Chromatin plasticity predetermines neuronal eligibility for memory trace formation.
Giulia SantoniSimone AstoriMarion LeleuLiliane GlauserSimon A ZamoraMyriam SchioppaIsabella TarulliCarmen SandiJohannes GräffPublished in: Science (New York, N.Y.) (2024)
Memories are encoded by sparse populations of neurons but how such sparsity arises remains largely unknown. We found that a neuron's eligibility to be recruited into the memory trace depends on its epigenetic state prior to encoding. Principal neurons in the mouse lateral amygdala display intrinsic chromatin plasticity, which when experimentally elevated favors neuronal allocation into the encoding ensemble. Such chromatin plasticity occurred at genomic regions underlying synaptic plasticity and was accompanied by increased neuronal excitability in single neurons in real time. Lastly, optogenetic silencing of the epigenetically altered neurons prevented memory expression, revealing a cell-autonomous relationship between chromatin plasticity and memory trace formation. These results identify the epigenetic state of a neuron as a key factor enabling information encoding.
Keyphrases
- gene expression
- dna damage
- spinal cord
- working memory
- transcription factor
- genome wide
- dna methylation
- heavy metals
- poor prognosis
- cerebral ischemia
- healthcare
- minimally invasive
- machine learning
- oxidative stress
- stem cells
- functional connectivity
- bone marrow
- brain injury
- convolutional neural network
- social media
- subarachnoid hemorrhage