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Query: UMLS:C0025362 (
mental retardation
)
15,878
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The absence of the
fragile X mental retardation protein
(
FMRP
), encoded by the FMR1 gene, is responsible for pathologic manifestations in the Fragile X Syndrome, the most frequent cause of inherited
mental retardation
.
FMRP
is an RNA-binding protein associated with polysomes as part of a messenger ribonucleoprotein (mRNP) complex. Although its function is poorly understood, various observations suggest a role in local protein translation at neuronal dendrites and in dendritic spine maturation. We present here the identification of CYFIP1/2 (Cytoplasmic
FMRP
Interacting Proteins) as
FMRP
interactors. CYFIP1/2 share 88% amino acid sequence identity and represent the two members in humans of a highly conserved protein family. Remarkably, whereas CYFIP2 also interacts with the
FMRP
-related proteins FXR1P/2P, CYFIP1 interacts exclusively with
FMRP
.
FMRP
--CYFIP interaction involves the domain of
FMRP
also mediating homo- and heteromerization, thus suggesting a competition between interaction among the FXR proteins and interaction with CYFIP. CYFIP1/2 are proteins of unknown function, but CYFIP1 has recently been shown to interact with the small GTPase Rac1, which is implicated in development and maintenance of neuronal structures. Consistent with
FMRP
and Rac1 localization in dendritic fine structures, CYFIP1/2 are present in synaptosomal extracts.
...
PMID:A highly conserved protein family interacting with the fragile X mental retardation protein (FMRP) and displaying selective interactions with FMRP-related proteins FXR1P and FXR2P. 1143 99
1. Fragile X syndrome, the most common form of inherited
mental retardation
, is caused by the lack or dysfunction of
fragile X mental retardation protein
(
FMRP
). The 1304N mutation in the RNA-binding domain of
FMRP
results in an exceptionally severe form of
mental retardation
. 2. We have investigated the subcellular localization of
FMRP
and its 1304N-mutated form in cultured hippocampal neurons and PC12 cells, using immunofluorescence microscopy. In PC12 cells,
FMRP
was predominantly localized to the cytoplasm and also to the processes after differentiation by NGF. 3. In cultured hippocampal neurons, granular labeling was detected along the neuronal processes. 4. Double-labeling with synaptophysin antibody revealed
FMRP
at synaptic sites in neurons. 5. The 1304N mutation did not appear to affect the transport of
FMRP
to dendrites or its localization at synaptic sites. Thus,
FMRP
is a synaptic protein and the severe phenotype observed in the patient with the 1304N mutation is not produced by alterations in dendritic transport.
...
PMID:Subcellular localization of fragile X mental retardation protein with the I304N mutation in the RNA-binding domain in cultured hippocampal neurons. 1144 Jan 96
The 5' untranslated CGG repeat in the fragile X
mental retardation
-1 (FMR1) gene is expanded in families with fragile X syndrome, with more than 200 CGGs resulting in
mental retardation
due to the absence of the encoded
fragile X mental retardation protein
(
FMRP
). Intermediate and premutation alleles, containing between approximately 40 and 200 repeats, express grossly normal
FMRP
levels and such carriers are widely believed to be non-penetrant, despite continued reports of subtle cognitive/psychosocial impairment and other phenotypes. Using a highly sensitive quantification assay, we demonstrate significantly diminished
FMRP
levels in carriers, negatively correlated with repeat number. Despite reduced
FMRP
, these carrier alleles overexpress FMR1, resulting in a positive correlation between repeat number and FMR1 message level. These biochemical deviations associated with intermediate and premutation FMR1 alleles, found in approximately 4% of the population, suggest that the phenotypic spectrum of fragile X syndrome may need to be revisited.
...
PMID:Reduced FMRP and increased FMR1 transcription is proportionally associated with CGG repeat number in intermediate-length and premutation carriers. 1144 36
Loss of
fragile X mental retardation protein
(
FMRP
) function causes the fragile X
mental retardation
syndrome.
FMRP
harbors three RNA binding domains, associates with polysomes, and is thought to regulate mRNA translation and/or localization, but the RNAs to which it binds are unknown. We have used RNA selection to demonstrate that the
FMRP
RGG box binds intramolecular G quartets. This data allowed us to identify mRNAs encoding proteins involved in synaptic or developmental neurobiology that harbor
FMRP
binding elements. The majority of these mRNAs have an altered polysome association in fragile X patient cells. These data demonstrate that G quartets serve as physiologically relevant targets for
FMRP
and identify mRNAs whose dysregulation may underlie human
mental retardation
.
...
PMID:Fragile X mental retardation protein targets G quartet mRNAs important for neuronal function. 1173 54
The Fragile X syndrome, a common form of
mental retardation
in humans, is caused by silencing the fragile X
mental retardation
(FMR1) gene leading to the absence of the encoded
fragile X mental retardation protein
1 (FMRP). We describe morphological and behavioral abnormalities for both affected humans and Fmr1 knockout mice, a putative animal model for the human Fragile X syndrome. The aim of the present study was to identify possible neurochemical abnormalities in Fmr1 knockout mice, with particular focus on neurotransmission. Significant region-specific differences of basal neurotransmitter and metabolite levels were found between wildtype and Fmr1 knockout animals, predominantly in juveniles (post-natal days 28 to 31). Adults (postnatal days 209 to 221) showed only few abnormalities as compared with the wildtype. In juvenile knockout mice, aspartate and taurine were especially increased in cortical regions, striatum, hippocampus, cerebellum, and brainstem. In addition, juveniles showed an altered balance between excitatory and inhibitory amino acids in the caudal cortex, hippocampus, and brainstem. We detected very few differences in monoamine turnover in both age stages. The results presented here provide the first evidence that lack of FMRP expression in FMRP knockout mice is accompanied by age-dependent, region-specific alterations in neurotransmission.
...
PMID:Alterations of amino acids and monoamine metabolism in male Fmr1 knockout mice: a putative animal model of the human fragile X mental retardation syndrome. 1201 75
Fragile X syndrome, the most common inherited form of human
mental retardation
, is caused by mutations of the Fmr1 gene that encodes the
fragile X mental retardation protein
(
FMRP
). Biochemical evidence indicates that
FMRP
binds a subset of mRNAs and acts as a regulator of translation. However, the consequences of
FMRP
loss on neuronal function in mammals remain unknown. Here we show that a form of protein synthesis-dependent synaptic plasticity, long-term depression triggered by activation of metabotropic glutamate receptors, is selectively enhanced in the hippocampus of mutant mice lacking
FMRP
. This finding indicates that
FMRP
plays an important functional role in regulating activity-dependent synaptic plasticity in the brain and suggests new therapeutic approaches for fragile X syndrome.
...
PMID:Altered synaptic plasticity in a mouse model of fragile X mental retardation. 1203 54
Fragile X syndrome is one of the most common forms of inherited
mental retardation
. In most cases the disease is caused by the methylation-induced transcriptional silencing of the fragile X mental retardation 1 (FMR1) gene that occurs as a result of the expansion of a CGG repeat in the gene's 5'UTR and leads to the loss of protein product
fragile X mental retardation protein
(
FMRP
).
FMRP
is an RNA binding protein that associates with translating polyribosomes as part of a large messenger ribonucleoprotein (mRNP) and modulates the translation of its RNA ligands. Pathological studies from the brains of patients and from Fmr1 knockout mice show abnormal dendritic spines implicating
FMRP
in synapse formation and function. Evidence from both in vitro and in vivo neuronal studies indicates that
FMRP
is located at the synapse and the loss of
FMRP
alters synaptic plasticity. As synaptic plasticity has been implicated in learning and memory, analysis of synapse abnormalities in patients and Fmr1 knockout mice should prove useful in studying the pathogenesis of fragile X syndrome and understanding learning and cognition in general. If an appreciable portion of the total variance (in IQ) is due to sex linked genes, it is of more importance that a boy should have a clever mother than a clever father. Hogben 1932 (quoted in Lehrke 1974)
...
PMID:A decade of molecular studies of fragile X syndrome. 1205 12
Lack of
fragile X mental retardation protein
(
FMRP
) causes fragile X syndrome, a common form of inherited
mental retardation
.
FMRP
is an RNA binding protein thought to be involved in translation efficiency and/or trafficking of certain mRNAs. Recently, a subset of mRNAs to which
FMRP
binds with high affinity has been identified. These
FMRP
-associated mRNAs contain an intramolecular G-quartet structure. In neurons, dendritic mRNAs are involved in local synthesis of proteins in response to synaptic activity, and this represents a mechanism for synaptic plasticity. To determine the role of
FMRP
in dendritic mRNA transport, we have generated a stably FMR1-enhanced green fluorescent protein (EGFP)-transfected PC12 cell line with an inducible expression system (Tet-On) for regulated expression of the
FMRP
-GFP fusion protein. After doxycycline induction,
FMRP
-GFP was localized in granules in the neurites of PC12 cells. By using time-lapse microscopy, the trafficking of
FMRP
-GFP granules into the neurites of living PC12 cells was demonstrated. Motile
FMRP
-GFP granules displayed two types of movements: oscillatory (bidirectional) and unidirectional anterograde. The average velocity of the granules was 0.19 micro m/s with a maximum speed of 0.71 micro m/s. In addition, we showed that the movement of
FMRP
-GFP labeled granules into the neurites was microtubule dependent. Colocalization studies further showed that the
FMRP
-GFP labeled granules also contained RNA, ribosomal subunits, kinesin heavy chain, and FXR1P molecules. This report is the first example of trafficking of RNA-containing granules with
FMRP
as a core constituent in living PC12 cells.
...
PMID:Transport of fragile X mental retardation protein via granules in neurites of PC12 cells. 1241 34
Fragile X syndrome is the most common cause of
mental retardation
known to be inherited. The syndrome results from the suppressed expression of a single protein, the
fragile X mental retardation protein
(
FMRP
). Understanding the function and regulation of
FMRP
can, therefore, offer insights into both the pathophysiology of fragile X syndrome and the molecular mechanisms of learning and memory. We provide an overview of current concepts of how
FMRP
functions in the nervous system, with special emphasis on recent evidence that
FMRP
has a role in metabotropic glutamate receptor-activated protein translation and synaptic plasticity.
...
PMID:Fragile X mental retardation protein in plasticity and disease. 1242 29
In humans, failure to express the
fragile X mental retardation protein
(
FMRP
) gives rise to fragile X syndrome, the most common form of inherited
mental retardation
. A fragile X knockout (fmr1 KO) mouse has been described that has some of the characteristics of patients with fragile X syndrome, including immature dendritic spines and subtle behavioral deficits. In our behavioral studies, fmr1 KO mice exhibited hyperactivity and a higher rate of entrance into the center of an open field compared with controls, suggesting decreased levels of anxiety. Our finding of impaired performance of fmr1 KO mice on a passive avoidance task is suggestive of a deficit in learning and memory. In an effort to understand what brain regions are involved in the behavioral abnormalities, we applied the [(14)C]deoxyglucose method for the determination of cerebral metabolic rates for glucose (CMR(glc)). We measured CMR(glc) in 38 regions in adult male fmr1 KO and WT littermates. We found CMR(glc) was higher in all 38 regions in fmr1 KO mice, and in 26 of the regions, differences were statistically significant. Differences in CMR(glc) ranged from 12% to 46%, and the greatest differences occurred in regions of the limbic system and primary sensory and posterior parietal cortical areas. Regions most affected are consistent with behavioral deficiencies and regions in which
FMRP
expression is highest. Higher CMR(glc) in fragile X mice may be a function of abnormalities found in dendritic spines.
...
PMID:Increased rates of cerebral glucose metabolism in a mouse model of fragile X mental retardation. 1242 68
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