Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
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Gene/Protein
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Target Concepts:
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Query: EC:3.1.27.1 (
RNase
)
16,360
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Brevican is a brain-specific proteoglycan belonging to the aggrecan family. Phage clones containing the complete mouse
brevican
open reading frame of 2649 bp and the complete 3'-untranslated region of 341 bp were isolated from a mouse brain cDNA library, and cosmid clones containing the mouse
brevican
gene were isolated from a genomic library using a PCR-generated DNA fragment as probe. The obtained genomic sequence of 13,700 nucleotides revealed that the murine gene has a size of approximately 13 kb and contains the sequence of the mRNA for the secreted
brevican
isoform on 14 exons. The exon-intron structure reflected the structural organization of the multidomain protein
brevican
. No consensus TATA sequence was found upstream of the first exon, and
RNase
protection experiments revealed multiple transcriptional start sites for the
brevican
gene. The first part of the sequence of intron 8 corresponded to an alternative
brevican
cDNA, coding for a GPI-linked isoform. Single strand conformation polymorphism analysis mapped the
brevican
gene (Bcan) to chromosome 3 between the microsatellite markers D3Mit22 and D3Mit11.
...
PMID:Sequence and chromosomal localization of the mouse brevican gene. 928 96
BEHAB
(Brain Enriched HyAluronan Binding)/
brevican
, a brain-specific member of the lectican family of chondroitin sulfate proteoglycans (CSPGs), may play a role in both brain development and human glioma.
BEHAB
/
brevican
has been cloned from bovine, mouse and rat. Two isoforms have been reported: a full-length isoform that is secreted into the extracellular matrix (ECM) and a shorter isoform with a sequence that predicts a glycophosphatidylinositol (GPI) anchor. Here, we report the characterization of
BEHAB
/
brevican
isoforms in human brain. First,
BEHAB
/
brevican
maps to human chromosome 1q31. Second, we report the sequence of both isoforms of human
BEHAB
/
brevican
. The deduced protein sequence of full-length, secreted human
BEHAB
/
brevican
is 89.7, 83.3 and 83.2% identical to bovine, mouse and rat homologues, respectively. Third, by
RNase
protection analysis (RPA) we show the developmental regulation of
BEHAB
/
brevican
isoforms in normal human cortex. The secreted isoform is highly expressed from birth through 8years of age and is downregulated by 20years of age to low levels that are maintained in the normal adult cortex. The GPI isoform is expressed at uniformly low levels throughout development. Fourth, we confirm and extend previous studies from our laboratory, here demonstrating the upregulation of
BEHAB
/
brevican
mRNA in human glioma quantitatively. RPA analysis shows that both isoforms are upregulated in glioma, showing an approximately sevenfold increase in expression over normal levels. In contrast to the developmental regulation of
BEHAB
/
brevican
, where only the secreted isoform is regulated, both isoforms are increased in parallel in human glioma. The distinct patterns of regulation of expression of the two isoforms suggest distinct mechanisms of regulation of
BEHAB
/
brevican
during development and in glioma.
...
PMID:cDNA cloning, chromosomal localization, and expression analysis of human BEHAB/brevican, a brain specific proteoglycan regulated during cortical development and in glioma. 1105 43
Brevican is one of the most abundant extracellular matrix proteoglycans in the mammalian brain. We have previously shown that
brevican
produced by gray matter astrocytes constitutes a major component of perineuronal extracellular matrix in the adult brain. In this paper, we investigate the expression of
brevican
in the postnatal hippocampal fimbria to explore the role of the proteoglycan in central nervous system fiber tract development. We demonstrate that
brevican
is expressed by both oligodendrocytes and white matter astrocytes in the fimbria, but the expression of
brevican
in these two glial cell types is differently regulated during development. At P14,
brevican
immunoreactivity was observed throughout the fimbria, with particularly strong immunoreactivity in the developing interfascicular glial rows. In situ hybridization showed that oligodendrocytes in the glial rows strongly express
brevican
during the second and third postnatal weeks. Expression in oligodendrocytes was then down-regulated after P21. In the adult fimbria, no
brevican
expression was observed in oligodendrocytes. The time window of
brevican
expression coincides with the phase in which immature oligodendrocytes actively extend membrane processes and enwrap axon fibers. In contrast, the expression in astrocytes started around P21 as oligodendrocytes began to down-regulate the expression. In the adult fimbria,
brevican
expression was restricted to astrocytes. In situ hybridization with isoform-specific probes and
RNase
protection assays showed that the authentic, secreted form of
brevican
, not the glycosylphosphatidylinositol-anchored variant, is the predominant species expressed in the developing fimbria. Our results suggest that
brevican
plays a dual role in developing and adult fiber tracts.
...
PMID:Brevican in the developing hippocampal fimbria: differential expression in myelinating oligodendrocytes and adult astrocytes suggests a dual role for brevican in central nervous system fiber tract development. 1124 8
