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The challenges of clinical trials in fragile X syndrome
by
Des Portes, Vincent
, Gomez-Mancilla, Baltazar
, Berry-Kravis, Elizabeth
, Hagerman, Randi
, von Raison, Florian
, Apostol, George
, Ufer, Mike
, Jacquemont, Sébastien
, Gasparini, Fabrizio
in
Analysis
/ Animals
/ Autism
/ Biomedical and Life Sciences
/ Biomedicine
/ Care and treatment
/ Child Development Disorders, Pervasive - drug therapy
/ Child Development Disorders, Pervasive - physiopathology
/ Clinical trials
/ Clinical Trials as Topic - methods
/ Cognitive science
/ Developmental disabilities
/ Diagnosis
/ Fragile X syndrome
/ Fragile X Syndrome - diagnosis
/ Fragile X Syndrome - drug therapy
/ Fragile X Syndrome - genetics
/ Fragile X Syndrome - physiopathology
/ GABA
/ Genetic aspects
/ Genetic disorders
/ Humans
/ Methylation
/ Neurosciences
/ Pharmacology/Toxicology
/ Phenotype
/ Psychiatry
/ Psychopharmacology
/ Review
2014
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The challenges of clinical trials in fragile X syndrome
by
Des Portes, Vincent
, Gomez-Mancilla, Baltazar
, Berry-Kravis, Elizabeth
, Hagerman, Randi
, von Raison, Florian
, Apostol, George
, Ufer, Mike
, Jacquemont, Sébastien
, Gasparini, Fabrizio
in
Analysis
/ Animals
/ Autism
/ Biomedical and Life Sciences
/ Biomedicine
/ Care and treatment
/ Child Development Disorders, Pervasive - drug therapy
/ Child Development Disorders, Pervasive - physiopathology
/ Clinical trials
/ Clinical Trials as Topic - methods
/ Cognitive science
/ Developmental disabilities
/ Diagnosis
/ Fragile X syndrome
/ Fragile X Syndrome - diagnosis
/ Fragile X Syndrome - drug therapy
/ Fragile X Syndrome - genetics
/ Fragile X Syndrome - physiopathology
/ GABA
/ Genetic aspects
/ Genetic disorders
/ Humans
/ Methylation
/ Neurosciences
/ Pharmacology/Toxicology
/ Phenotype
/ Psychiatry
/ Psychopharmacology
/ Review
2014
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The challenges of clinical trials in fragile X syndrome
by
Des Portes, Vincent
, Gomez-Mancilla, Baltazar
, Berry-Kravis, Elizabeth
, Hagerman, Randi
, von Raison, Florian
, Apostol, George
, Ufer, Mike
, Jacquemont, Sébastien
, Gasparini, Fabrizio
in
Analysis
/ Animals
/ Autism
/ Biomedical and Life Sciences
/ Biomedicine
/ Care and treatment
/ Child Development Disorders, Pervasive - drug therapy
/ Child Development Disorders, Pervasive - physiopathology
/ Clinical trials
/ Clinical Trials as Topic - methods
/ Cognitive science
/ Developmental disabilities
/ Diagnosis
/ Fragile X syndrome
/ Fragile X Syndrome - diagnosis
/ Fragile X Syndrome - drug therapy
/ Fragile X Syndrome - genetics
/ Fragile X Syndrome - physiopathology
/ GABA
/ Genetic aspects
/ Genetic disorders
/ Humans
/ Methylation
/ Neurosciences
/ Pharmacology/Toxicology
/ Phenotype
/ Psychiatry
/ Psychopharmacology
/ Review
2014
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Journal Article
The challenges of clinical trials in fragile X syndrome
2014
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Overview
Rationale
Advances in understanding the underlying mechanisms of conditions such as fragile X syndrome (FXS) and autism spectrum disorders have revealed heterogeneous populations. Recent trials of novel FXS therapies have highlighted several challenges including subpopulations with possibly differential therapeutic responses, the lack of specific outcome measures capturing the full range of improvements of patients with FXS, and a lack of biomarkers that can track whether a specific mechanism is responsive to a new drug and whether the response correlates with clinical improvement.
Objectives
We review the phenotypic heterogeneity of FXS and the implications for clinical research in FXS and other neurodevelopmental disorders.
Results
Residual levels of fragile X mental retardation protein (FMRP) expression explain in part the heterogeneity in the FXS phenotype; studies indicate a correlation with both cognitive and behavioral deficits. However, this does not fully explain the extent of phenotypic variance observed or the variability of drug response. Post hoc analyses of studies involving the selective mGluR5 antagonist mavoglurant and the GABA
B
agonist arbaclofen have uncovered significant therapeutic responses following patient stratification according to
FMR1
promoter methylation patterns or baseline severity of social withdrawal, respectively. Future studies designed to quantify disease modification will need to develop new strategies to track changes effectively over time and in multiple symptom domains.
Conclusion
Appropriate selection of patients and outcome measures is central to optimizing future clinical investigations of these complex disorders.
Publisher
Springer Berlin Heidelberg,Springer,Springer Nature B.V,Springer Verlag
Subject
/ Animals
/ Autism
/ Biomedical and Life Sciences
/ Child Development Disorders, Pervasive - drug therapy
/ Child Development Disorders, Pervasive - physiopathology
/ Clinical Trials as Topic - methods
/ Fragile X Syndrome - diagnosis
/ Fragile X Syndrome - drug therapy
/ Fragile X Syndrome - genetics
/ Fragile X Syndrome - physiopathology
/ GABA
/ Humans
/ Review
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