Sterilizing immunity in the lung relies on targeting fungal apoptosis-like programmed cell death

Neta Shlezinger; Henriette Irmer; Sourabh Dhingra; Sarah R. Beattie; Robert A. Cramer; Gerhard H. Braus; Amir Sharon; Tobias M. Hohl

doi:10.1126/science.aan0365

Sterilizing immunity in the lung relies on targeting fungal apoptosis-like programmed cell death

Neta Shlezinger, Henriette Irmer, Sourabh Dhingra, Sarah R. Beattie, Robert A. Cramer, Gerhard H. Braus, Amir Sharon^*, Tobias M. Hohl

^*Corresponding author for this work

School of Plant Sciences and Food Security

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

79 Scopus citations

Abstract

Humans inhale mold conidia daily and typically experience lifelong asymptomatic clearance. Conidial germination into tissue-invasive hyphae can occur in individuals with defects in myeloid function, although the mechanism of myeloid cell-mediated immune surveillance remains unclear. By monitoring fungal physiology in vivo, we demonstrate that lung neutrophils trigger programmed cell death with apoptosis-like features in Aspergillus fumigatus conidia, the most prevalent human mold pathogen. An antiapoptotic protein, AfBIR1, opposes this process by inhibiting fungal caspase activation and DNA fragmentation in the murine lung. Genetic and pharmacologic studies indicate that AfBIR1 expression and activity underlie conidial susceptibility to NADPH (reduced form of nicotinamide adenine dinucleotide phosphate) oxidase-dependent killing and, in turn, host susceptibility to invasive aspergillosis. Immune surveillance exploits a fungal apoptosis-like programmed cell death pathway to maintain sterilizing immunity in the lung.

Original language	English
Pages (from-to)	1037-1041
Number of pages	5
Journal	Science
Volume	357
Issue number	6355
DOIs	https://doi.org/10.1126/science.aan0365
State	Published - 8 Sep 2017

Funding

Funders	Funder number
National Institutes of Health	R21 AI105617, P30 CA008748, P30GM106394, RO1 AI093808, T32 GM008704
National Institute of Allergy and Infectious Diseases	R01AI081838
Burroughs Wellcome Fund
Deutsche Forschungsgemeinschaft	BR1502/11-2
Israel Science Foundation	835/13

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title = "Sterilizing immunity in the lung relies on targeting fungal apoptosis-like programmed cell death",

abstract = "Humans inhale mold conidia daily and typically experience lifelong asymptomatic clearance. Conidial germination into tissue-invasive hyphae can occur in individuals with defects in myeloid function, although the mechanism of myeloid cell-mediated immune surveillance remains unclear. By monitoring fungal physiology in vivo, we demonstrate that lung neutrophils trigger programmed cell death with apoptosis-like features in Aspergillus fumigatus conidia, the most prevalent human mold pathogen. An antiapoptotic protein, AfBIR1, opposes this process by inhibiting fungal caspase activation and DNA fragmentation in the murine lung. Genetic and pharmacologic studies indicate that AfBIR1 expression and activity underlie conidial susceptibility to NADPH (reduced form of nicotinamide adenine dinucleotide phosphate) oxidase-dependent killing and, in turn, host susceptibility to invasive aspergillosis. Immune surveillance exploits a fungal apoptosis-like programmed cell death pathway to maintain sterilizing immunity in the lung.",

author = "Neta Shlezinger and Henriette Irmer and Sourabh Dhingra and Beattie, {Sarah R.} and Cramer, {Robert A.} and Braus, {Gerhard H.} and Amir Sharon and Hohl, {Tobias M.}",

note = "Funding Information: We thank E. Pamer, M. Li, S. Kasahara, B. Zhai, and L. Heung for discussions and critical reading of the manuscript; the Memorial Sloan Kettering Cancer Center Cytology Facility, C. Franqui, and I. Leiner for technical assistance; S. Knoblaugh (Ohio State University) for histopathology; and D. Askew (University of Cincinnati) for expertise on fungal strains. This research was supported by NIH grants RO1 AI093808 (T.M.H.), R21 AI105617 (T.M.H.), RO1 AI081838 (R.A.C.), T32 GM008704 (S.R.B.), P30 CA008748 (to MSKCC), and P30GM106394 (B. Stanton, principal investigator; R.A.C., Pilot Project); Burroughs Wellcome Fund Investigator in the Pathogenesis of Infectious Disease Awards (T.M.H. and R.A.C.); Israel Science Foundation grant 835/13 (A.S.); and Deutsche Forschungsgemeinschaft grant BR1502/11-2 (G.H.B.). All data and code to understand and address the conclusions of this research are available in the main text and supplementary materials.",

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AU - Shlezinger, Neta

AU - Irmer, Henriette

AU - Dhingra, Sourabh

AU - Beattie, Sarah R.

AU - Cramer, Robert A.

AU - Braus, Gerhard H.

AU - Sharon, Amir

AU - Hohl, Tobias M.

N1 - Funding Information: We thank E. Pamer, M. Li, S. Kasahara, B. Zhai, and L. Heung for discussions and critical reading of the manuscript; the Memorial Sloan Kettering Cancer Center Cytology Facility, C. Franqui, and I. Leiner for technical assistance; S. Knoblaugh (Ohio State University) for histopathology; and D. Askew (University of Cincinnati) for expertise on fungal strains. This research was supported by NIH grants RO1 AI093808 (T.M.H.), R21 AI105617 (T.M.H.), RO1 AI081838 (R.A.C.), T32 GM008704 (S.R.B.), P30 CA008748 (to MSKCC), and P30GM106394 (B. Stanton, principal investigator; R.A.C., Pilot Project); Burroughs Wellcome Fund Investigator in the Pathogenesis of Infectious Disease Awards (T.M.H. and R.A.C.); Israel Science Foundation grant 835/13 (A.S.); and Deutsche Forschungsgemeinschaft grant BR1502/11-2 (G.H.B.). All data and code to understand and address the conclusions of this research are available in the main text and supplementary materials.

PY - 2017/9/8

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N2 - Humans inhale mold conidia daily and typically experience lifelong asymptomatic clearance. Conidial germination into tissue-invasive hyphae can occur in individuals with defects in myeloid function, although the mechanism of myeloid cell-mediated immune surveillance remains unclear. By monitoring fungal physiology in vivo, we demonstrate that lung neutrophils trigger programmed cell death with apoptosis-like features in Aspergillus fumigatus conidia, the most prevalent human mold pathogen. An antiapoptotic protein, AfBIR1, opposes this process by inhibiting fungal caspase activation and DNA fragmentation in the murine lung. Genetic and pharmacologic studies indicate that AfBIR1 expression and activity underlie conidial susceptibility to NADPH (reduced form of nicotinamide adenine dinucleotide phosphate) oxidase-dependent killing and, in turn, host susceptibility to invasive aspergillosis. Immune surveillance exploits a fungal apoptosis-like programmed cell death pathway to maintain sterilizing immunity in the lung.

AB - Humans inhale mold conidia daily and typically experience lifelong asymptomatic clearance. Conidial germination into tissue-invasive hyphae can occur in individuals with defects in myeloid function, although the mechanism of myeloid cell-mediated immune surveillance remains unclear. By monitoring fungal physiology in vivo, we demonstrate that lung neutrophils trigger programmed cell death with apoptosis-like features in Aspergillus fumigatus conidia, the most prevalent human mold pathogen. An antiapoptotic protein, AfBIR1, opposes this process by inhibiting fungal caspase activation and DNA fragmentation in the murine lung. Genetic and pharmacologic studies indicate that AfBIR1 expression and activity underlie conidial susceptibility to NADPH (reduced form of nicotinamide adenine dinucleotide phosphate) oxidase-dependent killing and, in turn, host susceptibility to invasive aspergillosis. Immune surveillance exploits a fungal apoptosis-like programmed cell death pathway to maintain sterilizing immunity in the lung.

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ER -

Sterilizing immunity in the lung relies on targeting fungal apoptosis-like programmed cell death

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