Translation dysregulation in cancer as a source for targetable antigens

Chen Weller; Osnat Bartok; Christopher S. McGinnis; Heyilimu Palashati; Tian Gen Chang; Dmitry Malko; Merav D. Shmueli; Asuteka Nagao; Deborah Hayoun; Ayaka Murayama; Yuriko Sakaguchi; Panagiotis Poulis; Aseel Khatib; Bracha Erlanger Avigdor; Sagi Gordon; Sapir Cohen Shvefel; Marie J. Zemanek; Morten M. Nielsen; Sigalit Boura-Halfon; Shira Sagie; Nofar Gumpert; Weiwen Yang; Dmitry Alexeev; Pelgia Kyriakidou; Winnie Yao; Mirie Zerbib; Polina Greenberg; Gil Benedek; Kevin Litchfield; Ekaterina Petrovich-Kopitman; Adi Nagler; Roni Oren; Shifra Ben-Dor; Yishai Levin; Yitzhak Pilpel; Marina Rodnina; Jürgen Cox; Yifat Merbl; Ansuman T. Satpathy; Yaron Carmi; Florian Erhard; Tsutomu Suzuki; Allen R. Buskirk; Johanna Olweus; Eytan Ruppin; Andreas Schlosser; Yardena Samuels

doi:10.1016/j.ccell.2025.03.003

Translation dysregulation in cancer as a source for targetable antigens

Chen Weller, Osnat Bartok, Christopher S. McGinnis, Heyilimu Palashati, Tian Gen Chang, Dmitry Malko, Merav D. Shmueli, Asuteka Nagao, Deborah Hayoun, Ayaka Murayama, Yuriko Sakaguchi, Panagiotis Poulis, Aseel Khatib, Bracha Erlanger Avigdor, Sagi Gordon, Sapir Cohen Shvefel, Marie J. Zemanek, Morten M. Nielsen, Sigalit Boura-Halfon, Shira SagieNofar Gumpert, Weiwen Yang, Dmitry Alexeev, Pelgia Kyriakidou, Winnie Yao, Mirie Zerbib, Polina Greenberg, Gil Benedek, Kevin Litchfield, Ekaterina Petrovich-Kopitman, Adi Nagler, Roni Oren, Shifra Ben-Dor, Yishai Levin, Yitzhak Pilpel, Marina Rodnina, Jürgen Cox, Yifat Merbl, Ansuman T. Satpathy, Yaron Carmi, Florian Erhard, Tsutomu Suzuki, Allen R. Buskirk, Johanna Olweus, Eytan Ruppin, Andreas Schlosser, Yardena Samuels

Pathology

Tel Aviv University

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

Abstract

Aberrant peptides presented by major histocompatibility complex (MHC) molecules are targets for tumor eradication, as these peptides can be recognized as foreign by T cells. Protein synthesis in malignant cells is dysregulated, which may result in the generation and presentation of aberrant peptides that can be exploited for T cell-based therapies. To investigate the role of translational dysregulation in immunological tumor control, we disrupt translation fidelity by deleting tRNA wybutosine (yW)-synthesizing protein 2 (TYW2) in tumor cells and characterize the downstream impact on translation fidelity and immunogenicity using immunopeptidomics, genomics, and functional assays. These analyses reveal that TYW2 knockout (KO) cells generate immunogenic out-of-frame peptides. Furthermore, Tyw2 loss increases tumor immunogenicity and leads to anti-programmed cell death 1 (PD-1) checkpoint blockade sensitivity in vivo. Importantly, reduced TYW2 expression is associated with increased response to checkpoint blockade in patients. Together, we demonstrate that defects in translation fidelity drive tumor immunogenicity and may be leveraged for cancer immunotherapy.

Original language	English
Journal	Cancer Cell
DOIs	https://doi.org/10.1016/j.ccell.2025.03.003
State	Accepted/In press - 1 Jan 2025

Keywords

cancer immunopeptidome
immune checkpoint blockade
neoantigens
non-canonical peptides
translation fidelity

All Science Journal Classification (ASJC) codes

Oncology
Cancer Research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1016/j.ccell.2025.03.003

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Weller, C., Bartok, O., McGinnis, C. S., Palashati, H., Chang, T. G., Malko, D., Shmueli, M. D., Nagao, A., Hayoun, D., Murayama, A., Sakaguchi, Y., Poulis, P., Khatib, A., Erlanger Avigdor, B., Gordon, S., Cohen Shvefel, S., Zemanek, M. J., Nielsen, M. M., Boura-Halfon, S., ... Samuels, Y. (Accepted/In press). Translation dysregulation in cancer as a source for targetable antigens. Cancer Cell. https://doi.org/10.1016/j.ccell.2025.03.003

@article{83887edd432c4589ada0adbb7af76227,

title = "Translation dysregulation in cancer as a source for targetable antigens",

abstract = "Aberrant peptides presented by major histocompatibility complex (MHC) molecules are targets for tumor eradication, as these peptides can be recognized as foreign by T cells. Protein synthesis in malignant cells is dysregulated, which may result in the generation and presentation of aberrant peptides that can be exploited for T cell-based therapies. To investigate the role of translational dysregulation in immunological tumor control, we disrupt translation fidelity by deleting tRNA wybutosine (yW)-synthesizing protein 2 (TYW2) in tumor cells and characterize the downstream impact on translation fidelity and immunogenicity using immunopeptidomics, genomics, and functional assays. These analyses reveal that TYW2 knockout (KO) cells generate immunogenic out-of-frame peptides. Furthermore, Tyw2 loss increases tumor immunogenicity and leads to anti-programmed cell death 1 (PD-1) checkpoint blockade sensitivity in vivo. Importantly, reduced TYW2 expression is associated with increased response to checkpoint blockade in patients. Together, we demonstrate that defects in translation fidelity drive tumor immunogenicity and may be leveraged for cancer immunotherapy.",

keywords = "cancer immunopeptidome, immune checkpoint blockade, neoantigens, non-canonical peptides, translation fidelity",

author = "Chen Weller and Osnat Bartok and McGinnis, {Christopher S.} and Heyilimu Palashati and Chang, {Tian Gen} and Dmitry Malko and Shmueli, {Merav D.} and Asuteka Nagao and Deborah Hayoun and Ayaka Murayama and Yuriko Sakaguchi and Panagiotis Poulis and Aseel Khatib and {Erlanger Avigdor}, Bracha and Sagi Gordon and {Cohen Shvefel}, Sapir and Zemanek, {Marie J.} and Nielsen, {Morten M.} and Sigalit Boura-Halfon and Shira Sagie and Nofar Gumpert and Weiwen Yang and Dmitry Alexeev and Pelgia Kyriakidou and Winnie Yao and Mirie Zerbib and Polina Greenberg and Gil Benedek and Kevin Litchfield and Ekaterina Petrovich-Kopitman and Adi Nagler and Roni Oren and Shifra Ben-Dor and Yishai Levin and Yitzhak Pilpel and Marina Rodnina and J{\"u}rgen Cox and Yifat Merbl and Satpathy, {Ansuman T.} and Yaron Carmi and Florian Erhard and Tsutomu Suzuki and Buskirk, {Allen R.} and Johanna Olweus and Eytan Ruppin and Andreas Schlosser and Yardena Samuels",

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

year = "2025",

month = jan,

day = "1",

doi = "10.1016/j.ccell.2025.03.003",

language = "الإنجليزيّة",

journal = "Cancer Cell",

issn = "1535-6108",

publisher = "Cell Press",

}

Weller, C, Bartok, O, McGinnis, CS, Palashati, H, Chang, TG, Malko, D, Shmueli, MD, Nagao, A, Hayoun, D, Murayama, A, Sakaguchi, Y, Poulis, P, Khatib, A, Erlanger Avigdor, B, Gordon, S, Cohen Shvefel, S, Zemanek, MJ, Nielsen, MM, Boura-Halfon, S, Sagie, S, Gumpert, N, Yang, W, Alexeev, D, Kyriakidou, P, Yao, W, Zerbib, M, Greenberg, P, Benedek, G, Litchfield, K, Petrovich-Kopitman, E, Nagler, A, Oren, R, Ben-Dor, S, Levin, Y, Pilpel, Y, Rodnina, M, Cox, J, Merbl, Y, Satpathy, AT, Carmi, Y, Erhard, F, Suzuki, T, Buskirk, AR, Olweus, J, Ruppin, E, Schlosser, A & Samuels, Y 2025, 'Translation dysregulation in cancer as a source for targetable antigens', Cancer Cell. https://doi.org/10.1016/j.ccell.2025.03.003

TY - JOUR

T1 - Translation dysregulation in cancer as a source for targetable antigens

AU - Weller, Chen

AU - Bartok, Osnat

AU - McGinnis, Christopher S.

AU - Palashati, Heyilimu

AU - Chang, Tian Gen

AU - Malko, Dmitry

AU - Shmueli, Merav D.

AU - Nagao, Asuteka

AU - Hayoun, Deborah

AU - Murayama, Ayaka

AU - Sakaguchi, Yuriko

AU - Poulis, Panagiotis

AU - Khatib, Aseel

AU - Erlanger Avigdor, Bracha

AU - Gordon, Sagi

AU - Cohen Shvefel, Sapir

AU - Zemanek, Marie J.

AU - Nielsen, Morten M.

AU - Boura-Halfon, Sigalit

AU - Sagie, Shira

AU - Gumpert, Nofar

AU - Yang, Weiwen

AU - Alexeev, Dmitry

AU - Kyriakidou, Pelgia

AU - Yao, Winnie

AU - Zerbib, Mirie

AU - Greenberg, Polina

AU - Benedek, Gil

AU - Litchfield, Kevin

AU - Petrovich-Kopitman, Ekaterina

AU - Nagler, Adi

AU - Oren, Roni

AU - Ben-Dor, Shifra

AU - Levin, Yishai

AU - Pilpel, Yitzhak

AU - Rodnina, Marina

AU - Cox, Jürgen

AU - Merbl, Yifat

AU - Satpathy, Ansuman T.

AU - Carmi, Yaron

AU - Erhard, Florian

AU - Suzuki, Tsutomu

AU - Buskirk, Allen R.

AU - Olweus, Johanna

AU - Ruppin, Eytan

AU - Schlosser, Andreas

AU - Samuels, Yardena

PY - 2025/1/1

Y1 - 2025/1/1

N2 - Aberrant peptides presented by major histocompatibility complex (MHC) molecules are targets for tumor eradication, as these peptides can be recognized as foreign by T cells. Protein synthesis in malignant cells is dysregulated, which may result in the generation and presentation of aberrant peptides that can be exploited for T cell-based therapies. To investigate the role of translational dysregulation in immunological tumor control, we disrupt translation fidelity by deleting tRNA wybutosine (yW)-synthesizing protein 2 (TYW2) in tumor cells and characterize the downstream impact on translation fidelity and immunogenicity using immunopeptidomics, genomics, and functional assays. These analyses reveal that TYW2 knockout (KO) cells generate immunogenic out-of-frame peptides. Furthermore, Tyw2 loss increases tumor immunogenicity and leads to anti-programmed cell death 1 (PD-1) checkpoint blockade sensitivity in vivo. Importantly, reduced TYW2 expression is associated with increased response to checkpoint blockade in patients. Together, we demonstrate that defects in translation fidelity drive tumor immunogenicity and may be leveraged for cancer immunotherapy.

AB - Aberrant peptides presented by major histocompatibility complex (MHC) molecules are targets for tumor eradication, as these peptides can be recognized as foreign by T cells. Protein synthesis in malignant cells is dysregulated, which may result in the generation and presentation of aberrant peptides that can be exploited for T cell-based therapies. To investigate the role of translational dysregulation in immunological tumor control, we disrupt translation fidelity by deleting tRNA wybutosine (yW)-synthesizing protein 2 (TYW2) in tumor cells and characterize the downstream impact on translation fidelity and immunogenicity using immunopeptidomics, genomics, and functional assays. These analyses reveal that TYW2 knockout (KO) cells generate immunogenic out-of-frame peptides. Furthermore, Tyw2 loss increases tumor immunogenicity and leads to anti-programmed cell death 1 (PD-1) checkpoint blockade sensitivity in vivo. Importantly, reduced TYW2 expression is associated with increased response to checkpoint blockade in patients. Together, we demonstrate that defects in translation fidelity drive tumor immunogenicity and may be leveraged for cancer immunotherapy.

KW - cancer immunopeptidome

KW - immune checkpoint blockade

KW - neoantigens

KW - non-canonical peptides

KW - translation fidelity

UR - http://www.scopus.com/inward/record.url?scp=105001399748&partnerID=8YFLogxK

U2 - 10.1016/j.ccell.2025.03.003

DO - 10.1016/j.ccell.2025.03.003

M3 - مقالة

C2 - 40154482

SN - 1535-6108

JO - Cancer Cell

JF - Cancer Cell

ER -

Translation dysregulation in cancer as a source for targetable antigens

Abstract

Keywords

All Science Journal Classification (ASJC) codes

UN SDGs

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