1.Clinical characteristics of children with mental retardation of unknown etiology in Korea.
Journal of Korean Medical Science 1999;14(2):128-132
The purpose of this study was to investigate the clinical characteristics of children with mental retardation (MR) of unknown etiology for early recognition and intervention. In this study, we defined children with MR of unknown etiology as those without clear etiologies for MR despite extensive evaluation and were not associated with pathological behavioral problems such as pervasive developmental disorders and attention-deficit/hyperactivity disorder. The clinical characteristics of children with MR of unknown etiology were as follows. 1) MR of unknown etiology was 48.8% of all MR. 2) MR of unknown etiology was more common in males. 3) Delayed language development was a leading factor that made the parents of children with MR of unknown etiology seek help from physicians. However, most of the children with MR of unknown etiology showed a relatively uniform delay in several areas of development. 4) Most children with MR of unknown etiology were delayed walkers. 5) Most children with MR of unknown etiology were mild cases.
Child
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Child, Preschool
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Female
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Human
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Korea
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Language Development Disorders
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Male
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Mental Retardation/psychology
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Mental Retardation/physiopathology*
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Mental Retardation/etiology
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Retrospective Studies
2.Fragile X syndrome and epilepsy.
Li-Feng QIU ; Yan-Hong HAO ; Qing-Zhang LI ; Zhi-Qi XIONG
Neuroscience Bulletin 2008;24(5):338-344
Fragile X syndrome (FXS) is one of the most prevalent mental retardations. It is mainly caused by the loss of fragile X mental retardation protein (FMRP). FMRP is an RNA binding protein and can regulate the translation of its binding RNA, thus regulate several signaling pathways. Many FXS patients show high susceptibility to epilepsy. Epilepsy is a chronic neurological disorder which is characterized by the recurrent appearance of spontaneous seizures due to neuronal hyperactivity in the brain. Both the abnormal activation of several signaling pathway and morphological abnormality that are caused by the loss of FMRP can lead to a high susceptibility to epilepsy. Combining with the research progresses on both FXS and epilepsy, we outlined the possible mechanisms of high susceptibility to epilepsy in FXS and tried to give a prospect on the future research on the mechanism of epilepsy that happened in other mental retardations.
Brain
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physiopathology
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Epilepsy
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etiology
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genetics
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pathology
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Fragile X Mental Retardation Protein
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genetics
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metabolism
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Fragile X Syndrome
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complications
;
genetics
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Humans
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RNA-Binding Proteins
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metabolism