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

Jin A. Lee; Sue Hyun Lee; Changhoon Lee; Deok Jin Chang; Yong Lee; Hyoung Kim; Ye Hwang Cheang; Hyoung Gon Ko; Yong Seok Lee; Heejung Jun; Dusan Bartsch; Eric R. Kandel; Bong Kiun Kaang

doi:10.1083/jcb.200512066

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

Jin A. Lee, Sue Hyun Lee, Changhoon Lee, Deok Jin Chang, Yong Lee, Hyoung Kim, Ye Hwang Cheang, Hyoung Gon Ko, Yong Seok Lee, Heejung Jun, Dusan Bartsch, Eric R. Kandel, Bong Kiun Kaang

Research output: Contribution to journal › Article › peer-review

19 Scopus citations

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.

Original language	English (US)
Pages (from-to)	827-838
Number of pages	12
Journal	Journal of Cell Biology
Volume	174
Issue number	6
DOIs	https://doi.org/10.1083/jcb.200512066
State	Published - Sep 11 2006
Externally published	Yes

ASJC Scopus subject areas

Cell Biology

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Lee, J. A., Lee, S. H., Lee, C., Chang, D. J., Lee, Y., Kim, H., Cheang, Y. H., Ko, H. G., Lee, Y. S., Jun, H., Bartsch, D., Kandel, E. R., & Kaang, B. K. (2006). 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. Journal of Cell Biology, 174(6), 827-838. https://doi.org/10.1083/jcb.200512066

Lee, JA, Lee, SH, Lee, C, Chang, DJ, Lee, Y, Kim, H, Cheang, YH, Ko, HG, Lee, YS, Jun, H, Bartsch, D, Kandel, ER & Kaang, BK 2006, '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', Journal of Cell Biology, vol. 174, no. 6, pp. 827-838. https://doi.org/10.1083/jcb.200512066

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title = "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",

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.",

author = "Lee, {Jin A.} and Lee, {Sue Hyun} and Changhoon Lee and Chang, {Deok Jin} and Yong Lee and Hyoung Kim and Cheang, {Ye Hwang} and Ko, {Hyoung Gon} and Lee, {Yong Seok} and Heejung Jun and Dusan Bartsch and Kandel, {Eric R.} and Kaang, {Bong Kiun}",

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AU - Lee, Jin A.

AU - Lee, Sue Hyun

AU - Lee, Changhoon

AU - Chang, Deok Jin

AU - Lee, Yong

AU - Kim, Hyoung

AU - Cheang, Ye Hwang

AU - Ko, Hyoung Gon

AU - Lee, Yong Seok

AU - Jun, Heejung

AU - Bartsch, Dusan

AU - Kandel, Eric R.

AU - Kaang, Bong Kiun

PY - 2006/9/11

Y1 - 2006/9/11

N2 - 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.

AB - 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.

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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

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