Treating Schizophrenia by Correcting Abnormal Brain Development

Information

PI Name

T.-U. Wilson Woo, M.D., Ph.D.

PI Location

Beth Israel Deaconess Medical Center, Harvard Medical School

Protocol Type

Interventional

Conditions

schizophrenia

Age

Adult

Gender

All

Recruitment Status

Active, not recruiting

Phase

Phase 3

ClinicalTrials.Gov Identifier

NCT00179465

Last Update Posted on Clintrials.gov

06/07/2023

Study First Posted

09/16/2005

Collaborators

Dartmouth-Hitchcock Medical Center

Organization

Beth Israel Deaconess Medical Center

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Description

It is hypothesized that enhancement of GABA neurotransmission during the early course of the illness by tiagabine (Gabitril), a GABA transporter GAT-1-specific inhibitor and a FDA-approved anticonvulsant, will improve both clinical symptoms and working memory in schizophrenia. This improvement is postulated to be the result of tiagabine-mediated modification of the developmental synaptic pruning of prefrontal cortical circuitry. The occurrence of circuitry modification after tiagabine treatment will be assessed by the following independent methodologic approaches: MRI morphometric analysis of prefrontal gray matter volume and fMRI measurements of brain activity patterns during performance of tasks that probe working memory.

Treating Schizophrenia by Correcting Abnormal Brain Development

Treating Schizophrenia by Correcting Abnormal Brain Development

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