An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection

Susanna Commandeur; Krista E. Van Meijgaarden; Corine Prins; Alexander V. Pichugin; Karin Dijkman; Susan J.F. Van Den Eeden; Annemieke H. Friggen; Kees L.M.C. Franken; Gregory Dolganov; Igor Kramnik; Gary K. Schoolnik; Fredrik Oftung; Gro Ellen Korsvold; Annemieke Geluk; Tom H.M. Ottenhoff

doi:10.4049/jimmunol.1201593

An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection

Susanna Commandeur
, Krista E. Van Meijgaarden
, Corine Prins
, Alexander V. Pichugin
, Karin Dijkman
, Susan J.F. Van Den Eeden
, Annemieke H. Friggen
, Kees L.M.C. Franken
, Gregory Dolganov
, Igor Kramnik
, Gary K. Schoolnik
, Fredrik Oftung
, Gro Ellen Korsvold
, Annemieke Geluk
, Tom H.M. Ottenhoff^*

^*Corresponding author for this work

Affiliatie VU

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

Abstract

Mycobacterium tuberculosis is responsible for almost 2 million deaths annually. Mycobacterium bovis bacillus Calmette-Guérin, the only vaccine available against tuberculosis (TB), induces highly variable protection against TB, and better TB vaccines are urgently needed. A prerequisite for candidate vaccine Ags is that they are immunogenic and expressed by M. tuberculosis during infection of the primary target organ, that is, the lungs of susceptible individuals. In search of new TB vaccine candidate Ags, we have used a genome-wide, unbiased Ag discovery approach to investigate the in vivo expression of 2170 M. tuberculosis genes during M. tuberculosis infection in the lungs of mice. Four genetically related but distinct mouse strains were studied, representing a spectrum of TB susceptibility controlled by the supersusceptibility to TB 1 locus. We used stringent selection approaches to select in vivo-expressed M. tuberculosis (IVE-TB) genes and analyzed their expression patterns in distinct disease phenotypes such as necrosis and granuloma formation. To study the vaccine potential of these proteins, we analyzed their immunogenicity. Several M. tuberculosis proteins were recognized by immune cells from tuberculin skin test-positive, ESAT6/CFP10-responsive individuals, indicating that these Ags are presented during natural M. tuberculosis infection. Furthermore, TB patients also showed responses toward IVE-TB Ags, albeit lower than tuberculin skin test-positive, ESAT6/CFP10-responsive individuals. Finally, IVETB Ags induced strong IFN-γ⁺/TNF-α⁺ CD8⁺ and TNF-α⁺/IL-2⁺ CD154⁺/CD4⁺ T cell responses in PBMC from long-term latently M. tuberculosis-infected individuals. In conclusion, these IVE-TB Ags are expressed during pulmonary infection in vivo, are immunogenic, induce strong T cell responses in long-term latently M. tuberculosis-infected individuals, and may therefore represent attractive Ags for new TB vaccines.

Original language	English
Pages (from-to)	1659-1671
Number of pages	13
Journal	Journal of Immunology
Volume	190
Issue number	4
DOIs	https://doi.org/10.4049/jimmunol.1201593
Publication status	Published - 15 Feb 2013

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10.4049/jimmunol.1201593

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Commandeur, S., Van Meijgaarden, K. E., Prins, C., Pichugin, A. V., Dijkman, K., Van Den Eeden, S. J. F., Friggen, A. H., Franken, K. L. M. C., Dolganov, G., Kramnik, I., Schoolnik, G. K., Oftung, F., Korsvold, G. E., Geluk, A., & Ottenhoff, T. H. M. (2013). An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection. Journal of Immunology, 190(4), 1659-1671. https://doi.org/10.4049/jimmunol.1201593

@article{4148ce20b78d4839849b1e8b5deee16a,

title = "An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection",

abstract = "Mycobacterium tuberculosis is responsible for almost 2 million deaths annually. Mycobacterium bovis bacillus Calmette-Gu{\'e}rin, the only vaccine available against tuberculosis (TB), induces highly variable protection against TB, and better TB vaccines are urgently needed. A prerequisite for candidate vaccine Ags is that they are immunogenic and expressed by M. tuberculosis during infection of the primary target organ, that is, the lungs of susceptible individuals. In search of new TB vaccine candidate Ags, we have used a genome-wide, unbiased Ag discovery approach to investigate the in vivo expression of 2170 M. tuberculosis genes during M. tuberculosis infection in the lungs of mice. Four genetically related but distinct mouse strains were studied, representing a spectrum of TB susceptibility controlled by the supersusceptibility to TB 1 locus. We used stringent selection approaches to select in vivo-expressed M. tuberculosis (IVE-TB) genes and analyzed their expression patterns in distinct disease phenotypes such as necrosis and granuloma formation. To study the vaccine potential of these proteins, we analyzed their immunogenicity. Several M. tuberculosis proteins were recognized by immune cells from tuberculin skin test-positive, ESAT6/CFP10-responsive individuals, indicating that these Ags are presented during natural M. tuberculosis infection. Furthermore, TB patients also showed responses toward IVE-TB Ags, albeit lower than tuberculin skin test-positive, ESAT6/CFP10-responsive individuals. Finally, IVETB Ags induced strong IFN-γ+/TNF-α+ CD8+ and TNF-α+/IL-2+ CD154+/CD4+ T cell responses in PBMC from long-term latently M. tuberculosis-infected individuals. In conclusion, these IVE-TB Ags are expressed during pulmonary infection in vivo, are immunogenic, induce strong T cell responses in long-term latently M. tuberculosis-infected individuals, and may therefore represent attractive Ags for new TB vaccines.",

author = "Susanna Commandeur and \{Van Meijgaarden\}, \{Krista E.\} and Corine Prins and Pichugin, \{Alexander V.\} and Karin Dijkman and \{Van Den Eeden\}, \{Susan J.F.\} and Friggen, \{Annemieke H.\} and Franken, \{Kees L.M.C.\} and Gregory Dolganov and Igor Kramnik and Schoolnik, \{Gary K.\} and Fredrik Oftung and Korsvold, \{Gro Ellen\} and Annemieke Geluk and Ottenhoff, \{Tom H.M.\}",

year = "2013",

month = feb,

day = "15",

doi = "10.4049/jimmunol.1201593",

language = "English",

volume = "190",

pages = "1659--1671",

journal = "Journal of Immunology",

issn = "0022-1767",

publisher = "American Association of Immunologists",

number = "4",

}

Commandeur, S, Van Meijgaarden, KE, Prins, C, Pichugin, AV, Dijkman, K, Van Den Eeden, SJF, Friggen, AH, Franken, KLMC, Dolganov, G, Kramnik, I, Schoolnik, GK, Oftung, F, Korsvold, GE, Geluk, A & Ottenhoff, THM 2013, 'An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection', Journal of Immunology, vol. 190, no. 4, pp. 1659-1671. https://doi.org/10.4049/jimmunol.1201593

An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection. / Commandeur, Susanna; Van Meijgaarden, Krista E.; Prins, Corine et al.
In: Journal of Immunology, Vol. 190, No. 4, 15.02.2013, p. 1659-1671.

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

TY - JOUR

T1 - An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection

AU - Commandeur, Susanna

AU - Van Meijgaarden, Krista E.

AU - Prins, Corine

AU - Pichugin, Alexander V.

AU - Dijkman, Karin

AU - Van Den Eeden, Susan J.F.

AU - Friggen, Annemieke H.

AU - Franken, Kees L.M.C.

AU - Dolganov, Gregory

AU - Kramnik, Igor

AU - Schoolnik, Gary K.

AU - Oftung, Fredrik

AU - Korsvold, Gro Ellen

AU - Geluk, Annemieke

AU - Ottenhoff, Tom H.M.

PY - 2013/2/15

Y1 - 2013/2/15

N2 - Mycobacterium tuberculosis is responsible for almost 2 million deaths annually. Mycobacterium bovis bacillus Calmette-Guérin, the only vaccine available against tuberculosis (TB), induces highly variable protection against TB, and better TB vaccines are urgently needed. A prerequisite for candidate vaccine Ags is that they are immunogenic and expressed by M. tuberculosis during infection of the primary target organ, that is, the lungs of susceptible individuals. In search of new TB vaccine candidate Ags, we have used a genome-wide, unbiased Ag discovery approach to investigate the in vivo expression of 2170 M. tuberculosis genes during M. tuberculosis infection in the lungs of mice. Four genetically related but distinct mouse strains were studied, representing a spectrum of TB susceptibility controlled by the supersusceptibility to TB 1 locus. We used stringent selection approaches to select in vivo-expressed M. tuberculosis (IVE-TB) genes and analyzed their expression patterns in distinct disease phenotypes such as necrosis and granuloma formation. To study the vaccine potential of these proteins, we analyzed their immunogenicity. Several M. tuberculosis proteins were recognized by immune cells from tuberculin skin test-positive, ESAT6/CFP10-responsive individuals, indicating that these Ags are presented during natural M. tuberculosis infection. Furthermore, TB patients also showed responses toward IVE-TB Ags, albeit lower than tuberculin skin test-positive, ESAT6/CFP10-responsive individuals. Finally, IVETB Ags induced strong IFN-γ+/TNF-α+ CD8+ and TNF-α+/IL-2+ CD154+/CD4+ T cell responses in PBMC from long-term latently M. tuberculosis-infected individuals. In conclusion, these IVE-TB Ags are expressed during pulmonary infection in vivo, are immunogenic, induce strong T cell responses in long-term latently M. tuberculosis-infected individuals, and may therefore represent attractive Ags for new TB vaccines.

AB - Mycobacterium tuberculosis is responsible for almost 2 million deaths annually. Mycobacterium bovis bacillus Calmette-Guérin, the only vaccine available against tuberculosis (TB), induces highly variable protection against TB, and better TB vaccines are urgently needed. A prerequisite for candidate vaccine Ags is that they are immunogenic and expressed by M. tuberculosis during infection of the primary target organ, that is, the lungs of susceptible individuals. In search of new TB vaccine candidate Ags, we have used a genome-wide, unbiased Ag discovery approach to investigate the in vivo expression of 2170 M. tuberculosis genes during M. tuberculosis infection in the lungs of mice. Four genetically related but distinct mouse strains were studied, representing a spectrum of TB susceptibility controlled by the supersusceptibility to TB 1 locus. We used stringent selection approaches to select in vivo-expressed M. tuberculosis (IVE-TB) genes and analyzed their expression patterns in distinct disease phenotypes such as necrosis and granuloma formation. To study the vaccine potential of these proteins, we analyzed their immunogenicity. Several M. tuberculosis proteins were recognized by immune cells from tuberculin skin test-positive, ESAT6/CFP10-responsive individuals, indicating that these Ags are presented during natural M. tuberculosis infection. Furthermore, TB patients also showed responses toward IVE-TB Ags, albeit lower than tuberculin skin test-positive, ESAT6/CFP10-responsive individuals. Finally, IVETB Ags induced strong IFN-γ+/TNF-α+ CD8+ and TNF-α+/IL-2+ CD154+/CD4+ T cell responses in PBMC from long-term latently M. tuberculosis-infected individuals. In conclusion, these IVE-TB Ags are expressed during pulmonary infection in vivo, are immunogenic, induce strong T cell responses in long-term latently M. tuberculosis-infected individuals, and may therefore represent attractive Ags for new TB vaccines.

UR - https://www.scopus.com/pages/publications/84873548317

U2 - 10.4049/jimmunol.1201593

DO - 10.4049/jimmunol.1201593

M3 - Article

C2 - 23319735

SN - 0022-1767

VL - 190

SP - 1659

EP - 1671

JO - Journal of Immunology

JF - Journal of Immunology

IS - 4

ER -

An unbiased genome-wide Mycobacterium tuberculosis gene expression approach to discover antigens targeted by human T cells expressed during pulmonary infection

Abstract

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