Cell-autonomous innate immunity by proteasome-derived defence peptides

Karin Goldberg; Arseniy Lobov; Paola Antonello; Merav D. Shmueli; Idan Yakir; Tal Weizman; Adi Ulman; Daoud Sheban; Einav Laser; Matthias P. Kramer; Ronen Shteinvil; Guoyun Chen; Angham Ibraheem; Vera Sysoeva; Vered Fishbain-Yoskovitz; Gayatree Mohapatra; Anat Abramov; Sandy Shimshi; Kseniia Ogneva; Madhurima Nandy; Sivan Amidror; Hadar Bootz-Maoz; Shanny H. Kuo; Nili Dezorella; Assaf Kacen; Aaron Javitt; Gee W. Lau; Nissan Yissachar; Zvi Hayouka; Yifat Merbl

doi:10.1038/s41586-025-08615-w

Cell-autonomous innate immunity by proteasome-derived defence peptides

Karin Goldberg, Arseniy Lobov, Paola Antonello, Merav D. Shmueli, Idan Yakir, Tal Weizman, Adi Ulman, Daoud Sheban, Einav Laser, Matthias P. Kramer, Ronen Shteinvil, Guoyun Chen, Angham Ibraheem, Vera Sysoeva, Vered Fishbain-Yoskovitz, Gayatree Mohapatra, Anat Abramov, Sandy Shimshi, Kseniia Ogneva, Madhurima NandySivan Amidror, Hadar Bootz-Maoz, Shanny H. Kuo, Nili Dezorella, Assaf Kacen, Aaron Javitt, Gee W. Lau, Nissan Yissachar, Zvi Hayouka, Yifat Merbl^*

^*Corresponding author for this work

Institute of Biochemistry, Food Science and Nutrition

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

1 Scopus citations

Abstract

For decades, antigen presentation on major histocompatibility complex class I for T cell-mediated immunity has been considered the primary function of proteasome-derived peptides^1,2. However, whether the products of proteasomal degradation play additional parts in mounting immune responses remains unknown. Antimicrobial peptides serve as a first line of defence against invading pathogens before the adaptive immune system responds. Although the protective function of antimicrobial peptides across numerous tissues is well established, the cellular mechanisms underlying their generation are not fully understood. Here we uncover a role for proteasomes in the constitutive and bacterial-induced generation of defence peptides that impede bacterial growth both in vitro and in vivo by disrupting bacterial membranes. In silico prediction of proteome-wide proteasomal cleavage identified hundreds of thousands of potential proteasome-derived defence peptides with cationic properties that may be generated en route to degradation to act as a first line of defence. Furthermore, bacterial infection induces changes in proteasome composition and function, including PSME3 recruitment and increased tryptic-like cleavage, enhancing antimicrobial activity. Beyond providing mechanistic insights into the role of proteasomes in cell-autonomous innate immunity, our study suggests that proteasome-cleaved peptides may have previously overlooked functions downstream of degradation. From a translational standpoint, identifying proteasome-derived defence peptides could provide an untapped source of natural antibiotics for biotechnological applications and therapeutic interventions in infectious diseases and immunocompromised conditions.

Original language	English
Article number	836
Journal	Nature
DOIs	https://doi.org/10.1038/s41586-025-08615-w
State	Accepted/In press - 2025

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Publisher Copyright:
© The Author(s) 2025.

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Goldberg, K., Lobov, A., Antonello, P., Shmueli, M. D., Yakir, I., Weizman, T., Ulman, A., Sheban, D., Laser, E., Kramer, M. P., Shteinvil, R., Chen, G., Ibraheem, A., Sysoeva, V., Fishbain-Yoskovitz, V., Mohapatra, G., Abramov, A., Shimshi, S., Ogneva, K., ... Merbl, Y. (Accepted/In press). Cell-autonomous innate immunity by proteasome-derived defence peptides. Nature, Article 836. https://doi.org/10.1038/s41586-025-08615-w

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title = "Cell-autonomous innate immunity by proteasome-derived defence peptides",

abstract = "For decades, antigen presentation on major histocompatibility complex class I for T cell-mediated immunity has been considered the primary function of proteasome-derived peptides1,2. However, whether the products of proteasomal degradation play additional parts in mounting immune responses remains unknown. Antimicrobial peptides serve as a first line of defence against invading pathogens before the adaptive immune system responds. Although the protective function of antimicrobial peptides across numerous tissues is well established, the cellular mechanisms underlying their generation are not fully understood. Here we uncover a role for proteasomes in the constitutive and bacterial-induced generation of defence peptides that impede bacterial growth both in vitro and in vivo by disrupting bacterial membranes. In silico prediction of proteome-wide proteasomal cleavage identified hundreds of thousands of potential proteasome-derived defence peptides with cationic properties that may be generated en route to degradation to act as a first line of defence. Furthermore, bacterial infection induces changes in proteasome composition and function, including PSME3 recruitment and increased tryptic-like cleavage, enhancing antimicrobial activity. Beyond providing mechanistic insights into the role of proteasomes in cell-autonomous innate immunity, our study suggests that proteasome-cleaved peptides may have previously overlooked functions downstream of degradation. From a translational standpoint, identifying proteasome-derived defence peptides could provide an untapped source of natural antibiotics for biotechnological applications and therapeutic interventions in infectious diseases and immunocompromised conditions.",

author = "Karin Goldberg and Arseniy Lobov and Paola Antonello and Shmueli, {Merav D.} and Idan Yakir and Tal Weizman and Adi Ulman and Daoud Sheban and Einav Laser and Kramer, {Matthias P.} and Ronen Shteinvil and Guoyun Chen and Angham Ibraheem and Vera Sysoeva and Vered Fishbain-Yoskovitz and Gayatree Mohapatra and Anat Abramov and Sandy Shimshi and Kseniia Ogneva and Madhurima Nandy and Sivan Amidror and Hadar Bootz-Maoz and Kuo, {Shanny H.} and Nili Dezorella and Assaf Kacen and Aaron Javitt and Lau, {Gee W.} and Nissan Yissachar and Zvi Hayouka and Yifat Merbl",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

doi = "10.1038/s41586-025-08615-w",

language = "אנגלית",

journal = "Nature",

issn = "0028-0836",

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Goldberg, K, Lobov, A, Antonello, P, Shmueli, MD, Yakir, I, Weizman, T, Ulman, A, Sheban, D, Laser, E, Kramer, MP, Shteinvil, R, Chen, G, Ibraheem, A, Sysoeva, V, Fishbain-Yoskovitz, V, Mohapatra, G, Abramov, A, Shimshi, S, Ogneva, K, Nandy, M, Amidror, S, Bootz-Maoz, H, Kuo, SH, Dezorella, N, Kacen, A, Javitt, A, Lau, GW, Yissachar, N, Hayouka, Z & Merbl, Y 2025, 'Cell-autonomous innate immunity by proteasome-derived defence peptides', Nature. https://doi.org/10.1038/s41586-025-08615-w

TY - JOUR

T1 - Cell-autonomous innate immunity by proteasome-derived defence peptides

AU - Goldberg, Karin

AU - Lobov, Arseniy

AU - Antonello, Paola

AU - Shmueli, Merav D.

AU - Yakir, Idan

AU - Weizman, Tal

AU - Ulman, Adi

AU - Sheban, Daoud

AU - Laser, Einav

AU - Kramer, Matthias P.

AU - Shteinvil, Ronen

AU - Chen, Guoyun

AU - Ibraheem, Angham

AU - Sysoeva, Vera

AU - Fishbain-Yoskovitz, Vered

AU - Mohapatra, Gayatree

AU - Abramov, Anat

AU - Shimshi, Sandy

AU - Ogneva, Kseniia

AU - Nandy, Madhurima

AU - Amidror, Sivan

AU - Bootz-Maoz, Hadar

AU - Kuo, Shanny H.

AU - Dezorella, Nili

AU - Kacen, Assaf

AU - Javitt, Aaron

AU - Lau, Gee W.

AU - Yissachar, Nissan

AU - Hayouka, Zvi

AU - Merbl, Yifat

PY - 2025

Y1 - 2025

N2 - For decades, antigen presentation on major histocompatibility complex class I for T cell-mediated immunity has been considered the primary function of proteasome-derived peptides1,2. However, whether the products of proteasomal degradation play additional parts in mounting immune responses remains unknown. Antimicrobial peptides serve as a first line of defence against invading pathogens before the adaptive immune system responds. Although the protective function of antimicrobial peptides across numerous tissues is well established, the cellular mechanisms underlying their generation are not fully understood. Here we uncover a role for proteasomes in the constitutive and bacterial-induced generation of defence peptides that impede bacterial growth both in vitro and in vivo by disrupting bacterial membranes. In silico prediction of proteome-wide proteasomal cleavage identified hundreds of thousands of potential proteasome-derived defence peptides with cationic properties that may be generated en route to degradation to act as a first line of defence. Furthermore, bacterial infection induces changes in proteasome composition and function, including PSME3 recruitment and increased tryptic-like cleavage, enhancing antimicrobial activity. Beyond providing mechanistic insights into the role of proteasomes in cell-autonomous innate immunity, our study suggests that proteasome-cleaved peptides may have previously overlooked functions downstream of degradation. From a translational standpoint, identifying proteasome-derived defence peptides could provide an untapped source of natural antibiotics for biotechnological applications and therapeutic interventions in infectious diseases and immunocompromised conditions.

AB - For decades, antigen presentation on major histocompatibility complex class I for T cell-mediated immunity has been considered the primary function of proteasome-derived peptides1,2. However, whether the products of proteasomal degradation play additional parts in mounting immune responses remains unknown. Antimicrobial peptides serve as a first line of defence against invading pathogens before the adaptive immune system responds. Although the protective function of antimicrobial peptides across numerous tissues is well established, the cellular mechanisms underlying their generation are not fully understood. Here we uncover a role for proteasomes in the constitutive and bacterial-induced generation of defence peptides that impede bacterial growth both in vitro and in vivo by disrupting bacterial membranes. In silico prediction of proteome-wide proteasomal cleavage identified hundreds of thousands of potential proteasome-derived defence peptides with cationic properties that may be generated en route to degradation to act as a first line of defence. Furthermore, bacterial infection induces changes in proteasome composition and function, including PSME3 recruitment and increased tryptic-like cleavage, enhancing antimicrobial activity. Beyond providing mechanistic insights into the role of proteasomes in cell-autonomous innate immunity, our study suggests that proteasome-cleaved peptides may have previously overlooked functions downstream of degradation. From a translational standpoint, identifying proteasome-derived defence peptides could provide an untapped source of natural antibiotics for biotechnological applications and therapeutic interventions in infectious diseases and immunocompromised conditions.

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Cell-autonomous innate immunity by proteasome-derived defence peptides

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