Fragile X Syndrome Clinical Trial
Official title:
Add-on Pilot Trial of Minocycline in Fragile X Syndrome
Fragile X Syndrome (FXS) is the most common known inherited form of mental impairment, developmental disability and autism. Minocycline is an antibiotic that has recently been used to treat the mouse model for Fragile X, and was found to reverse the structural abnormalities that are seen their brain cells. The purpose of this research study is to determine if minocycline is an effective treatment for patients with fragile X syndrome (FXS).
Fragile X Syndrome (FXS) is the most common known inherited form of mental impairment and is
also associated with a range of learning disabilities, neurological problems, such as
seizures, and behavioural difficulties. For many individuals with FXS, behavioral
difficulties result in severe problems within the family and community, particularly in the
form of agitation, temper outbursts, hyperactivity, and aggression. These problems often
require a variety of psychopharmacological and behavioural approaches. Although a variety of
medications can be helpful in FXS there are no targeted interventions based on molecular
abnormalities that have been studied. Defects in dendritic spine formation have been found
in the brains of patients with Fragile X, suggesting these structures may represent an
anatomical and physiological basis for the cognitive deficits associated with this disorder.
Recent research has suggested that minocycline may have a specific benefit in the treatment
of FXS. Minocycline is an antibiotic that has been found to inhibit the activity of matrix
metallo-proteinase-9 (MMP-9), which is up-regulated in the hippocampus of FMR1 KO (Fragile X
Mental Retardation-1 Knockout) mice and may be responsible for the immature dendritic spine
profile of hippocampal neurons. Minocycline has recently been used to treat the FXS KO mouse
model for Fragile X, and was found to rescue this abnormal phenotype by inducing the
formation of mature dendritic spines in FMR1 KO hippocampal neurons, both in vitro and in
vivo. Minocycline treated FXS KO mice also performed significantly better in the elevated
maze, a cognitive performance test that measures activity and anxiety.
Exciting preclinical effects of minocycline with regard to the FXS disease model have led to
this pilot proposal, which is designed to generate preliminary data that could be used to
support a larger clinical trial.
The overall hypothesis is that minocycline is a specific molecular targeted treatment for
FXS that will display beneficial effects on disruptive behaviour and possibly other
associated features of FXS via a reduction in MMP-9 activity.
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Endpoint Classification: Efficacy Study, Intervention Model: Single Group Assignment, Masking: Open Label, Primary Purpose: Treatment
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