Investigating intracellular persistence of Staphylococcus aureus within a murine alveolar macrophage cell line

A. Lacoma; V. Cano; D. Moranta; V. Regueiro; D. Domínguez-Villanueva; M. Laabei; M. González-Nicolau; V. Ausina; C. Prat; J. A. Bengoechea

doi:10.1080/21505594.2017.1361089

Investigating intracellular persistence of Staphylococcus aureus within a murine alveolar macrophage cell line

A. Lacoma^*, V. Cano, D. Moranta, V. Regueiro, D. Domínguez-Villanueva, M. Laabei, M. González-Nicolau, V. Ausina, C. Prat, J. A. Bengoechea

^*Corresponding author for this work

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

47 Citations (Scopus)

Abstract

Objective: Staphylococcus aureus is a particularly difficult pathogen to eradicate from the respiratory tract. Previous studies have highlighted the intracellular capacity of S.aureus in several phagocytic and non-phagocytic cells. The aim of this study was to define S.aureus interaction within a murine alveolar macrophage cell line. Methods: Cell line MH-S was infected with Newman strain. Molecular mechanisms involved in phagocytosis were explored. To assess whether S.aureus survives intracellularly quantitative (gentamicin protection assays and bacterial plating) and qualitative analysis (immunofluorescence microscopy) were performed. Bacterial colocalization with different markers of the endocytic pathway was examined to characterize its intracellular trafficking. Results: We found that S.aureus uptake requires host actin polymerization, microtubule assembly and activation of phosphatidylinositol 3-kinase signaling. Time course experiments showed that Newman strain was able to persist within macrophages at least until 28.5 h post infection. We observed that intracellular bacteria are located inside an acidic subcellular compartment, which co-localizes with the late endosome/lysosome markers Lamp-1, Rab7 and RILP. Colocalization counts with TMR-dextran might reflect a balance between bacterial killing and intracellular survival. Conclusions: This study indicates that S.aureus persists and replicates inside murine alveolar macrophages, representing a privileged niche that can potentially offer protection from antimicrobial activity and immunological host defense mechanisms.

Original language	English
Pages (from-to)	1761-1775
Number of pages	15
Journal	Virulence
Volume	8
Issue number	8
DOIs	https://doi.org/10.1080/21505594.2017.1361089
Publication status	Published - 17 Nov 2017
Externally published	Yes

Keywords

invasion
macrophage
persistence
phagocytosis
Staphylococcus aureus

Access to Document

10.1080/21505594.2017.1361089

Cite this

@article{f2ecbf5515c346118f0a4ab385a76900,

title = "Investigating intracellular persistence of Staphylococcus aureus within a murine alveolar macrophage cell line",

abstract = "Objective: Staphylococcus aureus is a particularly difficult pathogen to eradicate from the respiratory tract. Previous studies have highlighted the intracellular capacity of S.aureus in several phagocytic and non-phagocytic cells. The aim of this study was to define S.aureus interaction within a murine alveolar macrophage cell line. Methods: Cell line MH-S was infected with Newman strain. Molecular mechanisms involved in phagocytosis were explored. To assess whether S.aureus survives intracellularly quantitative (gentamicin protection assays and bacterial plating) and qualitative analysis (immunofluorescence microscopy) were performed. Bacterial colocalization with different markers of the endocytic pathway was examined to characterize its intracellular trafficking. Results: We found that S.aureus uptake requires host actin polymerization, microtubule assembly and activation of phosphatidylinositol 3-kinase signaling. Time course experiments showed that Newman strain was able to persist within macrophages at least until 28.5 h post infection. We observed that intracellular bacteria are located inside an acidic subcellular compartment, which co-localizes with the late endosome/lysosome markers Lamp-1, Rab7 and RILP. Colocalization counts with TMR-dextran might reflect a balance between bacterial killing and intracellular survival. Conclusions: This study indicates that S.aureus persists and replicates inside murine alveolar macrophages, representing a privileged niche that can potentially offer protection from antimicrobial activity and immunological host defense mechanisms.",

keywords = "invasion, macrophage, persistence, phagocytosis, Staphylococcus aureus",

author = "A. Lacoma and V. Cano and D. Moranta and V. Regueiro and D. Dom{\'i}nguez-Villanueva and M. Laabei and M. Gonz{\'a}lez-Nicolau and V. Ausina and C. Prat and Bengoechea, {J. A.}",

note = "Funding Information: This work has been funded by the project PI13/01418 which is part of “Plan Nacional de ICD CI” and co-funded by ISCIII-Subdirecci{\'o}n General de Evaluaci{\'o}n and “Fondo Europeo de Desarrollo Regional” (FEDER). This work also received a grant from the Spanish Society of Pneumology and Thoracic Surgery (SEPAR 054/2011) and Instituto de Salud Carlos III: CIBERES (Corporate Research Program on Host-Pathogen interactions). Funding Information: D. Dom{\'i}nguez-Villanueva is funded by “Plan Nacional de ICD CI” and co-funded by ISCIII-Subdirecci{\'o}n General de Evaluaci{\'o}n and “Fondo Europeo de Desarrollo Regional” (FEDER). M.Laabei was supported by a joint ERS/SEPAR fellowship (LTRF 2015). A. Lacoma has been a recipient of a grant from Sociedad Espa{\~n}ola de Microbiologia Cl{\'i}nica y Enfermedades Infecciosas (SEIMC) and from CIBERES (Pro-grama de perfeccionamiento y movilidad). Funding Information: We thank Kok van Kessel (UMC, Utrecht) and I.Lasa (Universidad P?blica de Navarra/ CSIC) for providing S.aureus Newman and GFP-Newman strains, respectively. We are indebted to S. Grinstein, J. Neefjes and Y. Koide for sending us plasmids. We are grateful to members of the Laboratory ?Infection and Immunity? for helpful discussions. We thank the IGTP Microscopy Core Facility and staff (MP. Armengol and G. Requena) for their contribution to this publication.We also thank Oriol Martos for his kind technical assistance. This work has been funded by the project PI13/01418 which is part of ?Plan Nacional de I+D +I? and co-funded by ISCIII- Subdirecci?n General de Evaluaci?n and ?Fondo Europeo de Desarrollo Regional? (FEDER). This work also received a grant from the Spanish Society of Pneumology and Thoracic Surgery (SEPAR 054/2011) and Instituto de Salud Carlos III: CIBERES (Corporate Research Program on Host-Pathogen interactions). D. Dom?nguez-Villanueva is funded by ?Plan Nacional de I+D +I? and co-funded by ISCIII- Subdirecci?n General de Evaluaci?n and ?Fondo Europeo de Desarrollo Regional? (FEDER). M.Laabei was supported by a joint ERS/SEPAR fellowship (LTRF 2015). A. Lacoma has been a recipient of a grant from Sociedad Espa?ola de Microbiologia Cl?nica y Enfermedades Infecciosas (SEIMC) and from CIBERES (Programa de perfeccionamiento y movilidad). Publisher Copyright: {\textcopyright} 2017 The Author(s). Published with license by Taylor & Francis {\textcopyright} 2017, {\textcopyright} A. Lacoma, V. Cano, D. Moranta, V. Regueiro, D. Dominguez-Villanueva, M. Laabei, M. Gonzalez-Nicolau, V. Ausina, C. Prat, and J. A. Bengoechea.",

year = "2017",

month = nov,

day = "17",

doi = "10.1080/21505594.2017.1361089",

language = "English",

volume = "8",

pages = "1761--1775",

journal = "Virulence",

issn = "2150-5594",

publisher = "Landes Bioscience",

number = "8",

}

TY - JOUR

T1 - Investigating intracellular persistence of Staphylococcus aureus within a murine alveolar macrophage cell line

AU - Lacoma, A.

AU - Cano, V.

AU - Moranta, D.

AU - Regueiro, V.

AU - Domínguez-Villanueva, D.

AU - Laabei, M.

AU - González-Nicolau, M.

AU - Ausina, V.

AU - Prat, C.

AU - Bengoechea, J. A.

N1 - Funding Information: This work has been funded by the project PI13/01418 which is part of “Plan Nacional de ICD CI” and co-funded by ISCIII-Subdirección General de Evaluación and “Fondo Europeo de Desarrollo Regional” (FEDER). This work also received a grant from the Spanish Society of Pneumology and Thoracic Surgery (SEPAR 054/2011) and Instituto de Salud Carlos III: CIBERES (Corporate Research Program on Host-Pathogen interactions). Funding Information: D. Domínguez-Villanueva is funded by “Plan Nacional de ICD CI” and co-funded by ISCIII-Subdirección General de Evaluación and “Fondo Europeo de Desarrollo Regional” (FEDER). M.Laabei was supported by a joint ERS/SEPAR fellowship (LTRF 2015). A. Lacoma has been a recipient of a grant from Sociedad Española de Microbiologia Clínica y Enfermedades Infecciosas (SEIMC) and from CIBERES (Pro-grama de perfeccionamiento y movilidad). Funding Information: We thank Kok van Kessel (UMC, Utrecht) and I.Lasa (Universidad P?blica de Navarra/ CSIC) for providing S.aureus Newman and GFP-Newman strains, respectively. We are indebted to S. Grinstein, J. Neefjes and Y. Koide for sending us plasmids. We are grateful to members of the Laboratory ?Infection and Immunity? for helpful discussions. We thank the IGTP Microscopy Core Facility and staff (MP. Armengol and G. Requena) for their contribution to this publication.We also thank Oriol Martos for his kind technical assistance. This work has been funded by the project PI13/01418 which is part of ?Plan Nacional de I+D +I? and co-funded by ISCIII- Subdirecci?n General de Evaluaci?n and ?Fondo Europeo de Desarrollo Regional? (FEDER). This work also received a grant from the Spanish Society of Pneumology and Thoracic Surgery (SEPAR 054/2011) and Instituto de Salud Carlos III: CIBERES (Corporate Research Program on Host-Pathogen interactions). D. Dom?nguez-Villanueva is funded by ?Plan Nacional de I+D +I? and co-funded by ISCIII- Subdirecci?n General de Evaluaci?n and ?Fondo Europeo de Desarrollo Regional? (FEDER). M.Laabei was supported by a joint ERS/SEPAR fellowship (LTRF 2015). A. Lacoma has been a recipient of a grant from Sociedad Espa?ola de Microbiologia Cl?nica y Enfermedades Infecciosas (SEIMC) and from CIBERES (Programa de perfeccionamiento y movilidad). Publisher Copyright: © 2017 The Author(s). Published with license by Taylor & Francis © 2017, © A. Lacoma, V. Cano, D. Moranta, V. Regueiro, D. Dominguez-Villanueva, M. Laabei, M. Gonzalez-Nicolau, V. Ausina, C. Prat, and J. A. Bengoechea.

PY - 2017/11/17

Y1 - 2017/11/17

N2 - Objective: Staphylococcus aureus is a particularly difficult pathogen to eradicate from the respiratory tract. Previous studies have highlighted the intracellular capacity of S.aureus in several phagocytic and non-phagocytic cells. The aim of this study was to define S.aureus interaction within a murine alveolar macrophage cell line. Methods: Cell line MH-S was infected with Newman strain. Molecular mechanisms involved in phagocytosis were explored. To assess whether S.aureus survives intracellularly quantitative (gentamicin protection assays and bacterial plating) and qualitative analysis (immunofluorescence microscopy) were performed. Bacterial colocalization with different markers of the endocytic pathway was examined to characterize its intracellular trafficking. Results: We found that S.aureus uptake requires host actin polymerization, microtubule assembly and activation of phosphatidylinositol 3-kinase signaling. Time course experiments showed that Newman strain was able to persist within macrophages at least until 28.5 h post infection. We observed that intracellular bacteria are located inside an acidic subcellular compartment, which co-localizes with the late endosome/lysosome markers Lamp-1, Rab7 and RILP. Colocalization counts with TMR-dextran might reflect a balance between bacterial killing and intracellular survival. Conclusions: This study indicates that S.aureus persists and replicates inside murine alveolar macrophages, representing a privileged niche that can potentially offer protection from antimicrobial activity and immunological host defense mechanisms.

AB - Objective: Staphylococcus aureus is a particularly difficult pathogen to eradicate from the respiratory tract. Previous studies have highlighted the intracellular capacity of S.aureus in several phagocytic and non-phagocytic cells. The aim of this study was to define S.aureus interaction within a murine alveolar macrophage cell line. Methods: Cell line MH-S was infected with Newman strain. Molecular mechanisms involved in phagocytosis were explored. To assess whether S.aureus survives intracellularly quantitative (gentamicin protection assays and bacterial plating) and qualitative analysis (immunofluorescence microscopy) were performed. Bacterial colocalization with different markers of the endocytic pathway was examined to characterize its intracellular trafficking. Results: We found that S.aureus uptake requires host actin polymerization, microtubule assembly and activation of phosphatidylinositol 3-kinase signaling. Time course experiments showed that Newman strain was able to persist within macrophages at least until 28.5 h post infection. We observed that intracellular bacteria are located inside an acidic subcellular compartment, which co-localizes with the late endosome/lysosome markers Lamp-1, Rab7 and RILP. Colocalization counts with TMR-dextran might reflect a balance between bacterial killing and intracellular survival. Conclusions: This study indicates that S.aureus persists and replicates inside murine alveolar macrophages, representing a privileged niche that can potentially offer protection from antimicrobial activity and immunological host defense mechanisms.

KW - invasion

KW - macrophage

KW - persistence

KW - phagocytosis

KW - Staphylococcus aureus

UR - http://www.scopus.com/inward/record.url?scp=85029420665&partnerID=8YFLogxK

U2 - 10.1080/21505594.2017.1361089

DO - 10.1080/21505594.2017.1361089

M3 - Article

C2 - 28762868

AN - SCOPUS:85029420665

SN - 2150-5594

VL - 8

SP - 1761

EP - 1775

JO - Virulence

JF - Virulence

IS - 8

ER -

Investigating intracellular persistence of Staphylococcus aureus within a murine alveolar macrophage cell line

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Cite this