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A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases

A 15‐kDa lectin, termed SeviL, was isolated from Mytilisepta virgata (purplish bifurcate mussel). SeviL forms a noncovalent dimer that binds strongly to ganglio‐series GM1b oligosaccharide (Neu5Acɑ2‐3Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc) and its precursor, asialo‐GM1 (Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc). SeviL also...

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Autores principales: Fujii, Yuki, Gerdol, Marco, Kawsar, Sarkar M. A., Hasan, Imtiaj, Spazzali, Francesca, Yoshida, Tatsusada, Ogawa, Yukiko, Rajia, Sultana, Kamata, Kenichi, Koide, Yasuhiro, Sugawara, Shigeki, Hosono, Masahiro, Tame, Jeremy R. H., Fujita, Hideaki, Pallavicini, Alberto, Ozeki, Yasuhiro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7317968/
https://www.ncbi.nlm.nih.gov/pubmed/31769916
http://dx.doi.org/10.1111/febs.15154
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author Fujii, Yuki
Gerdol, Marco
Kawsar, Sarkar M. A.
Hasan, Imtiaj
Spazzali, Francesca
Yoshida, Tatsusada
Ogawa, Yukiko
Rajia, Sultana
Kamata, Kenichi
Koide, Yasuhiro
Sugawara, Shigeki
Hosono, Masahiro
Tame, Jeremy R. H.
Fujita, Hideaki
Pallavicini, Alberto
Ozeki, Yasuhiro
author_facet Fujii, Yuki
Gerdol, Marco
Kawsar, Sarkar M. A.
Hasan, Imtiaj
Spazzali, Francesca
Yoshida, Tatsusada
Ogawa, Yukiko
Rajia, Sultana
Kamata, Kenichi
Koide, Yasuhiro
Sugawara, Shigeki
Hosono, Masahiro
Tame, Jeremy R. H.
Fujita, Hideaki
Pallavicini, Alberto
Ozeki, Yasuhiro
author_sort Fujii, Yuki
collection PubMed
description A 15‐kDa lectin, termed SeviL, was isolated from Mytilisepta virgata (purplish bifurcate mussel). SeviL forms a noncovalent dimer that binds strongly to ganglio‐series GM1b oligosaccharide (Neu5Acɑ2‐3Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc) and its precursor, asialo‐GM1 (Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc). SeviL also interacts weakly with the glycan moiety of SSEA‐4 hexaose (Neu5Acα2‐3Galβ1‐3GalNAcβ1‐3Galα1‐4Galβ1‐4Glc). A partial protein sequence of the lectin was determined by mass spectrometry, and the complete sequence was identified from transcriptomic analysis. SeviL, consisting of 129 amino acids, was classified as an R(icin B)‐type lectin, based on the presence of the QxW motif characteristic of this fold. SeviL mRNA is highly expressed in gills and, in particular, mantle rim tissues. Orthologue sequences were identified in other species of the family Mytilidae, including Mytilus galloprovincialis, from which lectin MytiLec‐1 was isolated and characterized in our previous studies. Thus, mytilid species contain lectins belonging to at least two distinct families (R‐type lectins and mytilectins) that have a common β‐trefoil fold structure but differing glycan‐binding specificities. SeviL displayed notable cytotoxic (apoptotic) effects against various cultured cell lines (human breast, ovarian, and colonic cancer; dog kidney) that possess asialo‐GM1 oligosaccharide at the cell surface. This cytotoxic effect was inhibited by the presence of anti‐asialo‐GM1 oligosaccharide antibodies. With HeLa ovarian cancer cells, SeviL showed dose‐ and time‐dependent activation of kinase MKK3/6, p38 MAPK, and caspase‐3/9. The transduction pathways activated by SeviL via the glycosphingolipid oligosaccharide were triggered apoptosis. DATABASE: Nucleotide sequence data have been deposited in the GenBank database under accession numbers MK434191, MK434192, MK434193, MK434194, MK434195, MK434196, MK434197, MK434198, MK434199, MK434200, and MK434201.
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spelling pubmed-73179682020-06-29 A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases Fujii, Yuki Gerdol, Marco Kawsar, Sarkar M. A. Hasan, Imtiaj Spazzali, Francesca Yoshida, Tatsusada Ogawa, Yukiko Rajia, Sultana Kamata, Kenichi Koide, Yasuhiro Sugawara, Shigeki Hosono, Masahiro Tame, Jeremy R. H. Fujita, Hideaki Pallavicini, Alberto Ozeki, Yasuhiro FEBS J Original Articles A 15‐kDa lectin, termed SeviL, was isolated from Mytilisepta virgata (purplish bifurcate mussel). SeviL forms a noncovalent dimer that binds strongly to ganglio‐series GM1b oligosaccharide (Neu5Acɑ2‐3Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc) and its precursor, asialo‐GM1 (Galβ1‐3GalNAcβ1‐4Galβ1‐4Glc). SeviL also interacts weakly with the glycan moiety of SSEA‐4 hexaose (Neu5Acα2‐3Galβ1‐3GalNAcβ1‐3Galα1‐4Galβ1‐4Glc). A partial protein sequence of the lectin was determined by mass spectrometry, and the complete sequence was identified from transcriptomic analysis. SeviL, consisting of 129 amino acids, was classified as an R(icin B)‐type lectin, based on the presence of the QxW motif characteristic of this fold. SeviL mRNA is highly expressed in gills and, in particular, mantle rim tissues. Orthologue sequences were identified in other species of the family Mytilidae, including Mytilus galloprovincialis, from which lectin MytiLec‐1 was isolated and characterized in our previous studies. Thus, mytilid species contain lectins belonging to at least two distinct families (R‐type lectins and mytilectins) that have a common β‐trefoil fold structure but differing glycan‐binding specificities. SeviL displayed notable cytotoxic (apoptotic) effects against various cultured cell lines (human breast, ovarian, and colonic cancer; dog kidney) that possess asialo‐GM1 oligosaccharide at the cell surface. This cytotoxic effect was inhibited by the presence of anti‐asialo‐GM1 oligosaccharide antibodies. With HeLa ovarian cancer cells, SeviL showed dose‐ and time‐dependent activation of kinase MKK3/6, p38 MAPK, and caspase‐3/9. The transduction pathways activated by SeviL via the glycosphingolipid oligosaccharide were triggered apoptosis. DATABASE: Nucleotide sequence data have been deposited in the GenBank database under accession numbers MK434191, MK434192, MK434193, MK434194, MK434195, MK434196, MK434197, MK434198, MK434199, MK434200, and MK434201. John Wiley and Sons Inc. 2019-12-24 2020-06 /pmc/articles/PMC7317968/ /pubmed/31769916 http://dx.doi.org/10.1111/febs.15154 Text en © 2019 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Articles
Fujii, Yuki
Gerdol, Marco
Kawsar, Sarkar M. A.
Hasan, Imtiaj
Spazzali, Francesca
Yoshida, Tatsusada
Ogawa, Yukiko
Rajia, Sultana
Kamata, Kenichi
Koide, Yasuhiro
Sugawara, Shigeki
Hosono, Masahiro
Tame, Jeremy R. H.
Fujita, Hideaki
Pallavicini, Alberto
Ozeki, Yasuhiro
A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title_full A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title_fullStr A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title_full_unstemmed A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title_short A GM1b/asialo‐GM1 oligosaccharide‐binding R‐type lectin from purplish bifurcate mussels Mytilisepta virgata and its effect on MAP kinases
title_sort gm1b/asialo‐gm1 oligosaccharide‐binding r‐type lectin from purplish bifurcate mussels mytilisepta virgata and its effect on map kinases
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7317968/
https://www.ncbi.nlm.nih.gov/pubmed/31769916
http://dx.doi.org/10.1111/febs.15154
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