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Open AccessJournal ArticleDOI

Genomic structure of DNA encoding the lymphocyte homing receptor CD44 reveals at least 12 alternatively spliced exons.

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TLDR
The genomic structure of CD44 reveals a remarkable degree of complexity, and the role of alternative splicing as the basis of the structural and functional diversity seen in the CD44 molecule is confirmed.
Abstract
The CD44 molecule is known to display extensive size heterogeneity, which has been attributed both to alternative splicing and to differential glycosylation within the extracellular domain. Although the presence of several alternative exons has been partly inferred from cDNA sequencing, the precise intron-exon organization of the CD44 gene has not been described to date to our knowledge. In the present study we describe the structure of the human CD44 gene, which contains at least 19 exons spanning some 50 kilobases of DNA. We have identified 10 alternatively spliced exons within the extracellular domain, including 1 exon that has not been previously reported. In addition to the inclusion or exclusion of whole exons, more diversity is generated through the utilization of internal splice donor and acceptor sites within 2 of the individual exons. The variation previously reported for the cytoplasmic domain is shown to result from the alternative splicing of 2 exons. The genomic structure of CD44 reveals a remarkable degree of complexity, and we confirm the role of alternative splicing as the basis of the structural and functional diversity seen in the CD44 molecule.

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Citations
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Journal ArticleDOI

CD44: From adhesion molecules to signalling regulators

TL;DR: Cell-adhesion molecules, once believed to function primarily in tethering cells to extracellular ligands, are now recognized as having broader functions in cellular signalling cascades and the CD44 transmembrane glycoprotein family adds new aspects to these roles by participating in signal-transduction processes.
Journal ArticleDOI

Function of alternative splicing.

TL;DR: Evidence is now accumulating that alternative splicing coordinates physiologically meaningful changes in protein isoform expression and is a key mechanism to generate the complex proteome of multicellular organisms.
Journal ArticleDOI

MapSplice: Accurate mapping of RNA-seq reads for splice junction discovery

TL;DR: A second generation splice detection algorithm, MapSplice, whose focus is high sensitivity and specificity in the detection of splices as well as CPU and memory efficiency is introduced, which indicates that Map Splice is a highly accurate algorithm for the alignment of RNA-seq reads to splice junctions.
Book ChapterDOI

CD44 and its interaction with extracellular matrix.

TL;DR: A great variety of responses has been reported to result from CD44 ligation, which indicates that downstream events following ligand binding by CD44 may vary depending on the cell type expressing CD44 and on the environment of that cell.
Journal ArticleDOI

CD44: can a cancer-initiating cell profit from an abundantly expressed molecule?

TL;DR: Can an abundantly expressed molecule be a reliable marker for the cancer-initiating cells (CICs) and is CD44 expression advantageous as it fulfils some of the special properties that are displayed by CICs, such as self-renewal, niche preparation, epithelial–mesenchymal transition and resistance to apoptosis?
References
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Book

Molecular Cloning: A Laboratory Manual

TL;DR: Molecular Cloning has served as the foundation of technical expertise in labs worldwide for 30 years as mentioned in this paper and has been so popular, or so influential, that no other manual has been more widely used and influential.
Journal ArticleDOI

Selection of splice sites in pre-mRNAs with short internal exons.

TL;DR: Model pre-mRNAs containing two introns and three exons, derived from the human beta-globin gene, were used to study the effects of internal exon length on splice site selection, suggesting that a balance between the length of the uninterrupted polypyrimidine tract and thelength of the exon is an important determinant of the relative strength of the splice sites, ensuring correct splicing patterns of multiintron pre- mRNAs.
Journal ArticleDOI

Expression of CD44 is repressed in neuroblastoma cells.

TL;DR: A DNA segment including about 150 bp of the CD44 upstream region and the 5' end of the gene itself was sufficient to induce substantial transcription of the chloramphenicol acetyltransferase gene in both neuroblastoma and melanoma cells, suggesting that multiple factors might be involved in downregulation of CD44 in Neuroblastoma cells.
Journal ArticleDOI

At least 27 alternatively spliced forms of the neural cell adhesion molecule mRNA are expressed during rat heart development

TL;DR: The characterization of tissue-specific patterns of alternative splicing at the exon 12-exon 13 junction by using the polymerase chain reaction suggests a role for NCAM diversity in cardiac development.
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