yong Lee
Sue-Hyun Lee
Hyoung F. Kim
Yongseok Lee
Ye-Hwang Cheang
Dusan Bartsch
Heejung Jun
Eric R. Kandel
Hyoung-Gon Ko
Jin-A Lee
Changhoon Lee
Source :
The Journal of Cell Biology
Publication Year :
2006
Publisher :
Rockefeller University Press, 2006.

Abstract

Long-term memory requires transcriptional regulation by a combination of positive and negative transcription factors. Aplysia activating factor (ApAF) is known to be a positive transcription factor that forms heterodimers with ApC/EBP and ApCREB2. How these heterodimers are regulated and how they participate in the consolidation of long-term facilitation (LTF) has not, however, been characterized. We found that the functional activation of ApAF required phosphorylation of ApAF by PKA on Ser-266. In addition, ApAF lowered the threshold of LTF by forming a heterodimer with ApCREB2. Moreover, once activated by PKA, the ApAF–ApC/EBP heterodimer transactivates enhancer response element–containing genes and can induce LTF in the absence of CRE- and CREB-mediated gene expression. Collectively, these results suggest that PKA-activated ApAF–ApC/EBP heterodimer is a core downstream effector of ApCREB in the consolidation of LTF.

Details

ISSN :
15408140 and 00219525
Volume :
174
Database :
OpenAIRE
Journal :
Journal of Cell Biology
Accession number :
edsair.doi.dedup.....67158b269feae9aeecfcd0080035bfb5