Ferroptosis-like cell death promotes and prolongs inflammation in Drosophila

Andrew J. Davidson; Rosalind Heron; Jyotirekha Das; Michael Overholtzer; Will Wood

doi:10.1038/s41556-024-01450-7

Ferroptosis-like cell death promotes and prolongs inflammation in Drosophila

Andrew J. Davidson, Rosalind Heron, Jyotirekha Das, Michael Overholtzer, Will Wood

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

Abstract

Ferroptosis is a distinct form of necrotic cell death caused by overwhelming lipid peroxidation, and emerging evidence indicates a major contribution to organ damage in multiple pathologies. However, ferroptosis has not yet been visualized in vivo due to a lack of specific probes, which has severely limited the study of how the immune system interacts with ferroptotic cells and how this process contributes to inflammation. Consequently, whether ferroptosis has a physiological role has remained a key outstanding question. Here we identify a distinct, ferroptotic-like, necrotic cell death occurring in vivo during wounding of the Drosophila embryo using live imaging. We further demonstrate that macrophages rapidly engage these necrotic cells within the embryo but struggle to engulf them, leading to prolonged, frustrated phagocytosis and frequent corpse disintegration. Conversely, suppression of the ferroptotic programme during wounding delays macrophage recruitment to the injury site, pointing to conflicting roles for ferroptosis during inflammation in vivo.

Original language	English
Pages (from-to)	1535-1544
Journal	Nature Cell Biology
Volume	26
Issue number	9
Early online date	25 Jun 2024
DOIs	https://doi.org/10.1038/s41556-024-01450-7
Publication status	Published - Sept 2024

Keywords / Materials (for Non-textual outputs)

Animals
Animals, Genetically Modified
Cell Death
Drosophila Proteins/metabolism
Drosophila melanogaster
Drosophila/metabolism
Embryo, Nonmammalian/metabolism
Ferroptosis
Inflammation/pathology
Lipid Peroxidation
Macrophages/metabolism
Necrosis
Phagocytosis

Access to Document

10.1038/s41556-024-01450-7

NCB-A51877C manuscript_William WoodAccepted author manuscript, 240 KB
s41556-024-01450-7Final published version, 7.69 MB

CIR Sir Henry Wellcome Postdoctoral Fellowship, `Investigating immune cell chemotaxis by using Chromophore Assisted Light Inactivation (CALI) to manipulate actin regulators in real-time.
Wood, W. (Principal Investigator) & Davidson, A. (Co-investigator)
UK-based charities
1/09/18 → 1/10/19
Project: Research
Drosophilia as a model to study immune cell signal integration in vivo
Wood, W. (Principal Investigator)
UK-based charities
1/02/18 → 1/12/22
Project: Research

Cite this

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title = "Ferroptosis-like cell death promotes and prolongs inflammation in Drosophila",

abstract = "Ferroptosis is a distinct form of necrotic cell death caused by overwhelming lipid peroxidation, and emerging evidence indicates a major contribution to organ damage in multiple pathologies. However, ferroptosis has not yet been visualized in vivo due to a lack of specific probes, which has severely limited the study of how the immune system interacts with ferroptotic cells and how this process contributes to inflammation. Consequently, whether ferroptosis has a physiological role has remained a key outstanding question. Here we identify a distinct, ferroptotic-like, necrotic cell death occurring in vivo during wounding of the Drosophila embryo using live imaging. We further demonstrate that macrophages rapidly engage these necrotic cells within the embryo but struggle to engulf them, leading to prolonged, frustrated phagocytosis and frequent corpse disintegration. Conversely, suppression of the ferroptotic programme during wounding delays macrophage recruitment to the injury site, pointing to conflicting roles for ferroptosis during inflammation in vivo.",

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author = "Davidson, {Andrew J.} and Rosalind Heron and Jyotirekha Das and Michael Overholtzer and Will Wood",

year = "2024",

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T1 - Ferroptosis-like cell death promotes and prolongs inflammation in Drosophila

AU - Davidson, Andrew J.

AU - Heron, Rosalind

AU - Das, Jyotirekha

AU - Overholtzer, Michael

AU - Wood, Will

PY - 2024/9

Y1 - 2024/9

N2 - Ferroptosis is a distinct form of necrotic cell death caused by overwhelming lipid peroxidation, and emerging evidence indicates a major contribution to organ damage in multiple pathologies. However, ferroptosis has not yet been visualized in vivo due to a lack of specific probes, which has severely limited the study of how the immune system interacts with ferroptotic cells and how this process contributes to inflammation. Consequently, whether ferroptosis has a physiological role has remained a key outstanding question. Here we identify a distinct, ferroptotic-like, necrotic cell death occurring in vivo during wounding of the Drosophila embryo using live imaging. We further demonstrate that macrophages rapidly engage these necrotic cells within the embryo but struggle to engulf them, leading to prolonged, frustrated phagocytosis and frequent corpse disintegration. Conversely, suppression of the ferroptotic programme during wounding delays macrophage recruitment to the injury site, pointing to conflicting roles for ferroptosis during inflammation in vivo.

AB - Ferroptosis is a distinct form of necrotic cell death caused by overwhelming lipid peroxidation, and emerging evidence indicates a major contribution to organ damage in multiple pathologies. However, ferroptosis has not yet been visualized in vivo due to a lack of specific probes, which has severely limited the study of how the immune system interacts with ferroptotic cells and how this process contributes to inflammation. Consequently, whether ferroptosis has a physiological role has remained a key outstanding question. Here we identify a distinct, ferroptotic-like, necrotic cell death occurring in vivo during wounding of the Drosophila embryo using live imaging. We further demonstrate that macrophages rapidly engage these necrotic cells within the embryo but struggle to engulf them, leading to prolonged, frustrated phagocytosis and frequent corpse disintegration. Conversely, suppression of the ferroptotic programme during wounding delays macrophage recruitment to the injury site, pointing to conflicting roles for ferroptosis during inflammation in vivo.

KW - Animals

KW - Animals, Genetically Modified

KW - Cell Death

KW - Drosophila Proteins/metabolism

KW - Drosophila melanogaster

KW - Drosophila/metabolism

KW - Embryo, Nonmammalian/metabolism

KW - Ferroptosis

KW - Inflammation/pathology

KW - Lipid Peroxidation

KW - Macrophages/metabolism

KW - Necrosis

KW - Phagocytosis

U2 - 10.1038/s41556-024-01450-7

DO - 10.1038/s41556-024-01450-7

M3 - Article

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SN - 1465-7392

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JO - Nature Cell Biology

JF - Nature Cell Biology

IS - 9

ER -

Ferroptosis-like cell death promotes and prolongs inflammation in Drosophila

Abstract

Keywords / Materials (for Non-textual outputs)

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Projects

CIR Sir Henry Wellcome Postdoctoral Fellowship, `Investigating immune cell chemotaxis by using Chromophore Assisted Light Inactivation (CALI) to manipulate actin regulators in real-time.

Drosophilia as a model to study immune cell signal integration in vivo

Cite this