3.8 Article

A family of novel, acidic N-glycans in Bowes melanoma tissue plasminogen activator have L2/HNK-1-bearing antennae, many with sulfation of the fucosylated chitobiose core

Journal

EUROPEAN JOURNAL OF BIOCHEMISTRY
Volume 268, Issue 14, Pages 4063-4078

Publisher

WILEY-BLACKWELL
DOI: 10.1046/j.1432-1327.2001.02320.x

Keywords

tissue plasminogen activator; N-linked glycans; sulfate; MALDI MS; LZ/HNK-1

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A family of about 20 novel acidic bi- and tri-antennary N-glycans, amounting to almost half those expressed on Bowes melanoma tissue-plasminogen activator (t-PA) were found to possess Ga1beta1-4GlcNAcbeta1-, sulfated and sialylated Ga1NAcbeta1-4G1cNAbeta1- or sulfated G1cAbeta1-3Ga1beta1-4G1cNAbeta1- antennae, of which those containing sulfated G1cA, depicting the L2/HNK-1 carbohydrate epitope, were preferentially located on the 6 arm. A proportion of the glycans were highly charged, because of multiple and variously distributed sulfation, some of which was located on the fucosylated chitobiose core. Multiple expression of the L2/HNK-1 epitope on a single glycan was observed. The most abundant compound was a biantennary glycan carrying sulfated GlcA on the 6-branched antenna and an alpha2-6 sialylated Ga1NAc on the other. The N-glycosylation sequon containing Asn448, which is known to express all of the sulfate-carrying N-glycans contains, unusually, an arginine residue. An electrostatic interaction between this cationic amino acid and the core-sulfate group of the N-glycan is proposed to reduce mobility of the carbohydrate in the region of the t-PA active site. Because of the 'brain-type' nature of the N-glycans described in this neuro-ectodermal cell line, the possibility of neural t-PA interacting with the L2/HNK1-recognizing molecule, laminin, of the central nervous system extracellular matrix is discussed.

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