[cid:image001.jpg@01D158FE.B69B8D00] SPECIAL LECTURE: B R A I N A W A R E N E S S W E E K
D A T E Wednesday, March 14th, 2018 12Noon *Followed by a Trainee Lunch in SR415, KIAM
L O C A T I O N Theatre C, BMSB
S P E A K E R D R . PIERRE MARQUET C A N A D A EXCELLENCE R E S E A R C H C H A I R NEUROPHOTONICS
T O P I C Neurophotonics to Intercept the Emergence of Major Psychiatric Disorders
Major psychiatric disorders (MPDs) including psychosis and mood disorders affect *4% of the population. MPDs have chronic courses since their diagnoses, solely based on clinical symptoms, are very late and thus better treatments are only palliative. The successful development of early treatment and primary prevention is largely impeded by the lack of reliable risk biomarkers or endophenotypes (B/Es). This is a critical issue since MPDs have a neurodevelopmental origin and early intervention can improve outcomes.
From a developmental standpoint, the identification of B/Es in patients with MPDs and in their offspring at genetic risk will play a pivotal role in the definition of childhood risk syndromes and their corresponding abnormal trajectories. This approach is particularly relevant given that high-risk children carry many of the indicators of brain dysfunctions that adult patients have.
Within this framework, I will present how the development of new multimodal optical imaging techniques in combination with stem cell technologies, including human induced pluripotent stem cells approaches, can contribute to identifying new cellular B/Es relevant both to define childhood risk syndromes and to determine cellular processes likely to be involved in the pathogenesis of these MPDs.
Kae Normandeau Administrative Manager Neuroscience Research Program
SR440 KIAM Building P: 204-318-2569 E: kae.normandeau@umanitoba.camailto:kae.normandeau@umanitoba.ca
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