A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation

Helicobacter pylori colonizes the stomach of half of the human population. Most H. pylori are located in the mucus layer, which is mainly comprised by glycosylated mucins. Using mass spectrometry, we identified 631 glycans (whereof 145 were fully characterized and the remainder assigned as compositi...

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Autores principales: Chahal, Gurdeep, Padra, Médea, Erhardsson, Mattias, Jin, Chunsheng, Quintana-Hayashi, Macarena, Venkatakrishnan, Vignesh, Padra, János Tamás, Stenbäck, Helen, Thorell, Anders, Karlsson, Niclas G., Lindén, Sara K.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Biochemistry and Molecular Biology 2022
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9661725/
https://www.ncbi.nlm.nih.gov/pubmed/36182101
http://dx.doi.org/10.1016/j.mcpro.2022.100421
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author Chahal, Gurdeep
Padra, Médea
Erhardsson, Mattias
Jin, Chunsheng
Quintana-Hayashi, Macarena
Venkatakrishnan, Vignesh
Padra, János Tamás
Stenbäck, Helen
Thorell, Anders
Karlsson, Niclas G.
Lindén, Sara K.
author_facet Chahal, Gurdeep
Padra, Médea
Erhardsson, Mattias
Jin, Chunsheng
Quintana-Hayashi, Macarena
Venkatakrishnan, Vignesh
Padra, János Tamás
Stenbäck, Helen
Thorell, Anders
Karlsson, Niclas G.
Lindén, Sara K.
author_sort Chahal, Gurdeep
collection PubMed
description Helicobacter pylori colonizes the stomach of half of the human population. Most H. pylori are located in the mucus layer, which is mainly comprised by glycosylated mucins. Using mass spectrometry, we identified 631 glycans (whereof 145 were fully characterized and the remainder assigned as compositions) on mucins isolated from 14 Helicobacter spp.-infected and 14 Helicobacter spp.-noninfected stomachs. Only six identified glycans were common to all individuals, from a total of 60 to 189 glycans in each individual. An increased number of unique glycan structures together with an increased intraindividual diversity and larger interindividual variation were identified among O-glycans from Helicobacter spp.-infected stomachs compared with noninfected stomachs. H. pylori strain J99, which carries the blood group antigen–binding adhesin (BabA), the sialic acid–binding adhesin (SabA), and the LacdiNAc-binding adhesin, bound both to Lewis b (Leb)-positive and Leb-negative mucins. Among Leb-positive mucins, H. pylori J99 binding was higher to mucins from Helicobacter spp.-infected individuals than noninfected individuals. Statistical correlation analysis, binding experiments with J99 wt, and J99ΔbabAΔsabA and inhibition experiments using synthetic glycoconjugates demonstrated that the differences in H. pylori-binding ability among these four groups were governed by BabA-dependent binding to fucosylated structures. LacdiNAc levels were lower in mucins that bound to J99 lacking BabA and SabA than in mucins that did not, suggesting that LacdiNAc did not significantly contribute to the binding. We identified 24 O-glycans from Leb-negative mucins that correlated well with H. pylori binding whereof 23 contained α1,2-linked fucosylation. The large and diverse gastric glycan library identified, including structures that correlated with H. pylori binding, could be used to select glycodeterminants to experimentally investigate further for their importance in host–pathogen interactions and as candidates to develop glycan-based therapies.
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spelling pubmed-96617252022-11-14 A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation Chahal, Gurdeep Padra, Médea Erhardsson, Mattias Jin, Chunsheng Quintana-Hayashi, Macarena Venkatakrishnan, Vignesh Padra, János Tamás Stenbäck, Helen Thorell, Anders Karlsson, Niclas G. Lindén, Sara K. Mol Cell Proteomics Research Helicobacter pylori colonizes the stomach of half of the human population. Most H. pylori are located in the mucus layer, which is mainly comprised by glycosylated mucins. Using mass spectrometry, we identified 631 glycans (whereof 145 were fully characterized and the remainder assigned as compositions) on mucins isolated from 14 Helicobacter spp.-infected and 14 Helicobacter spp.-noninfected stomachs. Only six identified glycans were common to all individuals, from a total of 60 to 189 glycans in each individual. An increased number of unique glycan structures together with an increased intraindividual diversity and larger interindividual variation were identified among O-glycans from Helicobacter spp.-infected stomachs compared with noninfected stomachs. H. pylori strain J99, which carries the blood group antigen–binding adhesin (BabA), the sialic acid–binding adhesin (SabA), and the LacdiNAc-binding adhesin, bound both to Lewis b (Leb)-positive and Leb-negative mucins. Among Leb-positive mucins, H. pylori J99 binding was higher to mucins from Helicobacter spp.-infected individuals than noninfected individuals. Statistical correlation analysis, binding experiments with J99 wt, and J99ΔbabAΔsabA and inhibition experiments using synthetic glycoconjugates demonstrated that the differences in H. pylori-binding ability among these four groups were governed by BabA-dependent binding to fucosylated structures. LacdiNAc levels were lower in mucins that bound to J99 lacking BabA and SabA than in mucins that did not, suggesting that LacdiNAc did not significantly contribute to the binding. We identified 24 O-glycans from Leb-negative mucins that correlated well with H. pylori binding whereof 23 contained α1,2-linked fucosylation. The large and diverse gastric glycan library identified, including structures that correlated with H. pylori binding, could be used to select glycodeterminants to experimentally investigate further for their importance in host–pathogen interactions and as candidates to develop glycan-based therapies. American Society for Biochemistry and Molecular Biology 2022-09-29 /pmc/articles/PMC9661725/ /pubmed/36182101 http://dx.doi.org/10.1016/j.mcpro.2022.100421 Text en © 2022 The Authors https://creativecommons.org/licenses/by/4.0/This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Research
Chahal, Gurdeep
Padra, Médea
Erhardsson, Mattias
Jin, Chunsheng
Quintana-Hayashi, Macarena
Venkatakrishnan, Vignesh
Padra, János Tamás
Stenbäck, Helen
Thorell, Anders
Karlsson, Niclas G.
Lindén, Sara K.
A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title_full A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title_fullStr A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title_full_unstemmed A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title_short A Complex Connection Between the Diversity of Human Gastric Mucin O-Glycans, Helicobacter pylori Binding, Helicobacter Infection and Fucosylation
title_sort complex connection between the diversity of human gastric mucin o-glycans, helicobacter pylori binding, helicobacter infection and fucosylation
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9661725/
https://www.ncbi.nlm.nih.gov/pubmed/36182101
http://dx.doi.org/10.1016/j.mcpro.2022.100421
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