A regulatory cascade controls Staphylococcus aureus pathogenicity island activation

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A regulatory cascade controls Staphylococcus aureus pathogenicity island activation. / Haag, Andreas F.; Podkowik, Magdalena; Ibarra-Chávez, Rodrigo; del Sol, Francisca Gallego; Ram, Geeta; Chen, John; Marina, Alberto; Novick, Richard P.; Penadés, José R.

In: Nature Microbiology, Vol. 6, No. 10, 2021, p. 1300-1308.

Research output: Contribution to journalJournal articleResearchpeer-review

Harvard

Haag, AF, Podkowik, M, Ibarra-Chávez, R, del Sol, FG, Ram, G, Chen, J, Marina, A, Novick, RP & Penadés, JR 2021, 'A regulatory cascade controls Staphylococcus aureus pathogenicity island activation', Nature Microbiology, vol. 6, no. 10, pp. 1300-1308. https://doi.org/10.1038/s41564-021-00956-2

APA

Haag, A. F., Podkowik, M., Ibarra-Chávez, R., del Sol, F. G., Ram, G., Chen, J., Marina, A., Novick, R. P., & Penadés, J. R. (2021). A regulatory cascade controls Staphylococcus aureus pathogenicity island activation. Nature Microbiology, 6(10), 1300-1308. https://doi.org/10.1038/s41564-021-00956-2

Vancouver

Haag AF, Podkowik M, Ibarra-Chávez R, del Sol FG, Ram G, Chen J et al. A regulatory cascade controls Staphylococcus aureus pathogenicity island activation. Nature Microbiology. 2021;6(10):1300-1308. https://doi.org/10.1038/s41564-021-00956-2

Author

Haag, Andreas F. ; Podkowik, Magdalena ; Ibarra-Chávez, Rodrigo ; del Sol, Francisca Gallego ; Ram, Geeta ; Chen, John ; Marina, Alberto ; Novick, Richard P. ; Penadés, José R. / A regulatory cascade controls Staphylococcus aureus pathogenicity island activation. In: Nature Microbiology. 2021 ; Vol. 6, No. 10. pp. 1300-1308.

Bibtex

@article{cd272bfdd6ac458782e10e557cd9c057,
title = "A regulatory cascade controls Staphylococcus aureus pathogenicity island activation",
abstract = "Staphylococcal pathogenicity islands (SaPIs) are a family of closely related mobile chromosomal islands that encode and disseminate the superantigen toxins, toxic shock syndrome toxin 1 and superantigen enterotoxin B (SEB). They are regulated by master repressors, which are counteracted by helper phage-encoded proteins, thereby inducing their excision, replication, packaging and intercell transfer. SaPIs are major components of the staphylococcal mobilome, occupying five chromosomal att sites, with many strains harbouring two or more. As regulatory interactions between co-resident SaPIs could have profound effects on the spread of superantigen pathobiology, we initiated the current study to search for such interactions. Using classical genetics, we found that, with one exception, their regulatory systems do not cross-react. The exception was SaPI3, which was originally considered defective because it could not be mobilized by any known helper phage. We show here that SaPI3 has an atypical regulatory module and is induced not by a phage but by many other SaPIs, including SaPI2, SaPIbov1 and SaPIn1, each encoding a conserved protein, Sis, which counteracts the SaPI3 repressor, generating an intracellular regulatory cascade: the co-resident SaPI, when conventionally induced by a helper phage, expresses its sis gene which, in turn, induces SaPI3, enabling it to spread. Using bioinformatics analysis, we have identified more than 30 closely related coancestral SEB-encoding SaPI3 relatives occupying the same att site and controlled by a conserved regulatory module, immA-immR-str'. This module is functionally analogous but unrelated to the typical SaPI regulatory module, stl-str. As SaPIs are phage satellites, SaPI3 and its relatives are SaPI satellites.",
author = "Haag, {Andreas F.} and Magdalena Podkowik and Rodrigo Ibarra-Ch{\'a}vez and {del Sol}, {Francisca Gallego} and Geeta Ram and John Chen and Alberto Marina and Novick, {Richard P.} and Penad{\'e}s, {Jos{\'e} R.}",
note = "{\textcopyright} 2021. The Author(s), under exclusive licence to Springer Nature Limited.",
year = "2021",
doi = "10.1038/s41564-021-00956-2",
language = "English",
volume = "6",
pages = "1300--1308",
journal = "Nature Microbiology",
issn = "2058-5276",
publisher = "nature publishing group",
number = "10",

}

RIS

TY - JOUR

T1 - A regulatory cascade controls Staphylococcus aureus pathogenicity island activation

AU - Haag, Andreas F.

AU - Podkowik, Magdalena

AU - Ibarra-Chávez, Rodrigo

AU - del Sol, Francisca Gallego

AU - Ram, Geeta

AU - Chen, John

AU - Marina, Alberto

AU - Novick, Richard P.

AU - Penadés, José R.

N1 - © 2021. The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2021

Y1 - 2021

N2 - Staphylococcal pathogenicity islands (SaPIs) are a family of closely related mobile chromosomal islands that encode and disseminate the superantigen toxins, toxic shock syndrome toxin 1 and superantigen enterotoxin B (SEB). They are regulated by master repressors, which are counteracted by helper phage-encoded proteins, thereby inducing their excision, replication, packaging and intercell transfer. SaPIs are major components of the staphylococcal mobilome, occupying five chromosomal att sites, with many strains harbouring two or more. As regulatory interactions between co-resident SaPIs could have profound effects on the spread of superantigen pathobiology, we initiated the current study to search for such interactions. Using classical genetics, we found that, with one exception, their regulatory systems do not cross-react. The exception was SaPI3, which was originally considered defective because it could not be mobilized by any known helper phage. We show here that SaPI3 has an atypical regulatory module and is induced not by a phage but by many other SaPIs, including SaPI2, SaPIbov1 and SaPIn1, each encoding a conserved protein, Sis, which counteracts the SaPI3 repressor, generating an intracellular regulatory cascade: the co-resident SaPI, when conventionally induced by a helper phage, expresses its sis gene which, in turn, induces SaPI3, enabling it to spread. Using bioinformatics analysis, we have identified more than 30 closely related coancestral SEB-encoding SaPI3 relatives occupying the same att site and controlled by a conserved regulatory module, immA-immR-str'. This module is functionally analogous but unrelated to the typical SaPI regulatory module, stl-str. As SaPIs are phage satellites, SaPI3 and its relatives are SaPI satellites.

AB - Staphylococcal pathogenicity islands (SaPIs) are a family of closely related mobile chromosomal islands that encode and disseminate the superantigen toxins, toxic shock syndrome toxin 1 and superantigen enterotoxin B (SEB). They are regulated by master repressors, which are counteracted by helper phage-encoded proteins, thereby inducing their excision, replication, packaging and intercell transfer. SaPIs are major components of the staphylococcal mobilome, occupying five chromosomal att sites, with many strains harbouring two or more. As regulatory interactions between co-resident SaPIs could have profound effects on the spread of superantigen pathobiology, we initiated the current study to search for such interactions. Using classical genetics, we found that, with one exception, their regulatory systems do not cross-react. The exception was SaPI3, which was originally considered defective because it could not be mobilized by any known helper phage. We show here that SaPI3 has an atypical regulatory module and is induced not by a phage but by many other SaPIs, including SaPI2, SaPIbov1 and SaPIn1, each encoding a conserved protein, Sis, which counteracts the SaPI3 repressor, generating an intracellular regulatory cascade: the co-resident SaPI, when conventionally induced by a helper phage, expresses its sis gene which, in turn, induces SaPI3, enabling it to spread. Using bioinformatics analysis, we have identified more than 30 closely related coancestral SEB-encoding SaPI3 relatives occupying the same att site and controlled by a conserved regulatory module, immA-immR-str'. This module is functionally analogous but unrelated to the typical SaPI regulatory module, stl-str. As SaPIs are phage satellites, SaPI3 and its relatives are SaPI satellites.

U2 - 10.1038/s41564-021-00956-2

DO - 10.1038/s41564-021-00956-2

M3 - Journal article

C2 - 34518655

VL - 6

SP - 1300

EP - 1308

JO - Nature Microbiology

JF - Nature Microbiology

SN - 2058-5276

IS - 10

ER -

ID: 280053329