Advances in the Treatment of Fragile X Syndrome

Hagerman, Randi J; Berry‐Kravis, Elizabeth; Kaufmann, Walter E.; Ono, Michele Y.; Tartaglia, Nicole; Lachiewicz, Ave M.; Kronk, Rebecca; Delahunty, Carol; Hessl, David; Visootsak, Jeannie; Picker, Jonathan; Gane, Louise W.; Tranfaglia, Michael R.

doi:10.1542/peds.2008-0317

Cited by 512 publications

(551 citation statements)

References 169 publications

(154 reference statements)

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“…Around 13-16% of individuals with fragile X develop seizures during their lifetime, 27 which suggests a role for the FMR1 gene in epilepsy. Decreased inhibitory signaling from GABA-A receptors 28 and overactivity of the metabotropic glutamate receptor (mGluR) with resulting altered AMPA receptor activity 29 have been reported as pathogenic mechanisms for increased risk of seizures in fragile X syndrome.…”

Section: Discussionmentioning

confidence: 99%

De novo microduplication of the FMR1 gene in a patient with developmental delay, epilepsy and hyperactivity

et al. 2012

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Loss-of-function due to expansion of a CGG repeat located in the 5'UTR of the FMR1 gene is the most frequent cause of fragile X syndrome. Less than 1% of individuals with fragile X syndrome have been reported to have a partial or full deletion or point mutation of the FMR1 gene. However, whether a copy number gain of the FMR1 gene could result in certain clinical phenotypes has not been fully investigated. Here, we report the case of a child who presented with developmental delay starting at 9 months of age, fine motor and speech delay, progressive seizures since 18 months of age and hyperactivity. Molecular workup identified a de novo microduplication in the Xq27.3 region, including the FMR1 gene and the ASFMR1 gene. The expression level of the FMR1 gene in peripheral blood did not differ from that of the controls. In addition, an inherited 363-kb duplication on the chromosome 1q44 region and an inherited deletion of 168 kb on the chromosome 4p15.31 region were detected. It is not clear whether these inherited copy number variations (CNVs) also have a modifying role in the clinical phenotype of this patient.

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Section: Discussionmentioning

confidence: 99%

De novo microduplication of the FMR1 gene in a patient with developmental delay, epilepsy and hyperactivity

et al. 2012

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“…disorder (Hagerman et al, 2009). FXS patients diagnosed with autism display a more severe social impairment, as well as having lower cognitive and language ability, academic achievement and adaptive behaviour, than seen in FXS individuals without autism (Bailey, Jr. et al, 2001;Hagerman, 2006).…”

Section: Diagnostic and Statistical Manual Of Mental Disorders Fourtmentioning

confidence: 99%

“…FXS patients under the age of 5 years old are particularly difficult to treat, as stimulants that are routinely used to treat older patients are not as effective (Hagerman and Hagerman, 2002). The use of clonidine and guanfacine, agonists of the α-andrenergic receptor, are useful in younger children and are without the side effects of stimulants (Hagerman et al, 2009). Clonidine has also been used to treat sleep disturbances, which in some cases have been reported in up to one-third of patients with FXS (Ingrassia and Turk, 2005;Kronk et al, 2010).…”

Section: Diagnostic and Statistical Manual Of Mental Disorders Fourtmentioning

confidence: 99%

“…The use anticonvulsants must be carefully evaluated in these patients because many drugs can unintentionally exacerbate other symptoms of FXS. Common anticonvulsants such as phenobarbital and gabapentin are generally avoided, because they tend to increase hyperactivity in individuals with FXS (Hagerman et al, 2009). …”

Section: Diagnostic and Statistical Manual Of Mental Disorders Fourtmentioning

confidence: 99%

“…Reduction in intellectual ability ranges from mild to moderate and there is a significant positive correlation between the levels of FMRP and intellectual ability (Loesch et al, 2004). The behavioural phenotype of FXS patients also includes hyperactivity, anxiety, impaired visuo-spatial processing, and developmental delay (Hagerman et al, 2009). Girls with FXS usually suffer from milder cognitive and behavioural deficits than boys primarily due to the fact females still express some FMRP, depending on the ratio of X chromosome inactivation (Freund et al, 1993;Lachiewicz et al, 2006).…”

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Early developmental alterations in GABAergic protein expression in fragile X knockout mice

et al. 2010

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The purpose of this study was to examine the expression of GABAergic proteins in Fmr1 knockout mice during brain maturation and to assess behavioural changes potentially linked to perturbations in the GABAergic system. Quantitative western blotting of the forebrain revealed that compared to wild-type mice, the GABA A receptor α1, β2, and δ subunits, and the GABA catabolic enzymes GABA transaminase and SSADH were down-regulated during postnatal development, while GAD65 was up-regulated in the adult knockout mouse forebrain. In tests of locomotor activity, the suppressive effect on motor activity of the GABA A β2/3 subunit-selective drug loreclezole was impaired in the mutant mice. In addition, sleep time induced by the GABA A β2/3-selective anaesthetic drug etomidate was decreased in the knockout mice. Our results indicate that disruptions in the GABAergic system in the developing brain may result in behavioural consequences in adults with fragile X syndrome.iii

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