Title |
Multiple Drug Treatments That Increase cAMP Signaling Restore Long-Term Memory and Aberrant Signaling in Fragile X Syndrome Models
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Published in |
Frontiers in Behavioral Neuroscience, June 2016
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DOI | 10.3389/fnbeh.2016.00136 |
Pubmed ID | |
Authors |
Catherine H. Choi, Brian P. Schoenfeld, Aaron J. Bell, Joseph Hinchey, Cory Rosenfelt, Michael J. Gertner, Sean R. Campbell, Danielle Emerson, Paul Hinchey, Maria Kollaros, Neal J. Ferrick, Daniel B. Chambers, Steven Langer, Steven Sust, Aatika Malik, Allison M. Terlizzi, David A. Liebelt, David Ferreiro, Ali Sharma, Eric Koenigsberg, Richard J. Choi, Natalia Louneva, Steven E. Arnold, Robert E. Featherstone, Steven J. Siegel, R. Suzanne Zukin, Thomas V. McDonald, Francois V. Bolduc, Thomas A. Jongens, Sean M. J. McBride |
Abstract |
Fragile X is the most common monogenic disorder associated with intellectual disability (ID) and autism spectrum disorders (ASD). Additionally, many patients are afflicted with executive dysfunction, ADHD, seizure disorder and sleep disturbances. Fragile X is caused by loss of FMRP expression, which is encoded by the FMR1 gene. Both the fly and mouse models of fragile X are also based on having no functional protein expression of their respective FMR1 homologs. The fly model displays well defined cognitive impairments and structural brain defects and the mouse model, although having subtle behavioral defects, has robust electrophysiological phenotypes and provides a tool to do extensive biochemical analysis of select brain regions. Decreased cAMP signaling has been observed in samples from the fly and mouse models of fragile X as well as in samples derived from human patients. Indeed, we have previously demonstrated that strategies that increase cAMP signaling can rescue short term memory in the fly model and restore DHPG induced mGluR mediated long term depression (LTD) in the hippocampus to proper levels in the mouse model (McBride et al., 2005; Choi et al., 2011, 2015). Here, we demonstrate that the same three strategies used previously with the potential to be used clinically, lithium treatment, PDE-4 inhibitor treatment or mGluR antagonist treatment can rescue long term memory in the fly model and alter the cAMP signaling pathway in the hippocampus of the mouse model. |
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Geographical breakdown
Country | Count | As % |
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Unknown | 1 | 100% |
Demographic breakdown
Type | Count | As % |
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Members of the public | 1 | 100% |
Mendeley readers
Geographical breakdown
Country | Count | As % |
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United States | 2 | 2% |
Unknown | 99 | 98% |
Demographic breakdown
Readers by professional status | Count | As % |
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Student > Bachelor | 20 | 20% |
Researcher | 16 | 16% |
Student > Ph. D. Student | 15 | 15% |
Student > Master | 9 | 9% |
Student > Postgraduate | 5 | 5% |
Other | 14 | 14% |
Unknown | 22 | 22% |
Readers by discipline | Count | As % |
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Psychology | 18 | 18% |
Biochemistry, Genetics and Molecular Biology | 15 | 15% |
Neuroscience | 14 | 14% |
Medicine and Dentistry | 13 | 13% |
Agricultural and Biological Sciences | 8 | 8% |
Other | 13 | 13% |
Unknown | 20 | 20% |