Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus

Gerrit Koop; Manouk Vrieling; Daniel M L Storisteanu; Laurence S C Lok; Tom Monie; Glenn van Wigcheren; Claire Raisen; Xiaoliang Ba; Nicholas Gleadall; Nazreen Hadjirin; Arjen J Timmerman; Jaap A Wagenaar; Heleen M Klunder; J Ross Fitzgerald; Ruth Zadoks; Gavin K Paterson; Carmen Torres; Andrew S Waller; Anette Loeffler; Igor Loncaric; Armando E Hoet; Karin Bergström; Luisa De Martino; Constança Pomba; Hermínia de Lencastre; Karim Ben Slama; Haythem Gharsa; Emily J Richardson; Edwin R Chilvers; Carla de Haas; Kok van Kessel; Jos A G van Strijp; Ewan M Harrison; Mark A Holmes

doi:10.1038/srep40660

Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus

Gerrit Koop
, Manouk Vrieling
, Daniel M L Storisteanu
, Laurence S C Lok
, Tom Monie
, Glenn van Wigcheren
, Claire Raisen
, Xiaoliang Ba
, Nicholas Gleadall
, Nazreen Hadjirin
, Arjen J Timmerman
, Jaap A Wagenaar
, Heleen M Klunder
, J Ross Fitzgerald
, Ruth Zadoks
, Gavin K Paterson
, Carmen Torres
, Andrew S Waller
, Anette Loeffler
, Igor Loncaric

Armando E Hoet, Karin Bergström, Luisa De Martino, Constança Pomba, Hermínia de Lencastre, Karim Ben Slama, Haythem Gharsa, Emily J Richardson, Edwin R Chilvers, Carla de Haas, Kok van Kessel, Jos A G van Strijp, Ewan M Harrison, Mark A Holmes

Utrecht University
University Medical Center Utrecht
University of Cambridge
Medical Research Council Human Nutrition Research
University of Edinburgh
Moredun Research Institute
Universidad de La Rioja
Animal Health Trust
Hatfield
University of Veterinary Medicine Vienna
Ohio State University
SVA
University of Naples Federico II
University of Lisbon
Laboratório de Genética Molecular
Département de Biologie
University of Birmingham

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

Abstract

Bicomponent pore-forming leukocidins are a family of potent toxins secreted by Staphylococcus aureus, which target white blood cells preferentially and consist of an S- and an F-component. The S-component recognizes a receptor on the host cell, enabling high-affinity binding to the cell surface, after which the toxins form a pore that penetrates the cell lipid bilayer. Until now, six different leukocidins have been described, some of which are host and cell specific. Here, we identify and characterise a novel S. aureus leukocidin; LukPQ. LukPQ is encoded on a 45 kb prophage (ΦSaeq1) found in six different clonal lineages, almost exclusively in strains cultured from equids. We show that LukPQ is a potent and specific killer of equine neutrophils and identify equine-CXCRA and CXCR2 as its target receptors. Although the S-component (LukP) is highly similar to the S-component of LukED, the species specificity of LukPQ and LukED differs. By forming non-canonical toxin pairs, we identify that the F-component contributes to the observed host tropism of LukPQ, thereby challenging the current paradigm that leukocidin specificity is driven solely by the S-component.

Original language	English
Article number	40660
Journal	Scientific Reports
Volume	7
DOIs	https://doi.org/10.1038/srep40660
Publication status	Published - 20 Jan 2017

Keywords

Bacteriology
Pathogens
Phage biology

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10.1038/srep40660

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Koop, G., Vrieling, M., Storisteanu, D. M. L., Lok, L. S. C., Monie, T., van Wigcheren, G., Raisen, C., Ba, X., Gleadall, N., Hadjirin, N., Timmerman, A. J., Wagenaar, J. A., Klunder, H. M., Fitzgerald, J. R., Zadoks, R., Paterson, G. K., Torres, C., Waller, A. S., Loeffler, A., ... Holmes, M. A. (2017). Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus. Scientific Reports, 7, Article 40660. https://doi.org/10.1038/srep40660

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title = "Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus",

abstract = "Bicomponent pore-forming leukocidins are a family of potent toxins secreted by Staphylococcus aureus, which target white blood cells preferentially and consist of an S- and an F-component. The S-component recognizes a receptor on the host cell, enabling high-affinity binding to the cell surface, after which the toxins form a pore that penetrates the cell lipid bilayer. Until now, six different leukocidins have been described, some of which are host and cell specific. Here, we identify and characterise a novel S. aureus leukocidin; LukPQ. LukPQ is encoded on a 45 kb prophage (ΦSaeq1) found in six different clonal lineages, almost exclusively in strains cultured from equids. We show that LukPQ is a potent and specific killer of equine neutrophils and identify equine-CXCRA and CXCR2 as its target receptors. Although the S-component (LukP) is highly similar to the S-component of LukED, the species specificity of LukPQ and LukED differs. By forming non-canonical toxin pairs, we identify that the F-component contributes to the observed host tropism of LukPQ, thereby challenging the current paradigm that leukocidin specificity is driven solely by the S-component.",

keywords = "Bacteriology, Pathogens, Phage biology",

author = "Gerrit Koop and Manouk Vrieling and Storisteanu, \{Daniel M L\} and Lok, \{Laurence S C\} and Tom Monie and \{van Wigcheren\}, Glenn and Claire Raisen and Xiaoliang Ba and Nicholas Gleadall and Nazreen Hadjirin and Timmerman, \{Arjen J\} and Wagenaar, \{Jaap A\} and Klunder, \{Heleen M\} and Fitzgerald, \{J Ross\} and Ruth Zadoks and Paterson, \{Gavin K\} and Carmen Torres and Waller, \{Andrew S\} and Anette Loeffler and Igor Loncaric and Hoet, \{Armando E\} and Karin Bergstr{\"o}m and \{De Martino\}, Luisa and Constan{\c c}a Pomba and \{de Lencastre\}, Herm{\'i}nia and \{Ben Slama\}, Karim and Haythem Gharsa and Richardson, \{Emily J\} and Chilvers, \{Edwin R\} and \{de Haas\}, Carla and \{van Kessel\}, Kok and \{van Strijp\}, \{Jos A G\} and Harrison, \{Ewan M\} and Holmes, \{Mark A\}",

year = "2017",

month = jan,

day = "20",

doi = "10.1038/srep40660",

language = "English",

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Koop, G, Vrieling, M, Storisteanu, DML, Lok, LSC, Monie, T, van Wigcheren, G, Raisen, C, Ba, X, Gleadall, N, Hadjirin, N, Timmerman, AJ , Wagenaar, JA, Klunder, HM, Fitzgerald, JR, Zadoks, R, Paterson, GK, Torres, C, Waller, AS, Loeffler, A, Loncaric, I, Hoet, AE, Bergström, K, De Martino, L, Pomba, C, de Lencastre, H, Ben Slama, K, Gharsa, H, Richardson, EJ, Chilvers, ER, de Haas, C, van Kessel, K, van Strijp, JAG, Harrison, EM & Holmes, MA 2017, 'Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus', Scientific Reports, vol. 7, 40660. https://doi.org/10.1038/srep40660

TY - JOUR

T1 - Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus

AU - Koop, Gerrit

AU - Vrieling, Manouk

AU - Storisteanu, Daniel M L

AU - Lok, Laurence S C

AU - Monie, Tom

AU - van Wigcheren, Glenn

AU - Raisen, Claire

AU - Ba, Xiaoliang

AU - Gleadall, Nicholas

AU - Hadjirin, Nazreen

AU - Timmerman, Arjen J

AU - Wagenaar, Jaap A

AU - Klunder, Heleen M

AU - Fitzgerald, J Ross

AU - Zadoks, Ruth

AU - Paterson, Gavin K

AU - Torres, Carmen

AU - Waller, Andrew S

AU - Loeffler, Anette

AU - Loncaric, Igor

AU - Hoet, Armando E

AU - Bergström, Karin

AU - De Martino, Luisa

AU - Pomba, Constança

AU - de Lencastre, Hermínia

AU - Ben Slama, Karim

AU - Gharsa, Haythem

AU - Richardson, Emily J

AU - Chilvers, Edwin R

AU - de Haas, Carla

AU - van Kessel, Kok

AU - van Strijp, Jos A G

AU - Harrison, Ewan M

AU - Holmes, Mark A

PY - 2017/1/20

Y1 - 2017/1/20

N2 - Bicomponent pore-forming leukocidins are a family of potent toxins secreted by Staphylococcus aureus, which target white blood cells preferentially and consist of an S- and an F-component. The S-component recognizes a receptor on the host cell, enabling high-affinity binding to the cell surface, after which the toxins form a pore that penetrates the cell lipid bilayer. Until now, six different leukocidins have been described, some of which are host and cell specific. Here, we identify and characterise a novel S. aureus leukocidin; LukPQ. LukPQ is encoded on a 45 kb prophage (ΦSaeq1) found in six different clonal lineages, almost exclusively in strains cultured from equids. We show that LukPQ is a potent and specific killer of equine neutrophils and identify equine-CXCRA and CXCR2 as its target receptors. Although the S-component (LukP) is highly similar to the S-component of LukED, the species specificity of LukPQ and LukED differs. By forming non-canonical toxin pairs, we identify that the F-component contributes to the observed host tropism of LukPQ, thereby challenging the current paradigm that leukocidin specificity is driven solely by the S-component.

AB - Bicomponent pore-forming leukocidins are a family of potent toxins secreted by Staphylococcus aureus, which target white blood cells preferentially and consist of an S- and an F-component. The S-component recognizes a receptor on the host cell, enabling high-affinity binding to the cell surface, after which the toxins form a pore that penetrates the cell lipid bilayer. Until now, six different leukocidins have been described, some of which are host and cell specific. Here, we identify and characterise a novel S. aureus leukocidin; LukPQ. LukPQ is encoded on a 45 kb prophage (ΦSaeq1) found in six different clonal lineages, almost exclusively in strains cultured from equids. We show that LukPQ is a potent and specific killer of equine neutrophils and identify equine-CXCRA and CXCR2 as its target receptors. Although the S-component (LukP) is highly similar to the S-component of LukED, the species specificity of LukPQ and LukED differs. By forming non-canonical toxin pairs, we identify that the F-component contributes to the observed host tropism of LukPQ, thereby challenging the current paradigm that leukocidin specificity is driven solely by the S-component.

KW - Bacteriology

KW - Pathogens

KW - Phage biology

U2 - 10.1038/srep40660

DO - 10.1038/srep40660

M3 - Article

C2 - 28106142

SN - 2045-2322

VL - 7

JO - Scientific Reports

JF - Scientific Reports

M1 - 40660

ER -

Identification of LukPQ, a novel, equid-adapted leukocidin of Staphylococcus aureus

Abstract

Keywords

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