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Publication : Molecular polymorphism of the syndecans. Identification of a hypo-glycanated murine syndecan-1 splice variant.

First Author  Romarís M Year  1999
Journal  J Biol Chem Volume  274
Issue  26 Pages  18667-74
PubMed ID  10373479 Mgi Jnum  J:55871
Mgi Id  MGI:1339504 Doi  10.1074/jbc.274.26.18667
Citation  Romaris M, et al. (1999) Molecular polymorphism of the syndecans. Identification of a hypo-glycanated murine syndecan-1 splice variant. J Biol Chem 274(26):18667-74
abstractText  We have identified a cDNA that encodes a variant form of murine syndecan-1, The variant cDNA lacks the sequence corresponding to the first 132 nucleotides of the third exon of the syndecan-1 gene. The corresponding message is rare. The alternative splice respects the reading frame and deletes 44 amino acids from the protein, joining the S(45)GS(47)GT sequence to a variant immediate downstream context. This sequence context initiates with alanine instead of glycine as residue 50, reducing the number of SGXG sequence motifs in the protein from two to one. Expression of this variant syndecan-1 in Madin-Darby canine kidney or MOLT-4 cells yielded a recombinant proteoglycan with a reduced number and clustering of the heparan sulfate chains, Both the conversions of Ala(50) and of Lys(53) into glycine enhanced the heparan sulfate substitution of the variant protein. These findings support the concept that serine glycine dipeptide signals for glycosaminoglycan/heparan sulfate synthesis depend on sequence context (Zhang, L., David, G.., and Esko, J. D. (1995) J. Biol. Chem, 270, 27127-27135) and imply that alternative splicing mechanisms may in part control the molecular polymorphism of syndecan-1 and, therefore, the efficiency and versatility of this protein in its co- receptor functions.
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