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Query: UMLS:C0025362 (
mental retardation
)
15,878
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Down syndrome (DS), a major cause of
mental retardation
, is characterized by subtle abnormalities of cortical neuroanatomy, neurochemistry and function. Recent work has shown that chromosome band 21q22 is critical for many of the neurological phenotypes of DS. A gene,
DSCAM
(Down syndrome cell adhesion molecule), has now been isolated from chromosome band 21q22.2-22.3. Homology searches indicate that the putative
DSCAM
protein is a novel member of the immunoglobulin (Ig) superfamily that represents a new class of neural cell adhesion molecules. The sequence of cDNAs indicates alternative splicing and predicts two protein isoforms, both containing 10 Ig-C2 domains, with nine at the N-terminus and the tenth located between domains 4 and 5 of the following array of six fibronectin III domains, with or without the following transmembrane and intracellular domains. Northern analyses reveals the transcripts of 9.7, 8.5 and 7.6 kb primarily in brain. These transcripts are differentially expressed in substructures of the adult brain. Tissue in situ hybridization analyses of a mouse homolog of the
DSCAM
gene revealed broad expression within the nervous system at the time of neuronal differentiation in the neural tube, cortex, hippocampus, medulla, spinal cord and most neural crest-derived tissues. Given its location on chromosome 21, its specific expression in the central nervous system and neural crest, and the homologies to molecules involved in neural migration, differentiation, and synaptic function, we propose that
DSCAM
is involved in neural differentiation and contributes to the central and peripheral nervous system defects in DS.
...
PMID:DSCAM: a novel member of the immunoglobulin superfamily maps in a Down syndrome region and is involved in the development of the nervous system. 942 58
Down Syndrome (DS) caused by trisomy 21 is the most common birth defect associated with
mental retardation
. Recently, a novel gene named,
DSCAM
, has been identified in the DS critical region.
DSCAM
is predicted to be a transmembrane protein with a very high structural and sequence homology to Ig superfamily of cell adhesion molecules and is expressed in the developing nervous system with the highest level in fetal brain. Diverse glycoproteins of cell surfaces and extracellular matrices operationally termed as 'adhesion molecule' are important in the specification of cell interactions during development, maintenance and regeneration of the nervous system. To understand the cellular function of
DSCAM
protein, we transfected human
DSCAM
cDNA into mouse fibroblast L cells and analysed its expression. On Western blot analysis, antibodies raised against recombinant
DSCAM
-Ig3 recognized a 198 kDa protein band in the membrane fraction of
DSCAM
transfected L cells. Stable transformants expressing
DSCAM
showed uniform surface expression.
DSCAM
-expressing transfectants exhibited enhanced adhesive properties, aggregating with faster kinetics and forming aggregates in a homophilic manner. Divalent cations are not required for this cell aggregation. These results demonstrate that
DSCAM
is a cell adhesion molecule that can mediate cation-independent homophilic binding activity between
DSCAM
expressing cells.
...
PMID:Down syndrome cell adhesion molecule DSCAM mediates homophilic intercellular adhesion. 1092 49
Down Syndrome (DS) is a major cause of
mental retardation
and is associated with characteristic well-defined although subtle brain abnormalities, many of which arise after birth, with particular defects in the cortex, hippocampus and cerebellum. The neural cell adhesion molecule
DSCAM
(Down syndrome cell adhesion molecule) maps to 21q22.2-->q22.3, a region associated with DS
mental retardation
, and is expressed largely in the neurons of the central and peripheral nervous systems during development. In order to evaluate the contribution of
DSCAM
to postnatal morphogenetic and cognitive processes, we have analyzed the expression of the mouse
DSCAM
homolog, Dscam, in the adult mouse brain from 1 through 21 months of age. We have found that Dscam is widely expressed in the brain throughout adult life, with strongest levels in the cortex, the mitral and granular layers of the olfactory bulb, the granule cells of the dentate gyrus and the pyramidal cells of the CA1, CA2 and CA3 regions, the ventroposterior lateral nuclei of the thalamus, and in the Purkinje cells of the cerebellum. Dscam is also expressed ventrally in the adult spinal cord. Given the homology of
DSCAM
to cell adhesion molecules involved in development and synaptic plasticity, and its demonstrated role in axon guidance, we propose that
DSCAM
overexpression contributes not only to the structural defects seen in these regions of the DS brain, but also to the defects of learning and memory seen in adults with DS.
...
PMID:Down syndrome cell adhesion molecule is conserved in mouse and highly expressed in the adult mouse brain. 1185 73
