A loss-of-function study of CRTC1 in hippocampal neurons at basal state and during long-term synaptic plasticity
Encoding of long-term memory in neurons requires gene expression and protein synthesis. CREB, a well-characterised stimulus-induced transcription factor, is implicated in gene transcription supporting long-term plasticity. Several studies showed that CRTC1 is an important co-activator for CREB ac...
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| Format: | Theses and Dissertations |
| Language: | English |
| Published: |
2019
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| Subjects: | |
| Online Access: | https://hdl.handle.net/10356/85237 http://hdl.handle.net/10220/49191 |
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| Institution: | Nanyang Technological University |
| Language: | English |
| Summary: | Encoding of long-term memory in neurons requires gene expression and protein
synthesis. CREB, a well-characterised stimulus-induced transcription factor, is
implicated in gene transcription supporting long-term plasticity. Several studies showed
that CRTC1 is an important co-activator for CREB activity. Although CRTC1 is most
abundantly expressed in the brain, its function during memory formation remains poorly
understood. Studies have revealed that CRTC1 could modulate long-term plasticity in
the hippocampus, but extensive use of a conditional deletion strategy has never been
performed. Hence, the overall aim of this project is to rigorously examine the impact of
nuclear CRTC1 translocation and transcription in regulating long-term memories. We
investigated the role of CRTC1 in hippocampal neurons by knocking out CRTC1
protein expression using the lentiCRISPR/Cas9 system that we established. Our results
indicate that basal loss of CRTC1 reduced the number of inhibitory synaptic protein
expression in hippocampal neurons, therefore leading to enhanced action potential firing
and reduced mIPSCs. We report that the loss of excitatory synaptic protein expression
only occurred in bicuculline-stimulated cultures. We also show that chemically-induced
long-term potentiation and depression triggered CRTC1 nuclear accumulation in
hippocampal neurons. During long-term plasticity, loss of CRTC1 perturbed the overall
transcription of several CREB-mediated immediate early genes. In particular, the
expression of an important regulator of excitatory-inhibitory balance in the hippocampal
neurons, Npas4, is reduced. Hence, we speculate that CRTC1 is crucial for the
regulation of multiple CREB-mediated target gene transcription, including Npas4 and
that loss of Npas4 expression perhaps contributes to the reduction in inhibition. |
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