Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria

Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria

ABSTRACT Most mycolic acid-containing actinobacteria and some proteobacteria use steroids as growth substrates, but the catabolism of the last two steroid rings has yet to be elucidated. In Mycobacterium tuberculosis, this pathway includes virulence determinants and has been proposed to be encoded b...

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Autores principales: Adam M. Crowe, Israël Casabon, Kirstin L. Brown, Jie Liu, Jennifer Lian, Jason C. Rogalski, Timothy E. Hurst, Victor Snieckus, Leonard J. Foster, Lindsay D. Eltis
Formato: article
Lenguaje:EN
Publicado: American Society for Microbiology 2017
Materias:
CoA thioester
Mycobacterium tuberculosis
catabolism
cholesterol
ring opening
Microbiology
QR1-502
Acceso en línea:https://doaj.org/article/8a695f8dfbf74f748bcfad84bcde434f
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spelling oai:doaj.org-article:8a695f8dfbf74f748bcfad84bcde434f2021-11-15T15:50:59ZCatabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria10.1128/mBio.00321-172150-7511https://doaj.org/article/8a695f8dfbf74f748bcfad84bcde434f2017-05-01T00:00:00Zhttps://journals.asm.org/doi/10.1128/mBio.00321-17https://doaj.org/toc/2150-7511ABSTRACT Most mycolic acid-containing actinobacteria and some proteobacteria use steroids as growth substrates, but the catabolism of the last two steroid rings has yet to be elucidated. In Mycobacterium tuberculosis, this pathway includes virulence determinants and has been proposed to be encoded by the KstR2-regulated genes, which include a predicted coenzyme A (CoA) transferase gene (ipdAB) and an acyl-CoA reductase gene (ipdC). In the presence of cholesterol, ΔipdC and ΔipdAB mutants of either M. tuberculosis or Rhodococcus jostii strain RHA1 accumulated previously undescribed metabolites: 3aα-H-4α(carboxyl-CoA)-5-hydroxy-7aβ-methylhexahydro-1-indanone (5-OH HIC-CoA) and (R)-2-(2-carboxyethyl)-3-methyl-6-oxocyclohex-1-ene-1-carboxyl-CoA (COCHEA-CoA), respectively. A ΔfadE32 mutant of Mycobacterium smegmatis accumulated 4-methyl-5-oxo-octanedioic acid (MOODA). Incubation of synthetic 5-OH HIC-CoA with purified IpdF, IpdC, and enoyl-CoA hydratase 20 (EchA20), a crotonase superfamily member, yielded COCHEA-CoA and, upon further incubation with IpdAB and a CoA thiolase, yielded MOODA-CoA. Based on these studies, we propose a pathway for the final steps of steroid catabolism in which the 5-member ring is hydrolyzed by EchA20, followed by hydrolysis of the 6-member ring by IpdAB. Metabolites accumulated by ΔipdF and ΔechA20 mutants support the model. The conservation of these genes in known steroid-degrading bacteria suggests that the pathway is shared. This pathway further predicts that cholesterol catabolism yields four propionyl-CoAs, four acetyl-CoAs, one pyruvate, and one succinyl-CoA. Finally, a ΔipdAB M. tuberculosis mutant did not survive in macrophages and displayed severely depleted CoASH levels that correlated with a cholesterol-dependent toxicity. Our results together with the developed tools provide a basis for further elucidating bacterial steroid catabolism and virulence determinants in M. tuberculosis. IMPORTANCE Bacteria are the only known steroid degraders, but the pathway responsible for degrading the last two steroid rings has yet to be elucidated. In Mycobacterium tuberculosis, this pathway includes virulence determinants. Using a series of mutants in M. tuberculosis and related bacteria, we identified a number of novel CoA thioesters as pathway intermediates. Analysis of the metabolites combined with enzymological studies establishes how the last two steroid rings are hydrolytically opened by enzymes encoded by the KstR2 regulon. Our results provide experimental evidence for novel ring-degrading enzymes, significantly advance our understanding of bacterial steroid catabolism, and identify a previously uncharacterized cholesterol-dependent toxicity that may facilitate the development of novel tuberculosis therapeutics.Adam M. CroweIsraël CasabonKirstin L. BrownJie LiuJennifer LianJason C. RogalskiTimothy E. HurstVictor SnieckusLeonard J. FosterLindsay D. EltisAmerican Society for MicrobiologyarticleCoA thioesterMycobacterium tuberculosiscatabolismcholesterolring openingMicrobiologyQR1-502ENmBio, Vol 8, Iss 2 (2017)
institution DOAJ
collection DOAJ
language EN
topic CoA thioester
Mycobacterium tuberculosis
catabolism
cholesterol
ring opening
Microbiology
QR1-502
spellingShingle CoA thioester
Mycobacterium tuberculosis
catabolism
cholesterol
ring opening
Microbiology
QR1-502
Adam M. Crowe
Israël Casabon
Kirstin L. Brown
Jie Liu
Jennifer Lian
Jason C. Rogalski
Timothy E. Hurst
Victor Snieckus
Leonard J. Foster
Lindsay D. Eltis
Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
description ABSTRACT Most mycolic acid-containing actinobacteria and some proteobacteria use steroids as growth substrates, but the catabolism of the last two steroid rings has yet to be elucidated. In Mycobacterium tuberculosis, this pathway includes virulence determinants and has been proposed to be encoded by the KstR2-regulated genes, which include a predicted coenzyme A (CoA) transferase gene (ipdAB) and an acyl-CoA reductase gene (ipdC). In the presence of cholesterol, ΔipdC and ΔipdAB mutants of either M. tuberculosis or Rhodococcus jostii strain RHA1 accumulated previously undescribed metabolites: 3aα-H-4α(carboxyl-CoA)-5-hydroxy-7aβ-methylhexahydro-1-indanone (5-OH HIC-CoA) and (R)-2-(2-carboxyethyl)-3-methyl-6-oxocyclohex-1-ene-1-carboxyl-CoA (COCHEA-CoA), respectively. A ΔfadE32 mutant of Mycobacterium smegmatis accumulated 4-methyl-5-oxo-octanedioic acid (MOODA). Incubation of synthetic 5-OH HIC-CoA with purified IpdF, IpdC, and enoyl-CoA hydratase 20 (EchA20), a crotonase superfamily member, yielded COCHEA-CoA and, upon further incubation with IpdAB and a CoA thiolase, yielded MOODA-CoA. Based on these studies, we propose a pathway for the final steps of steroid catabolism in which the 5-member ring is hydrolyzed by EchA20, followed by hydrolysis of the 6-member ring by IpdAB. Metabolites accumulated by ΔipdF and ΔechA20 mutants support the model. The conservation of these genes in known steroid-degrading bacteria suggests that the pathway is shared. This pathway further predicts that cholesterol catabolism yields four propionyl-CoAs, four acetyl-CoAs, one pyruvate, and one succinyl-CoA. Finally, a ΔipdAB M. tuberculosis mutant did not survive in macrophages and displayed severely depleted CoASH levels that correlated with a cholesterol-dependent toxicity. Our results together with the developed tools provide a basis for further elucidating bacterial steroid catabolism and virulence determinants in M. tuberculosis. IMPORTANCE Bacteria are the only known steroid degraders, but the pathway responsible for degrading the last two steroid rings has yet to be elucidated. In Mycobacterium tuberculosis, this pathway includes virulence determinants. Using a series of mutants in M. tuberculosis and related bacteria, we identified a number of novel CoA thioesters as pathway intermediates. Analysis of the metabolites combined with enzymological studies establishes how the last two steroid rings are hydrolytically opened by enzymes encoded by the KstR2 regulon. Our results provide experimental evidence for novel ring-degrading enzymes, significantly advance our understanding of bacterial steroid catabolism, and identify a previously uncharacterized cholesterol-dependent toxicity that may facilitate the development of novel tuberculosis therapeutics.
format article
author Adam M. Crowe
Israël Casabon
Kirstin L. Brown
Jie Liu
Jennifer Lian
Jason C. Rogalski
Timothy E. Hurst
Victor Snieckus
Leonard J. Foster
Lindsay D. Eltis
author_facet Adam M. Crowe
Israël Casabon
Kirstin L. Brown
Jie Liu
Jennifer Lian
Jason C. Rogalski
Timothy E. Hurst
Victor Snieckus
Leonard J. Foster
Lindsay D. Eltis
author_sort Adam M. Crowe
title Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
title_short Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
title_full Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
title_fullStr Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
title_full_unstemmed Catabolism of the Last Two Steroid Rings in <italic toggle="yes">Mycobacterium tuberculosis</italic> and Other Bacteria
title_sort catabolism of the last two steroid rings in <italic toggle="yes">mycobacterium tuberculosis</italic> and other bacteria
publisher American Society for Microbiology
publishDate 2017
url https://doaj.org/article/8a695f8dfbf74f748bcfad84bcde434f
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