24 October 2025, 11:00
Memory aids on the chromatin – Epigenetic mechanisms of memory encoding
24 October 20252025External Faculty SpeakerEMBL Rome
AbstractMemory formation relies on a bidirectional interplay between synaptic plasticity and nucleus templated transcriptional programs but how precisely this interplay is orchestrated by epigenetic mechanisms remains to a large extent unknown In this talk I will showcase our recent efforts to better understand this aspect from two angles First we have found that chromatin plasticity in the... AbstractMemory formation relies on a bidirectional interplay between synaptic plasticity and nucleus-templated transcriptional programs, but how precisely this interplay is orchestrated by epigenetic mechanisms remains to a large extent unknown. In this talk, I will showcase our recent efforts to better understand this aspect from two angles. First, we have found that chromatin plasticity in the mouse brain is a key determinant for memory allocation, the process by which neurons become recruited into the memory trace: When we increased chromatin plasticity by enzymatic overexpression of histone acetyl transferases (HATs), neurons with elevated histone acetylation were preferentially recruited into the encoding ensemble and memory retention was enhanced, while optogenetic silencing of the epigenetically altered neurons prevented memory expression. Second, we have found that after...
Speaker(s): Johannes Graff, École Polytechnique Fédérale de Lausanne (EPFL), Switzerland
Place: Conf Room/Building 14
External Faculty Speaker
EMBL Rome
Additional information
Abstract
Memory formation relies on a bidirectional interplay between synaptic plasticity and nucleus-templated transcriptional programs, but how precisely this interplay is orchestrated by epigenetic mechanisms remains to a large extent unknown. In this talk, I will showcase our recent efforts to better understand this aspect from two angles. First, we have found that chromatin plasticity in the mouse brain is a key determinant for memory allocation, the process by which neurons become recruited into the memory trace: When we increased chromatin plasticity by enzymatic overexpression of histone acetyl transferases (HATs), neurons with elevated histone acetylation were preferentially recruited into the encoding ensemble and memory retention was enhanced, while optogenetic silencing of the epigenetically altered neurons prevented memory expression. Second, we have found that after learning, the epigenetic make-up of a single locus in the encoding ensemble is necessary and sufficient to bidirectionally alter memory performance across different phases of memory consolidation. Together, these findings stipulate that before and after memory encoding, epigenetic mechanisms play a pivotal role as molecular memory aids.