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Characterisation of novel functionality within the Blastocystis tryptophanase gene

In recent years, the human gut microbiome has been recognised to play a pivotal role in the health of the host. Intestinal homeostasis relies on this intricate and complex relationship between the gut microbiota and the human host. While much effort and attention has been placed on the characterizat...

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Autores principales: Leonardi, Steven Santino, Li, Feng-Jun, Chee, Melissa Su-Juan, Yason, John Anthony, Tay, Hui Yi, Chen, John Yu-Shen, Koh, Eileen Yiling, He, Cynthia Ying-Xin, Tan, Kevin Shyong-Wei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8448343/
https://www.ncbi.nlm.nih.gov/pubmed/34492012
http://dx.doi.org/10.1371/journal.pntd.0009730
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author Leonardi, Steven Santino
Li, Feng-Jun
Chee, Melissa Su-Juan
Yason, John Anthony
Tay, Hui Yi
Chen, John Yu-Shen
Koh, Eileen Yiling
He, Cynthia Ying-Xin
Tan, Kevin Shyong-Wei
author_facet Leonardi, Steven Santino
Li, Feng-Jun
Chee, Melissa Su-Juan
Yason, John Anthony
Tay, Hui Yi
Chen, John Yu-Shen
Koh, Eileen Yiling
He, Cynthia Ying-Xin
Tan, Kevin Shyong-Wei
author_sort Leonardi, Steven Santino
collection PubMed
description In recent years, the human gut microbiome has been recognised to play a pivotal role in the health of the host. Intestinal homeostasis relies on this intricate and complex relationship between the gut microbiota and the human host. While much effort and attention has been placed on the characterization of the organisms that inhabit the gut microbiome, the complex molecular cross-talk between the microbiota could also exert an effect on gastrointestinal conditions. Blastocystis is a single-cell eukaryotic parasite of emerging interest, as its beneficial or pathogenic role in the microbiota has been a subject of contention even to-date. In this study, we assessed the function of the Blastocystis tryptophanase gene (BhTnaA), which was acquired by horizontal gene transfer and likely to be of bacterial origin within Blastocystis. Bioinformatic analysis and phylogenetic reconstruction revealed distinct divergence of BhTnaA versus known bacterial homologs. Despite sharing high homology with the E. coli tryptophanase gene, we show that Blastocystis does not readily convert tryptophan into indole. Instead, BhTnaA preferentially catalyzes the conversion of indole to tryptophan. We also show a direct link between E. coli and Blastocystis tryptophan metabolism: In the presence of E. coli, Blastocystis ST7 is less able to metabolise indole to tryptophan. This study examines the potential for functional variation in horizontally-acquired genes relative to their canonical counterparts, and identifies Blastocystis as a possible producer of tryptophan within the gut.
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spelling pubmed-84483432021-09-18 Characterisation of novel functionality within the Blastocystis tryptophanase gene Leonardi, Steven Santino Li, Feng-Jun Chee, Melissa Su-Juan Yason, John Anthony Tay, Hui Yi Chen, John Yu-Shen Koh, Eileen Yiling He, Cynthia Ying-Xin Tan, Kevin Shyong-Wei PLoS Negl Trop Dis Research Article In recent years, the human gut microbiome has been recognised to play a pivotal role in the health of the host. Intestinal homeostasis relies on this intricate and complex relationship between the gut microbiota and the human host. While much effort and attention has been placed on the characterization of the organisms that inhabit the gut microbiome, the complex molecular cross-talk between the microbiota could also exert an effect on gastrointestinal conditions. Blastocystis is a single-cell eukaryotic parasite of emerging interest, as its beneficial or pathogenic role in the microbiota has been a subject of contention even to-date. In this study, we assessed the function of the Blastocystis tryptophanase gene (BhTnaA), which was acquired by horizontal gene transfer and likely to be of bacterial origin within Blastocystis. Bioinformatic analysis and phylogenetic reconstruction revealed distinct divergence of BhTnaA versus known bacterial homologs. Despite sharing high homology with the E. coli tryptophanase gene, we show that Blastocystis does not readily convert tryptophan into indole. Instead, BhTnaA preferentially catalyzes the conversion of indole to tryptophan. We also show a direct link between E. coli and Blastocystis tryptophan metabolism: In the presence of E. coli, Blastocystis ST7 is less able to metabolise indole to tryptophan. This study examines the potential for functional variation in horizontally-acquired genes relative to their canonical counterparts, and identifies Blastocystis as a possible producer of tryptophan within the gut. Public Library of Science 2021-09-07 /pmc/articles/PMC8448343/ /pubmed/34492012 http://dx.doi.org/10.1371/journal.pntd.0009730 Text en © 2021 Leonardi et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://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
Leonardi, Steven Santino
Li, Feng-Jun
Chee, Melissa Su-Juan
Yason, John Anthony
Tay, Hui Yi
Chen, John Yu-Shen
Koh, Eileen Yiling
He, Cynthia Ying-Xin
Tan, Kevin Shyong-Wei
Characterisation of novel functionality within the Blastocystis tryptophanase gene
title Characterisation of novel functionality within the Blastocystis tryptophanase gene
title_full Characterisation of novel functionality within the Blastocystis tryptophanase gene
title_fullStr Characterisation of novel functionality within the Blastocystis tryptophanase gene
title_full_unstemmed Characterisation of novel functionality within the Blastocystis tryptophanase gene
title_short Characterisation of novel functionality within the Blastocystis tryptophanase gene
title_sort characterisation of novel functionality within the blastocystis tryptophanase gene
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8448343/
https://www.ncbi.nlm.nih.gov/pubmed/34492012
http://dx.doi.org/10.1371/journal.pntd.0009730
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