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Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants

SRL is a cell wall associated developmental-stage specific lectin secreted by Sclerotium rolfsii, a soil-born pathogenic fungus. SRL displays specificity for TF antigen (Galβ1→3GalNAc-α-Ser//Thr) expressed in all cancer types and has tumour suppressing effects in vivo. Considering the immense potent...

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Autores principales: Peppa, Vassiliki I., Venkat, Hemalatha, Kantsadi, Anastassia L., Inamdar, Shashikala R., Bhat, Ganapati G., Eligar, Sachin, Shivanand, Anupama, Chachadi, Vishwanath B., Satisha, Gonchigar J., Swamy, Bale M., Skamnaki, Vassiliki T., Zographos, Spyridon E., Leonidas, Demetres D.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6272482/
https://www.ncbi.nlm.nih.gov/pubmed/26076107
http://dx.doi.org/10.3390/molecules200610848
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author Peppa, Vassiliki I.
Venkat, Hemalatha
Kantsadi, Anastassia L.
Inamdar, Shashikala R.
Bhat, Ganapati G.
Eligar, Sachin
Shivanand, Anupama
Chachadi, Vishwanath B.
Satisha, Gonchigar J.
Swamy, Bale M.
Skamnaki, Vassiliki T.
Zographos, Spyridon E.
Leonidas, Demetres D.
author_facet Peppa, Vassiliki I.
Venkat, Hemalatha
Kantsadi, Anastassia L.
Inamdar, Shashikala R.
Bhat, Ganapati G.
Eligar, Sachin
Shivanand, Anupama
Chachadi, Vishwanath B.
Satisha, Gonchigar J.
Swamy, Bale M.
Skamnaki, Vassiliki T.
Zographos, Spyridon E.
Leonidas, Demetres D.
author_sort Peppa, Vassiliki I.
collection PubMed
description SRL is a cell wall associated developmental-stage specific lectin secreted by Sclerotium rolfsii, a soil-born pathogenic fungus. SRL displays specificity for TF antigen (Galβ1→3GalNAc-α-Ser//Thr) expressed in all cancer types and has tumour suppressing effects in vivo. Considering the immense potential of SRL in cancer research, we have generated two variant gene constructs of SRL and expressed in E. coli to refine the sugar specificity and solubility by altering the surface charge. SSR1 and SSR2 are two different recombinant variants of SRL, both of which recognize TF antigen but only SSR1 binds to Tn antigen (GalNAcα-Ser/Thr). The glycan array analysis of the variants demonstrated that SSR1 recognizes TF antigen and their derivative with high affinity similar to SRL but showed highest affinity towards the sialylated Tn antigen, unlike SRL. The carbohydrate binding property of SSR2 remains unaltered compared to SRL. The crystal structures of the two variants were determined in free form and in complex with N-acetylglucosamine at 1.7 Å and 1.6 Å resolution, respectively. Structural analysis highlighted the structural basis of the fine carbohydrate specificity of the two SRL variants and results are in agreement with glycan array analysis.
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spelling pubmed-62724822018-12-31 Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants Peppa, Vassiliki I. Venkat, Hemalatha Kantsadi, Anastassia L. Inamdar, Shashikala R. Bhat, Ganapati G. Eligar, Sachin Shivanand, Anupama Chachadi, Vishwanath B. Satisha, Gonchigar J. Swamy, Bale M. Skamnaki, Vassiliki T. Zographos, Spyridon E. Leonidas, Demetres D. Molecules Article SRL is a cell wall associated developmental-stage specific lectin secreted by Sclerotium rolfsii, a soil-born pathogenic fungus. SRL displays specificity for TF antigen (Galβ1→3GalNAc-α-Ser//Thr) expressed in all cancer types and has tumour suppressing effects in vivo. Considering the immense potential of SRL in cancer research, we have generated two variant gene constructs of SRL and expressed in E. coli to refine the sugar specificity and solubility by altering the surface charge. SSR1 and SSR2 are two different recombinant variants of SRL, both of which recognize TF antigen but only SSR1 binds to Tn antigen (GalNAcα-Ser/Thr). The glycan array analysis of the variants demonstrated that SSR1 recognizes TF antigen and their derivative with high affinity similar to SRL but showed highest affinity towards the sialylated Tn antigen, unlike SRL. The carbohydrate binding property of SSR2 remains unaltered compared to SRL. The crystal structures of the two variants were determined in free form and in complex with N-acetylglucosamine at 1.7 Å and 1.6 Å resolution, respectively. Structural analysis highlighted the structural basis of the fine carbohydrate specificity of the two SRL variants and results are in agreement with glycan array analysis. MDPI 2015-06-12 /pmc/articles/PMC6272482/ /pubmed/26076107 http://dx.doi.org/10.3390/molecules200610848 Text en © 2015 by the authors. Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Peppa, Vassiliki I.
Venkat, Hemalatha
Kantsadi, Anastassia L.
Inamdar, Shashikala R.
Bhat, Ganapati G.
Eligar, Sachin
Shivanand, Anupama
Chachadi, Vishwanath B.
Satisha, Gonchigar J.
Swamy, Bale M.
Skamnaki, Vassiliki T.
Zographos, Spyridon E.
Leonidas, Demetres D.
Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title_full Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title_fullStr Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title_full_unstemmed Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title_short Molecular Cloning, Carbohydrate Specificity and the Crystal Structure of Two Sclerotium rolfsii Lectin Variants
title_sort molecular cloning, carbohydrate specificity and the crystal structure of two sclerotium rolfsii lectin variants
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6272482/
https://www.ncbi.nlm.nih.gov/pubmed/26076107
http://dx.doi.org/10.3390/molecules200610848
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