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Review
. 2018 Dec 5;8(12):214.
doi: 10.3390/brainsci8120214.

Clinical Development of Targeted Fragile X Syndrome Treatments: An Industry Perspective

Anna W Lee  1 Pamela Ventola  2 Dejan Budimirovic  3 Elizabeth Berry-Kravis  4 Jeannie Visootsak  5
Affiliations
Review

Clinical Development of Targeted Fragile X Syndrome Treatments: An Industry Perspective

Anna W Lee et al. Brain Sci. .

Abstract

Fragile X syndrome (FXS) is the leading known cause of inherited intellectual disability and autism spectrum disorder. It is caused by a mutation of the fragile X mental retardation 1 (FMR1) gene, resulting in a deficit of fragile X mental retardation protein (FMRP). The clinical presentation of FXS is variable, and is typically associated with developmental delays, intellectual disability, a wide range of behavioral issues, and certain identifying physical features. Over the past 25 years, researchers have worked to understand the complex relationship between FMRP deficiency and the symptoms of FXS and, in the process, have identified several potential targeted therapeutics, some of which have been tested in clinical trials. Whereas most of the basic research to date has been led by experts at academic institutions, the pharmaceutical industry is becoming increasingly involved with not only the scientific community, but also with patient advocacy organizations, as more promising pharmacological agents are moving into the clinical stages of development. The objective of this review is to provide an industry perspective on the ongoing development of mechanism-based treatments for FXS, including identification of challenges and recommendations for future clinical trials.

Keywords: clinical trials; drug development; fragile X syndrome; targeted treatments.

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Conflict of interest statement

A.W.L. and J.V. are employed by Ovid Therapeutics Inc. P.V. (Yale University) is also employed by Cogstate and has received funding from Roche Pharmaceuticals and Takeda Pharmaceutical Company to consult on clinical trial design in neurodevelopmental disorders. D.B. has received support for clinical trials in FXS from Seaside Therapeutics, Ovid Therapeutics Inc (and consult on trial design), and also NIH-research funding through Asuragen Inc. Within the last three years, D.B. has done ad hoc consulting work (rarely) for the American Academy of Child and Adolescent Psychiatry, Ironshore, MEDACorp, Guidepoint, Ovid Therapeutics, and Sunovion. E.B.-K. (Rush University) has received funding from Seaside Therapeutics, Novartis, Roche, Alcobra, Neuren, Cydan, Fulcrum, GW, Neurotrope, Marinus, BioMarin, Ovid Therapeutics, Zynerba, Tetra, and Yamo Pharmaceuticals to consult on trial design or development strategies and/or conduct clinical trials in FXS and other neurogenetic and neurodevelopmental disorders, from Vtesse/Sucampo/Mallinkcrodt to consult on trial design and results, and conduct clinical trials in NP-C, and from Asuragen Inc to do test validation studies and develop testing standards for FMR1 testing.

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