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Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria

BACKGROUND: A central tenet in biochemistry for over 50 years has held that microorganisms, plants and, more recently, certain apicomplexan parasites synthesize essential aromatic compounds via elaboration of a complete shikimic acid pathway, whereas metazoans lacking this pathway require a dietary...

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Autores principales: Zucko, Jurica, Dunlap, Walter C, Shick, J Malcolm, Cullum, John, Cercelet, François, Amin, Bijal, Hammen, Lena, Lau, Timothy, Williams, Jamal, Hranueli, Daslav, Long, Paul F
Formato: Texto
Lenguaje:English
Publicado: BioMed Central 2010
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3018139/
https://www.ncbi.nlm.nih.gov/pubmed/21070645
http://dx.doi.org/10.1186/1471-2164-11-628
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author Zucko, Jurica
Dunlap, Walter C
Shick, J Malcolm
Cullum, John
Cercelet, François
Amin, Bijal
Hammen, Lena
Lau, Timothy
Williams, Jamal
Hranueli, Daslav
Long, Paul F
author_facet Zucko, Jurica
Dunlap, Walter C
Shick, J Malcolm
Cullum, John
Cercelet, François
Amin, Bijal
Hammen, Lena
Lau, Timothy
Williams, Jamal
Hranueli, Daslav
Long, Paul F
author_sort Zucko, Jurica
collection PubMed
description BACKGROUND: A central tenet in biochemistry for over 50 years has held that microorganisms, plants and, more recently, certain apicomplexan parasites synthesize essential aromatic compounds via elaboration of a complete shikimic acid pathway, whereas metazoans lacking this pathway require a dietary source of these compounds. The large number of sequenced bacterial and archaean genomes now available for comparative genomic analyses allows the fundamentals of this contention to be tested in prokaryotes. Using Hidden Markov Model profiles (HMM profiles) to identify all known enzymes of the pathway, we report the presence of genes encoding shikimate pathway enzymes in the hypothetical proteomes constructed from the genomes of 488 sequenced prokaryotes. RESULTS: Amongst free-living prokaryotes most Bacteria possess, as expected, genes encoding a complete shikimic acid pathway, whereas of the culturable Archaea, only one was found to have a complete complement of recognisable enzymes in its predicted proteome. It may be that in the Archaea, the primary amino-acid sequences of enzymes of the pathway are highly divergent and so are not detected by HMM profiles. Alternatively, structurally unrelated (non-orthologous) proteins might be performing the same biochemical functions as those encoding recognized genes of the shikimate pathway. Most surprisingly, 30% of host-associated (mutualistic, commensal and pathogenic) bacteria likewise do not possess a complete shikimic acid pathway. Many of these microbes show some degree of genome reduction, suggesting that these host-associated bacteria might sequester essential aromatic compounds from a parasitised host, as a 'shared metabolic adaptation' in mutualistic symbiosis, or obtain them from other consorts having the complete biosynthetic pathway. The HMM results gave 84% agreement when compared against data in the highly curated BioCyc reference database of genomes and metabolic pathways. CONCLUSIONS: These results challenge the conventional belief that the shikimic acid pathway is universal and essential in prokaryotes. The possibilities that non-orthologous enzymes catalyse reactions in this pathway (especially in the Archaea), or that there exist specific uptake mechanisms for the acquisition of shikimate intermediates or essential pathway products, warrant further examination to better understand the precise metabolic attributes of host-beneficial and pathogenic bacteria.
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spelling pubmed-30181392011-01-10 Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria Zucko, Jurica Dunlap, Walter C Shick, J Malcolm Cullum, John Cercelet, François Amin, Bijal Hammen, Lena Lau, Timothy Williams, Jamal Hranueli, Daslav Long, Paul F BMC Genomics Research Article BACKGROUND: A central tenet in biochemistry for over 50 years has held that microorganisms, plants and, more recently, certain apicomplexan parasites synthesize essential aromatic compounds via elaboration of a complete shikimic acid pathway, whereas metazoans lacking this pathway require a dietary source of these compounds. The large number of sequenced bacterial and archaean genomes now available for comparative genomic analyses allows the fundamentals of this contention to be tested in prokaryotes. Using Hidden Markov Model profiles (HMM profiles) to identify all known enzymes of the pathway, we report the presence of genes encoding shikimate pathway enzymes in the hypothetical proteomes constructed from the genomes of 488 sequenced prokaryotes. RESULTS: Amongst free-living prokaryotes most Bacteria possess, as expected, genes encoding a complete shikimic acid pathway, whereas of the culturable Archaea, only one was found to have a complete complement of recognisable enzymes in its predicted proteome. It may be that in the Archaea, the primary amino-acid sequences of enzymes of the pathway are highly divergent and so are not detected by HMM profiles. Alternatively, structurally unrelated (non-orthologous) proteins might be performing the same biochemical functions as those encoding recognized genes of the shikimate pathway. Most surprisingly, 30% of host-associated (mutualistic, commensal and pathogenic) bacteria likewise do not possess a complete shikimic acid pathway. Many of these microbes show some degree of genome reduction, suggesting that these host-associated bacteria might sequester essential aromatic compounds from a parasitised host, as a 'shared metabolic adaptation' in mutualistic symbiosis, or obtain them from other consorts having the complete biosynthetic pathway. The HMM results gave 84% agreement when compared against data in the highly curated BioCyc reference database of genomes and metabolic pathways. CONCLUSIONS: These results challenge the conventional belief that the shikimic acid pathway is universal and essential in prokaryotes. The possibilities that non-orthologous enzymes catalyse reactions in this pathway (especially in the Archaea), or that there exist specific uptake mechanisms for the acquisition of shikimate intermediates or essential pathway products, warrant further examination to better understand the precise metabolic attributes of host-beneficial and pathogenic bacteria. BioMed Central 2010-11-11 /pmc/articles/PMC3018139/ /pubmed/21070645 http://dx.doi.org/10.1186/1471-2164-11-628 Text en Copyright ©2010 Zucko et al; licensee BioMed Central Ltd. http://creativecommons.org/licenses/by/2.0 This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/2.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Zucko, Jurica
Dunlap, Walter C
Shick, J Malcolm
Cullum, John
Cercelet, François
Amin, Bijal
Hammen, Lena
Lau, Timothy
Williams, Jamal
Hranueli, Daslav
Long, Paul F
Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title_full Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title_fullStr Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title_full_unstemmed Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title_short Global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
title_sort global genome analysis of the shikimic acid pathway reveals greater gene loss in host-associated than in free-living bacteria
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3018139/
https://www.ncbi.nlm.nih.gov/pubmed/21070645
http://dx.doi.org/10.1186/1471-2164-11-628
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