Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI

Susanne Pfeiler; Avinash B. Khandagale; Astrid Magenau; Maryana Nichols; Harry F.G. Heijnen; Franz Rinninger; Tilman Ziegler; Stephanie Seveau; Sören Schubert; Stefan Zahler; Admar Verschoor; Eicke Latz; Steffen Massberg; Katharina Gaus; Bernd Engelmann

doi:10.1038/srep34440

Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI

Susanne Pfeiler, Avinash B. Khandagale, Astrid Magenau, Maryana Nichols, Harry F.G. Heijnen, Franz Rinninger, Tilman Ziegler, Stephanie Seveau, Sören Schubert, Stefan Zahler, Admar Verschoor, Eicke Latz, Steffen Massberg, Katharina Gaus, Bernd Engelmann^*

^*Korrespondierende/r Autor/-in für diese Arbeit

Institut für Systemische Entzündungsforschung

15 Zitate (Scopus)

Abstract

The mechanisms protecting from immunopathology during acute bacterial infections are incompletely known. We found that in response to apoptotic immune cells and live or dead Listeria monocytogenes scavenger receptor BI (SR-BI), an anti-atherogenic lipid exchange mediator, activated internalization mechanisms with characteristics of macropinocytosis and, assisted by Golgi fragmentation, initiated autophagic responses. This was supported by scavenger receptor-induced local increases in membrane cholesterol concentrations which generated lipid domains particularly in cell extensions and the Golgi. SR-BI was a key driver of beclin-1-dependent autophagy during acute bacterial infection of the liver and spleen. Autophagy regulated tissue infiltration of neutrophils, suppressed accumulation of Ly6C⁺ (inflammatory) macrophages, and prevented hepatocyte necrosis in the core of infectious foci. Perifocal levels of Ly6C⁺ macrophages and Ly6C^- macrophages were unaffected, indicating predominant regulation of the focus core. SR-BI-triggered autophagy promoted co-elimination of apoptotic immune cells and dead bacteria but barely influenced bacterial sequestration and survival or inflammasome activation, thus exclusively counteracting damage inflicted by immune responses. Hence, SR-BI-and autophagy promote a surveillance pathway that partially responds to products of antimicrobial defenses and selectively prevents immunity-induced damage during acute infection. Our findings suggest that control of infection-associated immunopathology can be based on a unified defense operation.

Originalsprache	Englisch
Aufsatznummer	34440
Zeitschrift	Scientific Reports
Jahrgang	6
ISSN	2045-2322
DOIs	https://doi.org/10.1038/srep34440
Publikationsstatus	Veröffentlicht - 03.10.2016

Fördermittel

We are grateful to Silke Dlugai-Esser, Martina Schiffner, Markus Wiedmann, Petra Vrabcova, Nikolaus Ackermann and Konrad Tr?lzsch for their participation in the experiments. We would like to thank Daniel J. Klionsky and Christian Steib for helpful suggestions. We thank all those who kindly provided material for the present work. We are grateful to Christoph von Hesler for technical assistance. This study has been supported by collaborative grant 1123 of Deutsche Forschungsgemeinschaft (Project B06) as well as by grants of Deutsche Krebshilfe and Wilhelm-Sander-Stiftung to B.E.

UN SDGs

Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 3 – Gesundheit und Wohlergehen

Strategische Forschungsbereiche und Zentren

Forschungsschwerpunkt: Infektion und Entzündung - Zentrum für Infektions- und Entzündungsforschung Lübeck (ZIEL)

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10.1038/srep34440

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Pfeiler, S., Khandagale, A. B., Magenau, A., Nichols, M., Heijnen, H. F. G., Rinninger, F., Ziegler, T., Seveau, S., Schubert, S., Zahler, S., Verschoor, A., Latz, E., Massberg, S., Gaus, K., & Engelmann, B. (2016). Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI. Scientific Reports, 6, Artikel 34440. https://doi.org/10.1038/srep34440

@article{93d57793fb4e4805a8b6e9a6d918d0ab,

title = "Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI",

abstract = "The mechanisms protecting from immunopathology during acute bacterial infections are incompletely known. We found that in response to apoptotic immune cells and live or dead Listeria monocytogenes scavenger receptor BI (SR-BI), an anti-atherogenic lipid exchange mediator, activated internalization mechanisms with characteristics of macropinocytosis and, assisted by Golgi fragmentation, initiated autophagic responses. This was supported by scavenger receptor-induced local increases in membrane cholesterol concentrations which generated lipid domains particularly in cell extensions and the Golgi. SR-BI was a key driver of beclin-1-dependent autophagy during acute bacterial infection of the liver and spleen. Autophagy regulated tissue infiltration of neutrophils, suppressed accumulation of Ly6C+ (inflammatory) macrophages, and prevented hepatocyte necrosis in the core of infectious foci. Perifocal levels of Ly6C+ macrophages and Ly6C- macrophages were unaffected, indicating predominant regulation of the focus core. SR-BI-triggered autophagy promoted co-elimination of apoptotic immune cells and dead bacteria but barely influenced bacterial sequestration and survival or inflammasome activation, thus exclusively counteracting damage inflicted by immune responses. Hence, SR-BI-and autophagy promote a surveillance pathway that partially responds to products of antimicrobial defenses and selectively prevents immunity-induced damage during acute infection. Our findings suggest that control of infection-associated immunopathology can be based on a unified defense operation.",

author = "Susanne Pfeiler and Khandagale, \{Avinash B.\} and Astrid Magenau and Maryana Nichols and Heijnen, \{Harry F.G.\} and Franz Rinninger and Tilman Ziegler and Stephanie Seveau and S{\"o}ren Schubert and Stefan Zahler and Admar Verschoor and Eicke Latz and Steffen Massberg and Katharina Gaus and Bernd Engelmann",

note = "Funding Information: We are grateful to Silke Dlugai-Esser, Martina Schiffner, Markus Wiedmann, Petra Vrabcova, Nikolaus Ackermann and Konrad Tr?lzsch for their participation in the experiments. We would like to thank Daniel J. Klionsky and Christian Steib for helpful suggestions. We thank all those who kindly provided material for the present work. We are grateful to Christoph von Hesler for technical assistance. This study has been supported by collaborative grant 1123 of Deutsche Forschungsgemeinschaft (Project B06) as well as by grants of Deutsche Krebshilfe and Wilhelm-Sander-Stiftung to B.E. Publisher Copyright: {\textcopyright} 2016 The Author(s). Copyright: Copyright 2016 Elsevier B.V., All rights reserved.",

year = "2016",

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day = "3",

doi = "10.1038/srep34440",

language = "English",

volume = "6",

journal = "Scientific Reports",

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T1 - Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI

AU - Pfeiler, Susanne

AU - Khandagale, Avinash B.

AU - Magenau, Astrid

AU - Nichols, Maryana

AU - Heijnen, Harry F.G.

AU - Rinninger, Franz

AU - Ziegler, Tilman

AU - Seveau, Stephanie

AU - Schubert, Sören

AU - Zahler, Stefan

AU - Verschoor, Admar

AU - Latz, Eicke

AU - Massberg, Steffen

AU - Gaus, Katharina

AU - Engelmann, Bernd

N1 - Funding Information: We are grateful to Silke Dlugai-Esser, Martina Schiffner, Markus Wiedmann, Petra Vrabcova, Nikolaus Ackermann and Konrad Tr?lzsch for their participation in the experiments. We would like to thank Daniel J. Klionsky and Christian Steib for helpful suggestions. We thank all those who kindly provided material for the present work. We are grateful to Christoph von Hesler for technical assistance. This study has been supported by collaborative grant 1123 of Deutsche Forschungsgemeinschaft (Project B06) as well as by grants of Deutsche Krebshilfe and Wilhelm-Sander-Stiftung to B.E. Publisher Copyright: © 2016 The Author(s). Copyright: Copyright 2016 Elsevier B.V., All rights reserved.

PY - 2016/10/3

Y1 - 2016/10/3

N2 - The mechanisms protecting from immunopathology during acute bacterial infections are incompletely known. We found that in response to apoptotic immune cells and live or dead Listeria monocytogenes scavenger receptor BI (SR-BI), an anti-atherogenic lipid exchange mediator, activated internalization mechanisms with characteristics of macropinocytosis and, assisted by Golgi fragmentation, initiated autophagic responses. This was supported by scavenger receptor-induced local increases in membrane cholesterol concentrations which generated lipid domains particularly in cell extensions and the Golgi. SR-BI was a key driver of beclin-1-dependent autophagy during acute bacterial infection of the liver and spleen. Autophagy regulated tissue infiltration of neutrophils, suppressed accumulation of Ly6C+ (inflammatory) macrophages, and prevented hepatocyte necrosis in the core of infectious foci. Perifocal levels of Ly6C+ macrophages and Ly6C- macrophages were unaffected, indicating predominant regulation of the focus core. SR-BI-triggered autophagy promoted co-elimination of apoptotic immune cells and dead bacteria but barely influenced bacterial sequestration and survival or inflammasome activation, thus exclusively counteracting damage inflicted by immune responses. Hence, SR-BI-and autophagy promote a surveillance pathway that partially responds to products of antimicrobial defenses and selectively prevents immunity-induced damage during acute infection. Our findings suggest that control of infection-associated immunopathology can be based on a unified defense operation.

AB - The mechanisms protecting from immunopathology during acute bacterial infections are incompletely known. We found that in response to apoptotic immune cells and live or dead Listeria monocytogenes scavenger receptor BI (SR-BI), an anti-atherogenic lipid exchange mediator, activated internalization mechanisms with characteristics of macropinocytosis and, assisted by Golgi fragmentation, initiated autophagic responses. This was supported by scavenger receptor-induced local increases in membrane cholesterol concentrations which generated lipid domains particularly in cell extensions and the Golgi. SR-BI was a key driver of beclin-1-dependent autophagy during acute bacterial infection of the liver and spleen. Autophagy regulated tissue infiltration of neutrophils, suppressed accumulation of Ly6C+ (inflammatory) macrophages, and prevented hepatocyte necrosis in the core of infectious foci. Perifocal levels of Ly6C+ macrophages and Ly6C- macrophages were unaffected, indicating predominant regulation of the focus core. SR-BI-triggered autophagy promoted co-elimination of apoptotic immune cells and dead bacteria but barely influenced bacterial sequestration and survival or inflammasome activation, thus exclusively counteracting damage inflicted by immune responses. Hence, SR-BI-and autophagy promote a surveillance pathway that partially responds to products of antimicrobial defenses and selectively prevents immunity-induced damage during acute infection. Our findings suggest that control of infection-associated immunopathology can be based on a unified defense operation.

UR - https://www.scopus.com/pages/publications/84989864215

U2 - 10.1038/srep34440

DO - 10.1038/srep34440

M3 - Journal articles

C2 - 27694929

AN - SCOPUS:84989864215

SN - 2045-2322

VL - 6

JO - Scientific Reports

JF - Scientific Reports

M1 - 34440

ER -

Distinct surveillance pathway for immunopathology during acute infection via autophagy and SR-BI

Abstract

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