On 28th November OxTalks will move to the new Halo platform and will become 'Oxford Events' (full details are available on the Staff Gateway).
There will be an OxTalks freeze beginning on Friday 14th November. This means you will need to publish any of your known events to OxTalks by then as there will be no facility to publish or edit events in that fortnight. During the freeze, all events will be migrated to the new Oxford Events site. It will still be possible to view events on OxTalks during this time.
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New approaches that bridge knowledge across genes and proteins to cells to whole-brain networks and to behaviour are beginning to transform our understanding of how the brain works in health and disease.
Translation of neuroimaging results depend on this mechanistic understanding and is critical for discovery of new druggable targets. This talk will provide an overview of recent work using our lab combining multimodal brain imaging methods to ask questions about the interactions between neurochemistry, neurophysiology and neuroanatomy in psychosis vulnerability, with a ficus on brain excitation-inhibition balance.
I will discuss our recent research using preclinical models and bioinformatic approaches to delineate with increased precision the biological mechanisms involved in the human neuroimaging observations. We also apply experimental medicine approaches to probe how to intervene on those mechanisms early to prevent or delay the development of psychosis.
Finally, and in parallel, we work to integrate this mechanistic understanding with large-scale approaches to neuroimaging data (ENIGMA Schizotypy) and real-world clinical outcomes using electronic health records.