PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection

Daniel Fisch; Moritz M Pfleiderer; Eleni Anastasakou; Gillian M Mackie; Fabian Wendt; Xiangyang Liu; Barbara Clough; Samuel Lara-Reyna; Vesela Encheva; Ambrosius P Snijders; Hironori Bando; Masahiro Yamamoto; Andrew D Beggs; Jason Mercer; Avinash R Shenoy; Bernd Wollscheid; Kendle M Maslowski; Wojtek P Galej; Eva-Maria Frickel

doi:10.1126/science.adg2253

PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection

Daniel Fisch, Moritz M Pfleiderer, Eleni Anastasakou, Gillian M Mackie, Fabian Wendt, Xiangyang Liu, Barbara Clough, Samuel Lara-Reyna, Vesela Encheva, Ambrosius P Snijders, Hironori Bando, Masahiro Yamamoto, Andrew D Beggs, Jason Mercer, Avinash R Shenoy, Bernd Wollscheid, Kendle M Maslowski, Wojtek P Galej, Eva-Maria Frickel^*

^*Corresponding author for this work

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

Abstract

Disruption of cellular activities by pathogen virulence factors can trigger innate immune responses. Interferon-γ (IFN-γ)-inducible antimicrobial factors, such as the guanylate binding proteins (GBPs), promote cell-intrinsic defense by attacking intracellular pathogens and by inducing programmed cell death. Working in human macrophages, we discovered that GBP1 expression in the absence of IFN-γ killed the cells and induced Golgi fragmentation. IFN-γ exposure improved macrophage survival through the activity of the kinase PIM1. PIM1 phosphorylated GBP1, leading to its sequestration by 14-3-3σ, which thereby prevented GBP1 membrane association. During Toxoplasma gondii infection, the virulence protein TgIST interfered with IFN-γ signaling and depleted PIM1, thereby increasing GBP1 activity. Although infected cells can restrain pathogens in a GBP1-dependent manner, this mechanism can protect uninfected bystander cells. Thus, PIM1 can provide a bait for pathogen virulence factors, guarding the integrity of IFN-γ signaling.

Original language	English
Article number	eadg2253
Number of pages	15
Journal	Science
Volume	382
Issue number	6666
DOIs	https://doi.org/10.1126/science.adg2253
Publication status	Published - 6 Oct 2023

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Fisch, D., Pfleiderer, M. M., Anastasakou, E., Mackie, G. M., Wendt, F., Liu, X., Clough, B., Lara-Reyna, S., Encheva, V., Snijders, A. P., Bando, H., Yamamoto, M., Beggs, A. D., Mercer, J., Shenoy, A. R., Wollscheid, B., Maslowski, K. M., Galej, W. P., & Frickel, E.-M. (2023). PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection. Science, 382(6666), Article eadg2253. https://doi.org/10.1126/science.adg2253

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title = "PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection",

abstract = "Disruption of cellular activities by pathogen virulence factors can trigger innate immune responses. Interferon-γ (IFN-γ)-inducible antimicrobial factors, such as the guanylate binding proteins (GBPs), promote cell-intrinsic defense by attacking intracellular pathogens and by inducing programmed cell death. Working in human macrophages, we discovered that GBP1 expression in the absence of IFN-γ killed the cells and induced Golgi fragmentation. IFN-γ exposure improved macrophage survival through the activity of the kinase PIM1. PIM1 phosphorylated GBP1, leading to its sequestration by 14-3-3σ, which thereby prevented GBP1 membrane association. During Toxoplasma gondii infection, the virulence protein TgIST interfered with IFN-γ signaling and depleted PIM1, thereby increasing GBP1 activity. Although infected cells can restrain pathogens in a GBP1-dependent manner, this mechanism can protect uninfected bystander cells. Thus, PIM1 can provide a bait for pathogen virulence factors, guarding the integrity of IFN-γ signaling.",

author = "Daniel Fisch and Pfleiderer, {Moritz M} and Eleni Anastasakou and Mackie, {Gillian M} and Fabian Wendt and Xiangyang Liu and Barbara Clough and Samuel Lara-Reyna and Vesela Encheva and Snijders, {Ambrosius P} and Hironori Bando and Masahiro Yamamoto and Beggs, {Andrew D} and Jason Mercer and Shenoy, {Avinash R} and Bernd Wollscheid and Maslowski, {Kendle M} and Galej, {Wojtek P} and Eva-Maria Frickel",

year = "2023",

month = oct,

day = "6",

doi = "10.1126/science.adg2253",

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Fisch, D, Pfleiderer, MM, Anastasakou, E, Mackie, GM, Wendt, F, Liu, X, Clough, B, Lara-Reyna, S, Encheva, V, Snijders, AP, Bando, H, Yamamoto, M, Beggs, AD, Mercer, J, Shenoy, AR, Wollscheid, B, Maslowski, KM, Galej, WP & Frickel, E-M 2023, 'PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection', Science, vol. 382, no. 6666, eadg2253. https://doi.org/10.1126/science.adg2253

TY - JOUR

T1 - PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection

AU - Fisch, Daniel

AU - Pfleiderer, Moritz M

AU - Anastasakou, Eleni

AU - Mackie, Gillian M

AU - Wendt, Fabian

AU - Liu, Xiangyang

AU - Clough, Barbara

AU - Lara-Reyna, Samuel

AU - Encheva, Vesela

AU - Snijders, Ambrosius P

AU - Bando, Hironori

AU - Yamamoto, Masahiro

AU - Beggs, Andrew D

AU - Mercer, Jason

AU - Shenoy, Avinash R

AU - Wollscheid, Bernd

AU - Maslowski, Kendle M

AU - Galej, Wojtek P

AU - Frickel, Eva-Maria

PY - 2023/10/6

Y1 - 2023/10/6

N2 - Disruption of cellular activities by pathogen virulence factors can trigger innate immune responses. Interferon-γ (IFN-γ)-inducible antimicrobial factors, such as the guanylate binding proteins (GBPs), promote cell-intrinsic defense by attacking intracellular pathogens and by inducing programmed cell death. Working in human macrophages, we discovered that GBP1 expression in the absence of IFN-γ killed the cells and induced Golgi fragmentation. IFN-γ exposure improved macrophage survival through the activity of the kinase PIM1. PIM1 phosphorylated GBP1, leading to its sequestration by 14-3-3σ, which thereby prevented GBP1 membrane association. During Toxoplasma gondii infection, the virulence protein TgIST interfered with IFN-γ signaling and depleted PIM1, thereby increasing GBP1 activity. Although infected cells can restrain pathogens in a GBP1-dependent manner, this mechanism can protect uninfected bystander cells. Thus, PIM1 can provide a bait for pathogen virulence factors, guarding the integrity of IFN-γ signaling.

AB - Disruption of cellular activities by pathogen virulence factors can trigger innate immune responses. Interferon-γ (IFN-γ)-inducible antimicrobial factors, such as the guanylate binding proteins (GBPs), promote cell-intrinsic defense by attacking intracellular pathogens and by inducing programmed cell death. Working in human macrophages, we discovered that GBP1 expression in the absence of IFN-γ killed the cells and induced Golgi fragmentation. IFN-γ exposure improved macrophage survival through the activity of the kinase PIM1. PIM1 phosphorylated GBP1, leading to its sequestration by 14-3-3σ, which thereby prevented GBP1 membrane association. During Toxoplasma gondii infection, the virulence protein TgIST interfered with IFN-γ signaling and depleted PIM1, thereby increasing GBP1 activity. Although infected cells can restrain pathogens in a GBP1-dependent manner, this mechanism can protect uninfected bystander cells. Thus, PIM1 can provide a bait for pathogen virulence factors, guarding the integrity of IFN-γ signaling.

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U2 - 10.1126/science.adg2253

DO - 10.1126/science.adg2253

M3 - Article

C2 - 37797010

SN - 0036-8075

VL - 382

JO - Science

JF - Science

IS - 6666

M1 - eadg2253

ER -

PIM1 controls GBP1 activity to limit self-damage and to guard against pathogen infection

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