Role of GalNAc4S-6ST in astrocytic tumor progression.
N-Acetylgalactosamine 4-sulfate 6-O-sulfotransferase (GalNAc4S-6ST) is the sulfotransferase responsible for biosynthesis of highly sulfated chondroitin sulfate CS-E. Although involvements of CS-E in neuronal cell functions have been extensively analyzed, the role of GalNAc4S-6ST in astrocytic tumor...
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doaj-947ead22c00f4d6683caa846f8a8497d2020-11-25T01:14:20ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0181e5427810.1371/journal.pone.0054278Role of GalNAc4S-6ST in astrocytic tumor progression.Tatsuya KobayashiHuimin YanYasuhiro KurahashiYuki ItoHiroshi MaedaTsuyoshi TadaKazuhiro HongoJun NakayamaN-Acetylgalactosamine 4-sulfate 6-O-sulfotransferase (GalNAc4S-6ST) is the sulfotransferase responsible for biosynthesis of highly sulfated chondroitin sulfate CS-E. Although involvements of CS-E in neuronal cell functions have been extensively analyzed, the role of GalNAc4S-6ST in astrocytic tumor progression remains unknown. Here, we reveal that GalNAc4S-6ST transcripts were detected in astrocytic tumors derived from all 30 patients examined using quantitative reverse transcription-PCR analysis. Patients with high GalNAc4S-6ST mRNA expression had significantly worse outcome compared with patients with low expression, and multivariate survival analysis disclosed that GalNAc4S-6ST is an independent poor prognostic factor for astrocytic tumors. We then tested whether CS-E enhanced haptotaxic migration of glioblastoma U251-MG cells that endogenously express both the CS-E's scaffold tyrosine phosphatase ζ (PTPζ) and GalNAc4S-6ST, in the presence of CS-E's preferred ligands, pleiotrophin (PTN) or midkine (MK), using a modified Boyden chamber method. Haptotaxic stimulation of cell migration by PTN was most robust on control siRNA-transfected U251-MG cells, while that enhancing effect was cancelled following transduction of GalNAc4S-6ST siRNA. Similar results were obtained using MK, suggesting that both PTN and MK enhance migration of U251-MG cells by binding to CS-E. We also found that PTPζ as well as PTN and MK were frequently expressed in astrocytic tumor cells. Thus, our findings indicate that GalNAc4S-6ST mRNA expressed by astrocytic tumor cells is associated with poor patient prognosis likely by enhancing CS-E-mediated tumor cell motility in the presence of PTN and/or MK.http://europepmc.org/articles/PMC3547881?pdf=render |
collection |
DOAJ |
language |
English |
format |
Article |
sources |
DOAJ |
author |
Tatsuya Kobayashi Huimin Yan Yasuhiro Kurahashi Yuki Ito Hiroshi Maeda Tsuyoshi Tada Kazuhiro Hongo Jun Nakayama |
spellingShingle |
Tatsuya Kobayashi Huimin Yan Yasuhiro Kurahashi Yuki Ito Hiroshi Maeda Tsuyoshi Tada Kazuhiro Hongo Jun Nakayama Role of GalNAc4S-6ST in astrocytic tumor progression. PLoS ONE |
author_facet |
Tatsuya Kobayashi Huimin Yan Yasuhiro Kurahashi Yuki Ito Hiroshi Maeda Tsuyoshi Tada Kazuhiro Hongo Jun Nakayama |
author_sort |
Tatsuya Kobayashi |
title |
Role of GalNAc4S-6ST in astrocytic tumor progression. |
title_short |
Role of GalNAc4S-6ST in astrocytic tumor progression. |
title_full |
Role of GalNAc4S-6ST in astrocytic tumor progression. |
title_fullStr |
Role of GalNAc4S-6ST in astrocytic tumor progression. |
title_full_unstemmed |
Role of GalNAc4S-6ST in astrocytic tumor progression. |
title_sort |
role of galnac4s-6st in astrocytic tumor progression. |
publisher |
Public Library of Science (PLoS) |
series |
PLoS ONE |
issn |
1932-6203 |
publishDate |
2013-01-01 |
description |
N-Acetylgalactosamine 4-sulfate 6-O-sulfotransferase (GalNAc4S-6ST) is the sulfotransferase responsible for biosynthesis of highly sulfated chondroitin sulfate CS-E. Although involvements of CS-E in neuronal cell functions have been extensively analyzed, the role of GalNAc4S-6ST in astrocytic tumor progression remains unknown. Here, we reveal that GalNAc4S-6ST transcripts were detected in astrocytic tumors derived from all 30 patients examined using quantitative reverse transcription-PCR analysis. Patients with high GalNAc4S-6ST mRNA expression had significantly worse outcome compared with patients with low expression, and multivariate survival analysis disclosed that GalNAc4S-6ST is an independent poor prognostic factor for astrocytic tumors. We then tested whether CS-E enhanced haptotaxic migration of glioblastoma U251-MG cells that endogenously express both the CS-E's scaffold tyrosine phosphatase ζ (PTPζ) and GalNAc4S-6ST, in the presence of CS-E's preferred ligands, pleiotrophin (PTN) or midkine (MK), using a modified Boyden chamber method. Haptotaxic stimulation of cell migration by PTN was most robust on control siRNA-transfected U251-MG cells, while that enhancing effect was cancelled following transduction of GalNAc4S-6ST siRNA. Similar results were obtained using MK, suggesting that both PTN and MK enhance migration of U251-MG cells by binding to CS-E. We also found that PTPζ as well as PTN and MK were frequently expressed in astrocytic tumor cells. Thus, our findings indicate that GalNAc4S-6ST mRNA expressed by astrocytic tumor cells is associated with poor patient prognosis likely by enhancing CS-E-mediated tumor cell motility in the presence of PTN and/or MK. |
url |
http://europepmc.org/articles/PMC3547881?pdf=render |
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