Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes

In this report we use ‘high-flux’ tributanoyl-modified N-acetylmannosamine (ManNAc) analogs with natural N-acetyl as well as non-natural azido- and alkyne N-acyl groups (specifically, 1,3,4-O-Bu(3)ManNAc, 1,3,4-O-Bu(3)ManNAz, and 1,3,4-O-Bu(3)ManNAl respectively) to probe intracellular sialic acid m...

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Autores principales: Saeui, Christopher T., Nairn, Alison V., Galizzi, Melina, Douville, Christopher, Gowda, Prateek, Park, Marian, Dharmarha, Vrinda, Shah, Sagar R., Clarke, Amelia, Austin, Melissa, Moremen, Kelley W., Yarema, Kevin J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2018
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5976204/
https://www.ncbi.nlm.nih.gov/pubmed/29847599
http://dx.doi.org/10.1371/journal.pone.0195812
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author Saeui, Christopher T.
Nairn, Alison V.
Galizzi, Melina
Douville, Christopher
Gowda, Prateek
Park, Marian
Dharmarha, Vrinda
Shah, Sagar R.
Clarke, Amelia
Austin, Melissa
Moremen, Kelley W.
Yarema, Kevin J.
author_facet Saeui, Christopher T.
Nairn, Alison V.
Galizzi, Melina
Douville, Christopher
Gowda, Prateek
Park, Marian
Dharmarha, Vrinda
Shah, Sagar R.
Clarke, Amelia
Austin, Melissa
Moremen, Kelley W.
Yarema, Kevin J.
author_sort Saeui, Christopher T.
collection PubMed
description In this report we use ‘high-flux’ tributanoyl-modified N-acetylmannosamine (ManNAc) analogs with natural N-acetyl as well as non-natural azido- and alkyne N-acyl groups (specifically, 1,3,4-O-Bu(3)ManNAc, 1,3,4-O-Bu(3)ManNAz, and 1,3,4-O-Bu(3)ManNAl respectively) to probe intracellular sialic acid metabolism in the near-normal MCF10A human breast cell line in comparison with earlier stage T-47D and more advanced stage MDA-MB-231 breast cancer lines. An integrated view of sialic acid metabolism was gained by measuring intracellular sialic acid production in tandem with transcriptional profiling of genes linked to sialic acid metabolism. The transcriptional profiling showed several differences between the three lines in the absence of ManNAc analog supplementation that helps explain the different sialoglycan profiles naturally associated with cancer. Only minor changes in mRNA transcript levels occurred upon exposure to the compounds confirming that metabolic flux alone can be a key determinant of sialoglycoconjugate display in breast cancer cells; this result complements the well-established role of genetic control (e.g., the transcription of STs) of sialylation abnormalities ubiquitously associated with cancer. A notable result was that the different cell lines produced significantly different levels of sialic acid upon exogenous ManNAc supplementation, indicating that feedback inhibition of UDP-GlcNAc 2-epimerase/ManNAc kinase (GNE)—generally regarded as the ‘gatekeeper’ enzyme for titering flux into sialic acid biosynthesis—is not the only regulatory mechanism that limits production of this sugar. A notable aspect of our metabolic glycoengineering approach is its ability to discriminate cell subtype based on intracellular metabolism by illuminating otherwise hidden cell type-specific features. We believe that this strategy combined with multi-dimensional analysis of sialic acid metabolism will ultimately provide novel insights into breast cancer subtypes and provide a foundation for new methods of diagnosis.
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spelling pubmed-59762042018-06-17 Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes Saeui, Christopher T. Nairn, Alison V. Galizzi, Melina Douville, Christopher Gowda, Prateek Park, Marian Dharmarha, Vrinda Shah, Sagar R. Clarke, Amelia Austin, Melissa Moremen, Kelley W. Yarema, Kevin J. PLoS One Research Article In this report we use ‘high-flux’ tributanoyl-modified N-acetylmannosamine (ManNAc) analogs with natural N-acetyl as well as non-natural azido- and alkyne N-acyl groups (specifically, 1,3,4-O-Bu(3)ManNAc, 1,3,4-O-Bu(3)ManNAz, and 1,3,4-O-Bu(3)ManNAl respectively) to probe intracellular sialic acid metabolism in the near-normal MCF10A human breast cell line in comparison with earlier stage T-47D and more advanced stage MDA-MB-231 breast cancer lines. An integrated view of sialic acid metabolism was gained by measuring intracellular sialic acid production in tandem with transcriptional profiling of genes linked to sialic acid metabolism. The transcriptional profiling showed several differences between the three lines in the absence of ManNAc analog supplementation that helps explain the different sialoglycan profiles naturally associated with cancer. Only minor changes in mRNA transcript levels occurred upon exposure to the compounds confirming that metabolic flux alone can be a key determinant of sialoglycoconjugate display in breast cancer cells; this result complements the well-established role of genetic control (e.g., the transcription of STs) of sialylation abnormalities ubiquitously associated with cancer. A notable result was that the different cell lines produced significantly different levels of sialic acid upon exogenous ManNAc supplementation, indicating that feedback inhibition of UDP-GlcNAc 2-epimerase/ManNAc kinase (GNE)—generally regarded as the ‘gatekeeper’ enzyme for titering flux into sialic acid biosynthesis—is not the only regulatory mechanism that limits production of this sugar. A notable aspect of our metabolic glycoengineering approach is its ability to discriminate cell subtype based on intracellular metabolism by illuminating otherwise hidden cell type-specific features. We believe that this strategy combined with multi-dimensional analysis of sialic acid metabolism will ultimately provide novel insights into breast cancer subtypes and provide a foundation for new methods of diagnosis. Public Library of Science 2018-05-30 /pmc/articles/PMC5976204/ /pubmed/29847599 http://dx.doi.org/10.1371/journal.pone.0195812 Text en © 2018 Saeui et al http://creativecommons.org/licenses/by/4.0/ This is an open access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Saeui, Christopher T.
Nairn, Alison V.
Galizzi, Melina
Douville, Christopher
Gowda, Prateek
Park, Marian
Dharmarha, Vrinda
Shah, Sagar R.
Clarke, Amelia
Austin, Melissa
Moremen, Kelley W.
Yarema, Kevin J.
Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title_full Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title_fullStr Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title_full_unstemmed Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title_short Integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
title_sort integration of genetic and metabolic features related to sialic acid metabolism distinguishes human breast cell subtypes
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5976204/
https://www.ncbi.nlm.nih.gov/pubmed/29847599
http://dx.doi.org/10.1371/journal.pone.0195812
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