Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides

Jacob A Mayfield; Sahadevan Raman; Alexandrea K Ramnarine; Vivek K Mishra; Annie D Huang; Sandrine Dudoit; Jeffrey Buter; Tan-Yun Cheng; David C Young; Yashodhan M Nair; Isobel G Ouellet; Braden T Griebel; Shuyi Ma; David R Sherman; Ludovic Mallet; Kyu Y Rhee; Adriaan J Minnaard; D Branch Moody

doi:10.1371/journal.pbio.3002813

Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides

Jacob A Mayfield
, Sahadevan Raman
, Alexandrea K Ramnarine
, Vivek K Mishra
, Annie D Huang
, Sandrine Dudoit
, Jeffrey Buter
, Tan-Yun Cheng
, David C Young
, Yashodhan M Nair
, Isobel G Ouellet
, Braden T Griebel
, Shuyi Ma
, David R Sherman
, Ludovic Mallet
, Kyu Y Rhee
, Adriaan J Minnaard
, D Branch Moody^*

^*Corresponding author for this work

Chemical Biology 2

Research output: Contribution to journal › Article › Academic › peer-review

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87 Downloads (Pure)

Abstract

Mycobacterium tuberculosis (Mtb) releases the unusual terpene nucleoside 1-tuberculosinyladenosine (1-TbAd) to block lysosomal function and promote survival in human macrophages. Using conventional approaches, we found that genes Rv3377c and Rv3378c, but not Rv3376, were necessary for 1-TbAd biosynthesis. Here, we introduce linear models for mass spectrometry (limms) software as a next-generation lipidomics tool to study the essential functions of lipid biosynthetic enzymes on a whole-cell basis. Using limms, whole-cell lipid profiles deepened the phenotypic landscape of comparative mass spectrometry experiments and identified a large family of approximately 100 terpene nucleoside metabolites downstream of Rv3378c. We validated the identity of previously unknown adenine-, adenosine-, and lipid-modified tuberculosinol-containing molecules using synthetic chemistry and collisional mass spectrometry, including comprehensive profiling of bacterial lipids that fragment to adenine. We tracked terpene nucleoside genotypes and lipid phenotypes among Mycobacterium tuberculosis complex (MTC) species that did or did not evolve to productively infect either human or nonhuman mammals. Although 1-TbAd biosynthesis genes were thought to be restricted to the MTC, we identified the locus in unexpected species outside the MTC. Sequence analysis of the locus showed nucleotide usage characteristic of plasmids from plant-associated bacteria, clarifying the origin and timing of horizontal gene transfer to a pre-MTC progenitor. The data demonstrated correlation between high level terpene nucleoside biosynthesis and mycobacterial competence for human infection, and 2 mechanisms of 1-TbAd biosynthesis loss. Overall, the selective gain and evolutionary retention of tuberculosinyl metabolites in modern species that cause human TB suggest a role in human TB disease, and the newly discovered molecules represent candidate disease-specific biomarkers.

Original language	English
Article number	e3002813
Number of pages	24
Journal	PLOS BIOLOGY
Volume	22
Issue number	9
DOIs	https://doi.org/10.1371/journal.pbio.3002813
Publication status	Published - 30-Sept-2024

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Mayfield, J. A., Raman, S., Ramnarine, A. K., Mishra, V. K., Huang, A. D., Dudoit, S., Buter, J., Cheng, T.-Y., Young, D. C., Nair, Y. M., Ouellet, I. G., Griebel, B. T., Ma, S., Sherman, D. R., Mallet, L., Rhee, K. Y., Minnaard, A. J., & Moody, D. B. (2024). Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides. PLOS BIOLOGY, 22(9), Article e3002813. https://doi.org/10.1371/journal.pbio.3002813

@article{d4b13943da4844b3ab84a0a701d6ee51,

title = "Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides",

abstract = "Mycobacterium tuberculosis (Mtb) releases the unusual terpene nucleoside 1-tuberculosinyladenosine (1-TbAd) to block lysosomal function and promote survival in human macrophages. Using conventional approaches, we found that genes Rv3377c and Rv3378c, but not Rv3376, were necessary for 1-TbAd biosynthesis. Here, we introduce linear models for mass spectrometry (limms) software as a next-generation lipidomics tool to study the essential functions of lipid biosynthetic enzymes on a whole-cell basis. Using limms, whole-cell lipid profiles deepened the phenotypic landscape of comparative mass spectrometry experiments and identified a large family of approximately 100 terpene nucleoside metabolites downstream of Rv3378c. We validated the identity of previously unknown adenine-, adenosine-, and lipid-modified tuberculosinol-containing molecules using synthetic chemistry and collisional mass spectrometry, including comprehensive profiling of bacterial lipids that fragment to adenine. We tracked terpene nucleoside genotypes and lipid phenotypes among Mycobacterium tuberculosis complex (MTC) species that did or did not evolve to productively infect either human or nonhuman mammals. Although 1-TbAd biosynthesis genes were thought to be restricted to the MTC, we identified the locus in unexpected species outside the MTC. Sequence analysis of the locus showed nucleotide usage characteristic of plasmids from plant-associated bacteria, clarifying the origin and timing of horizontal gene transfer to a pre-MTC progenitor. The data demonstrated correlation between high level terpene nucleoside biosynthesis and mycobacterial competence for human infection, and 2 mechanisms of 1-TbAd biosynthesis loss. Overall, the selective gain and evolutionary retention of tuberculosinyl metabolites in modern species that cause human TB suggest a role in human TB disease, and the newly discovered molecules represent candidate disease-specific biomarkers.",

author = "Mayfield, \{Jacob A\} and Sahadevan Raman and Ramnarine, \{Alexandrea K\} and Mishra, \{Vivek K\} and Huang, \{Annie D\} and Sandrine Dudoit and Jeffrey Buter and Tan-Yun Cheng and Young, \{David C\} and Nair, \{Yashodhan M\} and Ouellet, \{Isobel G\} and Griebel, \{Braden T\} and Shuyi Ma and Sherman, \{David R\} and Ludovic Mallet and Rhee, \{Kyu Y\} and Minnaard, \{Adriaan J\} and Moody, \{D Branch\}",

note = "Copyright: {\textcopyright} 2024 Mayfield et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.",

year = "2024",

month = sep,

day = "30",

doi = "10.1371/journal.pbio.3002813",

language = "English",

volume = "22",

journal = "PLOS BIOLOGY",

issn = "1544-9173",

publisher = "PUBLIC LIBRARY SCIENCE",

number = "9",

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Mayfield, JA, Raman, S, Ramnarine, AK, Mishra, VK, Huang, AD, Dudoit, S, Buter, J, Cheng, T-Y, Young, DC, Nair, YM, Ouellet, IG, Griebel, BT, Ma, S, Sherman, DR, Mallet, L, Rhee, KY, Minnaard, AJ & Moody, DB 2024, 'Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides', PLOS BIOLOGY, vol. 22, no. 9, e3002813. https://doi.org/10.1371/journal.pbio.3002813

TY - JOUR

T1 - Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides

AU - Mayfield, Jacob A

AU - Raman, Sahadevan

AU - Ramnarine, Alexandrea K

AU - Mishra, Vivek K

AU - Huang, Annie D

AU - Dudoit, Sandrine

AU - Buter, Jeffrey

AU - Cheng, Tan-Yun

AU - Young, David C

AU - Nair, Yashodhan M

AU - Ouellet, Isobel G

AU - Griebel, Braden T

AU - Ma, Shuyi

AU - Sherman, David R

AU - Mallet, Ludovic

AU - Rhee, Kyu Y

AU - Minnaard, Adriaan J

AU - Moody, D Branch

N1 - Copyright: © 2024 Mayfield et al. This is an open access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

PY - 2024/9/30

Y1 - 2024/9/30

N2 - Mycobacterium tuberculosis (Mtb) releases the unusual terpene nucleoside 1-tuberculosinyladenosine (1-TbAd) to block lysosomal function and promote survival in human macrophages. Using conventional approaches, we found that genes Rv3377c and Rv3378c, but not Rv3376, were necessary for 1-TbAd biosynthesis. Here, we introduce linear models for mass spectrometry (limms) software as a next-generation lipidomics tool to study the essential functions of lipid biosynthetic enzymes on a whole-cell basis. Using limms, whole-cell lipid profiles deepened the phenotypic landscape of comparative mass spectrometry experiments and identified a large family of approximately 100 terpene nucleoside metabolites downstream of Rv3378c. We validated the identity of previously unknown adenine-, adenosine-, and lipid-modified tuberculosinol-containing molecules using synthetic chemistry and collisional mass spectrometry, including comprehensive profiling of bacterial lipids that fragment to adenine. We tracked terpene nucleoside genotypes and lipid phenotypes among Mycobacterium tuberculosis complex (MTC) species that did or did not evolve to productively infect either human or nonhuman mammals. Although 1-TbAd biosynthesis genes were thought to be restricted to the MTC, we identified the locus in unexpected species outside the MTC. Sequence analysis of the locus showed nucleotide usage characteristic of plasmids from plant-associated bacteria, clarifying the origin and timing of horizontal gene transfer to a pre-MTC progenitor. The data demonstrated correlation between high level terpene nucleoside biosynthesis and mycobacterial competence for human infection, and 2 mechanisms of 1-TbAd biosynthesis loss. Overall, the selective gain and evolutionary retention of tuberculosinyl metabolites in modern species that cause human TB suggest a role in human TB disease, and the newly discovered molecules represent candidate disease-specific biomarkers.

AB - Mycobacterium tuberculosis (Mtb) releases the unusual terpene nucleoside 1-tuberculosinyladenosine (1-TbAd) to block lysosomal function and promote survival in human macrophages. Using conventional approaches, we found that genes Rv3377c and Rv3378c, but not Rv3376, were necessary for 1-TbAd biosynthesis. Here, we introduce linear models for mass spectrometry (limms) software as a next-generation lipidomics tool to study the essential functions of lipid biosynthetic enzymes on a whole-cell basis. Using limms, whole-cell lipid profiles deepened the phenotypic landscape of comparative mass spectrometry experiments and identified a large family of approximately 100 terpene nucleoside metabolites downstream of Rv3378c. We validated the identity of previously unknown adenine-, adenosine-, and lipid-modified tuberculosinol-containing molecules using synthetic chemistry and collisional mass spectrometry, including comprehensive profiling of bacterial lipids that fragment to adenine. We tracked terpene nucleoside genotypes and lipid phenotypes among Mycobacterium tuberculosis complex (MTC) species that did or did not evolve to productively infect either human or nonhuman mammals. Although 1-TbAd biosynthesis genes were thought to be restricted to the MTC, we identified the locus in unexpected species outside the MTC. Sequence analysis of the locus showed nucleotide usage characteristic of plasmids from plant-associated bacteria, clarifying the origin and timing of horizontal gene transfer to a pre-MTC progenitor. The data demonstrated correlation between high level terpene nucleoside biosynthesis and mycobacterial competence for human infection, and 2 mechanisms of 1-TbAd biosynthesis loss. Overall, the selective gain and evolutionary retention of tuberculosinyl metabolites in modern species that cause human TB suggest a role in human TB disease, and the newly discovered molecules represent candidate disease-specific biomarkers.

U2 - 10.1371/journal.pbio.3002813

DO - 10.1371/journal.pbio.3002813

M3 - Article

C2 - 39348416

SN - 1544-9173

VL - 22

JO - PLOS BIOLOGY

JF - PLOS BIOLOGY

IS - 9

M1 - e3002813

ER -

Mycobacteria that cause tuberculosis have retained ancestrally acquired genes for the biosynthesis of chemically diverse terpene nucleosides

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