Abstract

Over the last 15 years, several laboratories, including my laboratory, have identified multiple signaling pathways that regulate translation via the translation initiation factors eIF4E and eIF2? during protein synthesis-dependent forms of long-lasting synaptic plasticity and various memory processes in rodents, including the consolidation, reconsolidation, and extinction of auditory threat memory. These findings have generated much excitement because they demonstrate the complex biochemical regulation of translation during synaptic plasticity and memory. Despite this progress, a number of critical and unresolved questions regarding the requirement for de novo protein synthesis in memory consolidation remain unanswered. We plan to focus on auditory threat memory in the amygdala and address three new questions that are critical for a more complete understanding of the role of de novo protein synthesis in memory formation. First, which cell types in the lateral amygdala (LA) and centrolateral (CeL) amygdala require eIF4E-dependent translation for auditory threat memory? Second, which cell types in the LA and CeL require eIF2?-dependent translation for the consolidation and reconsolidation of auditory threat memory? Third, does auditory threat learning induce cell type-specific translation profiles in the LA and CeL? These questions will be addressed by utilizing the powerful multidisciplinary combination of new groundbreaking genetically-engineered mice, electrophysiological recordings, immunocytochemistry, innovative methods to measure de novo protein synthesis in vivo, and cell-type translational profiling. The results of these studies will provide fundamental insights into the molecular events in both excitatory and inhibitory neurons that support consolidation and reconsolidation of auditory threat memory. Moreover, these studies have the potential to provide cell type-specific therapeutic targets for multiple brain disorders that are associated with dysregulated translation.

Public Health Relevance

Previous studies have identified the signaling pathways that couple receptors to the translation machinery to regulate protein synthesis during long-lasting synaptic plasticity and long-term memory formation, and several of these translational control pathways are dysregulated in brain disorders including Alzheimer's disease, fragile X syndrome, and autism spectrum disorder. Herein we propose studies using new mouse lines that we have developed to determine the specific cell types in the amygdala that require de novo protein synthesis for the consolidation of threat memory and to identify the mRNAs that are translationally regulated in these cells. Our studies should provide insight into the cell type-specific role of de novo protein synthesis in threat memory consolidation and have the potential to identify new therapeutic targets for disorders associated with dysregulated protein synthesis.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS047384-15
Application #
9955336
Study Section
Special Emphasis Panel (ZRG1)
Program Officer
Mamounas, Laura
Project Start
2005-07-01
Project End
2023-05-31
Budget Start
2020-06-01
Budget End
2021-05-31
Support Year
15
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
New York University
Department
Neurosciences
Type
Schools of Arts and Sciences
DUNS #
041968306
City
New York
State
NY
Country
United States
Zip Code
10012

  Publications

Huynh, T N; Santini, E; Mojica, E et al. (2018) Activation of a novel p70 S6 kinase 1-dependent intracellular cascade in the basolateral nucleus of the amygdala is required for the acquisition of extinction memory. Mol Psychiatry 23:1394-1401
Santini, Emanuela; Huynh, Thu N; Longo, Francesco et al. (2017) Reducing eIF4E-eIF4G interactions restores the balance between protein synthesis and actin dynamics in fragile X syndrome model mice. Sci Signal 10:
Ostroff, Linnaea E; Botsford, Benjamin; Gindina, Sofya et al. (2017) Accumulation of Polyribosomes in Dendritic Spine Heads, But Not Bases and Necks, during Memory Consolidation Depends on Cap-Dependent Translation Initiation. J Neurosci 37:1862-1872
Oaks, Adam W; Zamarbide, Marta; Tambunan, Dimira E et al. (2017) Cc2d1a Loss of Function Disrupts Functional and Morphological Development in Forebrain Neurons Leading to Cognitive and Social Deficits. Cereb Cortex 27:1670-1685
Bowling, Heather; Bhattacharya, Aditi; Klann, Eric et al. (2016) Deconstructing brain-derived neurotrophic factor actions in adult brain circuits to bridge an existing informational gap in neuro-cell biology. Neural Regen Res 11:363-7
Bhattacharya, Aditi; Mamcarz, Maggie; Mullins, Caitlin et al. (2016) Targeting Translation Control with p70 S6 Kinase 1 Inhibitors to Reverse Phenotypes in Fragile X Syndrome Mice. Neuropsychopharmacology 41:1991-2000
Bowling, Heather; Bhattacharya, Aditi; Zhang, Guoan et al. (2016) BONLAC: A combinatorial proteomic technique to measure stimulus-induced translational profiles in brain slices. Neuropharmacology 100:76-89
Sethna, Ferzin; Zhang, Ming; Kaphzan, Hanoch et al. (2016) Calmodulin activity regulates group I metabotropic glutamate receptor-mediated signal transduction and synaptic depression. J Neurosci Res 94:401-8
Richter, Joel D; Bassell, Gary J; Klann, Eric (2015) Dysregulation and restoration of translational homeostasis in fragile X syndrome. Nat Rev Neurosci 16:595-605
Huynh, Thu N; Shah, Manan; Koo, So Yeon et al. (2015) eIF4E/Fmr1 double mutant mice display cognitive impairment in addition to ASD-like behaviors. Neurobiol Dis 83:67-74

Showing the most recent 10 out of 71 publications